Difference between revisions of "Medical liver disease"

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This article deals with '''medical liver disease'''.  An introduction to the liver and approach is found in the ''[[liver]]'' article.
[[Image:Ground glass hepatocytes high mag cropped 2.jpg|thumb|right|[[Micrograph]] showing ground glass hepatocytes, as seen in chronic [[hepatitis B]]. [[H&E stain]].]]
This article deals with '''medical [[liver]] disease'''.  An introduction to the liver and approach is found in the ''[[liver]]'' article.


Every differential in liver pathology has "drugs" -- if it isn't clearly malignancy.
Every differential in liver pathology has "drugs"<ref>{{Ref PCPBoD8|448}}</ref> -- if it isn't clearly malignancy.


Liver neoplasms are dealt with in the ''[[liver neoplasms]]'' article.
Liver neoplasms are dealt with in the ''[[liver neoplasms]]'' article.
Medical liver biopsies are often non-specific, as the liver has the same appearance for many mechanisms of injury, especially when the injury is marked. The clinical history, serology and imaging are essential for proper interpretations in this domain of pathology.
=Review of liver blood work=
===Inflammation activity===
*ALT.
*AST.
===Cholestatic markers===
*ALP.
*GGT - used to assess whether the ALP is an "honest" value, elevated in cirrhosis.
===Cirrhosis/decompensation===
*PLT - low is suggestive of dysfunction.
*INR - high is bad, unless anticoagulated.
===Other===
*Bilirubin.
**Direct (AKA conjugated).
**Indirect (AKA unconjugated).
A short DDx of elevated:<ref>{{Ref PCPBoD8|441}}</ref>
*Indirect:
**[[Gilbert syndrome]].
**Crigler-Najjar syndrome type 1.
**Crigler-Najjar syndrome type 2.
*Direct:
**Rotor syndrome.
**Dubin-Johnson syndomre.
===Viral hepatitis===
*HBV DNA.
*HCV RNA.
*HBs Ag, HBs Ab, HBe Ag, HBe Ab.
*HCV Ab.
Others:
*[[Epstein-Barr virus]] (EBV).
*[[Cytomegalovirus]] (CMV) - especially in the immune incompetent.
====Hepatitis B====
Meaning & utility of the various [[Hepatitis B]] tests:<ref>URL: [http://www.clevelandclinicmeded.com/medicalpubs/diseasemanagement/hepatology/hepatitis-B/ http://www.clevelandclinicmeded.com/medicalpubs/diseasemanagement/hepatology/hepatitis-B/]. Accessed on: 16 May 2011.</ref><ref name=lto_hepb>URL: [http://www.labtestsonline.org/understanding/analytes/hepatitis_b/test.html http://www.labtestsonline.org/understanding/analytes/hepatitis_b/test.html]. Accessed on: 16 May 2011.</ref>
{| class="wikitable sortable" border="1"
! Test name
! Location
! Positive test
! Negative test
! Usual question
|-
| HBs Ag||Surface||Virus active||No active infection||Active infection?
|-
| HBs Ab||Surface||Exposed OR vaccinated||No exposure OR no vaccine OR loss of Ab||Immunization status?
|-
| HBe Ag||Virus core||Infect. w/ viral replication||No active infection||Active infect. w/ viral replication?
|-
| HBe Ab||Virus core||Exposed to virus||Infect. w/o antibody response OR not exposed||Immune response to infection?
|-
| HBV DNA||-||Active||Not active/no exposure||Viral load/how active?
|-
| HBc Ab||Virus core||Virus active/previous exposure||No exposure||Early active infection?
|}
Notes:
*''HBc Ab'' may test for acute (IgM) or chronic infection - dependent on specific antibody test; it is often used to look for early infection.<ref name=lto_hepb>URL: [http://www.labtestsonline.org/understanding/analytes/hepatitis_b/test.html http://www.labtestsonline.org/understanding/analytes/hepatitis_b/test.html]. Accessed on: 16 May 2011.</ref>
*''Carriers of hepatitis B'': HBs Ag +ve, HBs Ab -ve, HBc Ag -ve, HBc Ab +ve, HBe Ag -ve, HBe Ab +ve.<ref>URL: [http://labtestsonline.org/understanding/analytes/hepatitis-b/tab/test http://labtestsonline.org/understanding/analytes/hepatitis-b/tab/test]. Accessed on: 3 May 2012.</ref>
===Markers for rare liver diseases===
*Ceruloplasm - low think ''[[Wilson's disease]]''; typical value for Wilson's ~ 0.12 g/L.
**<0.20 g/L is a criteria for Wilson's disease.<ref name=pmid18556333>Diagnostic accuracy of serum ceruloplasmin in Wilson disease: determination of sensitivity and specificity by ROC curve analysis among ATP7B-genotyped subjects. Mak CM, Lam CW, Tam S. Clin Chem. 2008 Aug;54(8):1356-62. Epub 2008 Jun 12. PMID 18556333. URL: [http://www.clinchem.org/cgi/reprint/54/8/1356.pdf http://www.clinchem.org/cgi/reprint/54/8/1356.pdf]. Accessed on: 28 September 2009.</ref>
*Alpha-1 antitrypsin - if low think ''deficiency''.
===Hemosiderosis===
*Ferritin - high.
*Iron saturation - high.
Causes:
*Hemochromatosis.
*Hemolysis, chronic.
*Cirrhosis.
=Medical imaging=
Blood flow:<ref>URL: [http://insidesurgery.com/2010/12/hepatopedal-hepatofugal-flow/ http://insidesurgery.com/2010/12/hepatopedal-hepatofugal-flow/]. Accessed on: 2 December 2011.</ref>
*Hepatopedal flow = normal portal vein flow.
*Hepatofugal flow = reversed portal vein flow.
==Interventional measurements==
Wedged to free hepatic venous pressure:<ref name=pmid1864548>{{Cite journal  | last1 = Bion | first1 = E. | last2 = Brenard | first2 = R. | last3 = Pariente | first3 = EA. | last4 = Lebrec | first4 = D. | last5 = Degott | first5 = C. | last6 = Maitre | first6 = F. | last7 = Benhamou | first7 = JP. | title = Sinusoidal portal hypertension in hepatic amyloidosis. | journal = Gut | volume = 32 | issue = 2 | pages = 227-30 | month = Feb | year = 1991 | doi =  | PMID = 1864548 | PMC = 1378815 | URL = http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1378815/?tool=pubmed }}</ref>
*Normal = 1-4 mmHg.
**Elevated in [[portal hypertension]].
=Liver biopsy=
==Medical liver biopsy adequacy==
Liver biopsy specimens should be:<ref>{{Ref MacSween|418}}</ref>
*2.0 cm in length and contain 11-15 portal tracts,
*The core should be deeper than 1.0 cm from the liver capsule; specimens close to the capsule may lead to over grading of fibrosis.
==Reporting==
{{Main|Pathology reports}}
<pre>
Specimen, procedure:
- Diagnosis.
</pre>
The diagnosis usually contains grading and staging information, e.g. ''activity 2 /4, Laennec fibrosis stage 1 /4''.
In the context of medical liver disease:
*Grade = inflammation/activity.
*Stage = severity of fibrosis/architectural changes.
Notes:
*The term "acute" is infrequently used in liver pathology.
*In the liver: neutrophils ''is not'' acute -- unlike most elsewhere in the body.<ref>OA. September 2009.</ref>
===A microscopic checklist===
<pre>
Size of biopsy: Adequate
Fragmentation: Absent
Fibrosis: Stage 2-3/4, mostly stage 2
Fibrous septa: Present
Septa with curved contours: Present – focally only
Large droplet steatosis (% of hepatocytes): Present, moderate 60%
Ballooning of hepatocytes: Present, rare
Mallory-Denk bodies: Present, rare
Portal inflammation: Present
Interface activity: Minimal (0-1/4)
Lobular necroinflammation: Minimal
Ducts: Present in normal numbers
Duct injury: Absent
Ductular reaction: Absent
Cholestasis: Absent
Terminal hepatic venules: Present
Iron stain: Absent
Ground glass cells with routine stains: Absent
PASD for alpha-1 antitrypsin droplets: Negative
</pre>
=Viral hepatitis=
These are common.  The diagnoses are based on serology. The serology is covered in the ''[[Liver_pathology#Viral_hepatitis|viral hepatitis]]'' section in the ''[[liver pathology]]'' article.
Typically classified as:<ref name=pmid8048409>{{Cite journal  | title = Terminology of chronic hepatitis, hepatic allograft rejection, and nodular lesions of the liver: summary of recommendations developed by an international working party, supported by the World Congresses of Gastroenterology, Los Angeles, 1994. | journal = Am J Gastroenterol | volume = 89 | issue = 8 Suppl | pages = S177-81 | month = Aug | year = 1994 | doi =  | PMID = 8048409 }}</ref><ref>URL: [http://familydoctor.org/familydoctor/en/diseases-conditions/hepatitis-b.html http://familydoctor.org/familydoctor/en/diseases-conditions/hepatitis-b.html]. Accessed on: 2 May 2012.</ref>
#Acute < 6 months duration.
#Chronic > 6 months duration.


==Hepatitis A==
==Hepatitis A==
*Uncommon biopsy specimen - as the infection is self-limited.
*Infection is self-limited, i.e. not persistent.
**May present as ''[[fulminant hepatic necrosis]]''.
*Usually asymptomatic in children.<ref name=pmid20068336>{{cite journal |author=Jeong SH, Lee HS |title=Hepatitis A: clinical manifestations and management |journal=Intervirology |volume=53 |issue=1 |pages=15–9 |year=2010 |pmid=20068336 |doi=10.1159/000252779 |url=}}</ref>
*Serology is diagnostic.
*Serology is diagnostic.


==Hepatitis B==
==Hepatitis B==
===General===
:''Hepatitis B virus'', abbreviated ''HBV'', redirects here.
*May lead to hepatocellular carcinoma without cirrhosis.
{{Main|Hepatitis B}}
*High prevalence.
 
*Diagnosis is by serology.
==Hepatitis C==
{{Main|Hepatitis C}}


===Histology===
=Other infections=
*Ground glass hepatocytes - see [[liver|introduction]].
*Hydatid disease (Hydatid cyst).
*Ascaris.
*Fasciola


==Hepatitis C==
==Hydatid disease==
*[[AKA]] ''hydatid cyst''.
===General===
===General===
*Leads to hepatocellular carcinoma in the setting of cirrhosis.
*Etiology: ''[[Echinococcus]]''.
*Tends to be chronic; the "C" in "hepatitis C" stands for ''chronic''.
*Diagnosis is by serology.


===Histology===
===Microscopic===
*Lobular inflammation - this is non-specific finding.
Features:
*Periportal steatosis in genotype 3.<ref name=pmid16614743>Yoon EJ, Hu KQ. Hepatitis C virus (HCV) infection and hepatic steatosis. Int J Med Sci. 2006;3(2):53-6. Epub 2006 Apr 1. PMID 16614743. Avialable at: [http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=1415843 http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=1415843]. Accessed on: September 9, 2009.</ref>
*Laminated wall +/- calcification.<ref name=Ref_PBPoD8_448>{{Ref PCPBoD8|448}}</ref>
**Steatosis in hepatitis C is usually a secondary pathology, i.e. a separate pathologic process.<ref>OA. September 2009.</ref>
*Organisms -- see ''[[Echinococcus]]''.


==Congestive hepatopathy==
====Images====  
*Liver failure due to (right) heart failure.
<gallery>
*AKA ''cardiac cirrhosis'' - a term used by clinicians.
Image:Liver_cyst_wall_-_intermed_mag.jpg | Liver cyst wall - intermed. mag. (WC)
**Generally, it does not satisfy pathologic criteria for cirrhosis.<ref>[http://emedicine.medscape.com/article/151792-overview]</ref>
Image:Liver_cyst_wall_-_high_mag.jpg | Liver cyst wall - high mag. (WC)
Image: Laminated liver cyst wall - intermed mag.jpg | Characteristic laminated portion - intermed. mag. (WC)
Image: Laminated liver cyst wall - high mag.jpg | Characteristic laminated portion - high mag. (WC)
</gallery>
[[www]]:
*[http://pathmicro.med.sc.edu/parasitology/hydatid-hist1.jpg Hydatid cyst (med.sc.edu)].
*[http://www.atlas.or.kr/atlas/include/viewImg.html?uid=645 Hydatid cyst (atlas.or.kr)].
*[http://casereports.bmj.com/content/2009/bcr.04.2009.1798.full Hydatid cyst (casereports.bmj.com)].


===Gross===
==Abscess==
*"Nutmeg" liver - yellow spotted appearance.
A. [[File:1 ABS 1 680x512px.tif|A process replaces most of the liver parenchyma (20X).]]
<br>
B. [[File:2 ABS 1 680x512px.tif|Fibrinopurulent exudate apposes granulation tissue (200X).]]
<br>
C. [[File:3 ABS 1 680x512px.tif|Neutrophils lie in widened sinusoids (200X)..]]
<br>
D. [[File:4 ABS 1 680x512px.tif|Trichrome shows collagenization of spaces of Disse. Scarring about an abscess or other mass lesion should not be interpreted as reflective of the liver in general (200X).]]
<br>
Abscess. A. A process replaces most of the liver parenchyma. B. Fibrinopurulent exudate apposes granulation tissue. C. Neutrophils lie in widened sinusoids. D. Trichrome shows collagenization of spaces of Disse. Scarring about an abscess or other mass lesion should not be interpreted as reflective of the liver in general (LR 200X).


===Histologic===
==Coccidiomycosis==
Features:<ref>[http://emedicine.medscape.com/article/151792-diagnosis http://emedicine.medscape.com/article/151792-diagnosis]</ref>
A. [[File:Coccidiomycosis - 1 - 40X 680x512px shot.tif|500x500px Granulomas at low power]]
*Zone III atrophy.
<br>
*Portal venule (central vein) distension.
B. [[File:Coccidiomycosis - 1 - 200X 680x513px shot.tif|500x500px Granulomas with centrally crowded cells & lady slipper macrophage nuclei]]
*Perisinusoidal fibrosis - progresses to centrilobular fibrosis and then diffuse fibrosis.
<br>
*Dilation of sinusoids in ''all'' zone III areas - '''key feature'''.<ref>Suggested by OA. September 2009.</ref>
C. [[File:Coccidiomycosis - 1 - 400X 1369x1024px shot.tif|500x500px Center of previous granuloma showing pyknotic macrophage nuclei]]
<br>
D. [[File:Coccidiomycosis - 1 - GMS 400X 1369x1024px shot.tif|500x500px Four Coccidiomycotic spherules]]
<br>
Coccidiomycosis. A. Note the granulomas in otherwise undisturbed liver (UL). B. Granuloma with centrally crowded cells & lady slipper macrophage nuclei. C. Center of granuloma with pyknotic macrophage nuclei, "necrotizing". D. Organisms on GMS stain.


=Metabolic and toxic=
==Alcoholic liver disease==
==Alcoholic liver disease==
*Acute and/or chronic liver changes due to alcohol use.
===General===
*Includes ASH (alcoholic steatohepatitis).
*Acute and/or chronic liver changes due to excessive [[alcohol]] use - includes:
**''[[Alcoholic steatohepatitis]]'' (ASH), [[AKA]] ''alcoholic hepatitis''.<ref>URL: [http://emedicine.medscape.com/article/170539-overview http://emedicine.medscape.com/article/170539-overview]. Accessed on: 3 May 2012.</ref>
***Alcoholic hepatitis can be with minimal steatosis.<ref>STC. 6 December 2010.</ref>
**[[Steatosis]] - classically macrovescicular and centrilobular.
**Alcoholic [[cirrhosis]].


===Classic lab findings in EtOH abusers===
====Classic lab findings in EtOH abusers====
*AST & ALT elevated with AST:ALT=2:1.
*AST & ALT elevated with AST:ALT=2:1.
*GGT elevated.
*GGT elevated.
Line 57: Line 226:
**May be macronodular.
**May be macronodular.


===Histopathology===
===Microscopic===
See:  
See:  
*''[[Steatohepatitis]]'' section and ''[[ballooning degeneration]]'' section.
*''[[Steatohepatitis]]'' section and ''[[ballooning degeneration]]'' section.
Line 63: Line 232:
Features:
Features:
*Often zone III damage.
*Often zone III damage.
*Neutrophils (often helpful to differentiate) -- few other things have PMNs.
*Cholestatsis common, i.e. yellow staining.
*Cholestatsis common, i.e. yellow staining.
**NASH (non-alcoholic steatohepatitis) usu. does not have cholestasis.<ref>STC. 6 December 2010.</ref>
*Fibrosis starts at central veins.
*Fibrosis starts at central veins.
*Neutrophils (often helpful) -- few other things have PMNs. (???)
**Neutrophils cluster around cells with Mallory hyaline.
====Images====
A. [[File:1 etoh 3 680x512px.tif| Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).]]
<br>
B. [[File:2 etoh 3 680x512px.tif| Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).]]
<br>
C. [[File:3 etoh 3 680x512px.tif| Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).]]
<br>
D. [[File:4 etoh 3 680x512px.tif| Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).]]
<br>
E. [[File:5 etoh 3 680x512px.tif| Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).]]
<br>
F. [[File:6 etoh 3 680x512px.tif| Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).]]
<br>
Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).
A. Trichrome shows relatively non-inflamed fibrous bands, as well as [between green dots] nodules. The lack of regeneration throughout might have precluded a diagnosis of cirrhosis, but stage IV fibrosis under the Metavir system is justified. B. Reticulin shows regenerative nodules [left] with mostly two or more nuclei between black lines juxtaposed to non-regenerative hepatocytes on the right, without piecemeal necrosis. C. Regenerative nodules show occasional neutrophils [red arrow] and cytoplasmic tufts of ballooned cells, sometimes possibly Mallory hyalin [green arrows]. D. Triads (note vein [green arrow], artery [yellow arrow], and interlobular bile duct [blue arrow]) generally showed little or no interface hepatitis, even when expanded by fibrosis and inflamed. E. Occasional foci of spotty necrosis were seen.  F. This edge of an inflamed triads shows neutrophils about proliferated bile ducts [red arrows], as well as Mallory-Denk bodies [blue arrows].
<br>
A. [[File:1 etoh 4 680x512px.tif| Cirrhosis in an alcoholic.]]
<br>
B. [[File:2 etoh 4 680x512px.tif| Cirrhosis in an alcoholic.]]
<br>
C. [[File:3 etoh 4 680x512px.tif| Cirrhosis in an alcoholic.]]
<br>
D. [[File:4 etoh 4 680x512px.tif| Cirrhosis in an alcoholic.]]
<br>
E. [[File:5 etoh 4 680x512px.tif| Cirrhosis in an alcoholic.]]
<br>
F. [[File:6 etoh 4 680x512px.tif| Cirrhosis in an alcoholic.]]
<br>
Definite cirrhosis in an alcoholic. A. Hepatocyte free bands parse tissue, with occasional definite islands [arrows]. B. Trichrome establishes blue fibrosis about isles [arrows]. C. Reticulin stain shows nodules with regeneration, wherein a large proportion of them are at least two nuclei thick [arrows]. D. Bile duct proliferation can be difficult, sometimes mimicking cholangiocarcinoma. Follow the double headed arrows to see how the ductules can be seen to proliferate from a single sources, with all ducts being complete, without necrotic epithelial cells. E. PAS with distase can help, as cholangiocarcinoma generally lacks the red rim of proliferating bile ductules [arrows]; again note the connections that can be made between the ductule openings by the blue double headed arrows. The cyan double headed arrows show general parallelism, consistent with uniform directionality induced by extrinsic force, not a neoplastic spread. F. Trichrome shows the most difficult focus. Double headed arrows display the connectivity seen before of the proliferated bile ductules. Note that numerous pairs of adjacent perpendicular glands without a head to foot appearance are not seen that would indicate the disorderly spread of cholangiocarcinoma.
<br>
A. [[File:1 ALC 2 680x512px.tif|Expanded, inflamed triads with increased bile duct/vascular openings. Mild steatosis (40X).]]
<br>
B. [[File:2 ALC 2 680x512px.tif|Trichrome stain shows periportal fibrosis [red arrowheads] (200X).]]
<br>
C. [[File:3 ALC 2 680x512px.tif|PAS with diastase stain shows proliferated bile ductules [blue arrowheads] in stroma with mixed inflammatory infiltrate (400X)]]
<br>
D. [[File:4 ALC 2 680x512px.tif|Neutrophils about ballooned hepatocyte (satellitosis) [yellow arrowheads]. Councilman bodies [green arrowheads] (400X).]]
<br>
Alcoholic hepatitis without cirrhosis. No history of viral disease. AMA negative. A. Expanded, inflamed triads with increased bile duct/vascular openings. Mild steatosis. B. Trichrome stain shows periportal fibrosis [red arrowheads]. C. PAS with diastase stain shows proliferated bile ductules [blue arrowheads] in stroma with mixed inflammatory infiltrate. D. Neutrophils about ballooned hepatocyte (satellitosis) [yellow arrowheads]. Councilman bodies [green arrowheads].


Notes:
Notes:
Line 82: Line 295:


==Steatohepatitis==
==Steatohepatitis==
*''Steatohepatitis'' is a label for a set of histopathologic findings.
{{Main|Steatohepatitis}}
**May arise due to numerous etiologies, e.g. alcoholic steatohepatitis (ASH), non-alcoholic steatohepatitis (NASH).
*Fat accumulation in hepatocytes. 
**It may be a pattern seen in drug toxicity, e.g. methotrexate toxicity.<ref>MG. 22 September 2009.</ref>
 
===Histology===
Features:
*Steatosis (usually macrovesicular) - '''key feature'''.
**If less than 10% ... consider alt. diagnosis/disease process.
*Hepatocyte injury:
**Ballooning degeneration - '''key feature''' (see above for features).
**Mallory bodies.
***Mallory body wannabes: "occasional cytoplasmic clumping".
*+/-''Chicken-wire'' perisinusoidal fibrosis +/- zone III (centrilobular) fibrosis (early).
**Late-stage disease - portal bridging.<ref name=pmid14991537>{{Cite journal  | last1 = Gramlich | first1 = T. | last2 = Kleiner | first2 = DE. | last3 = McCullough | first3 = AJ. | last4 = Matteoni | first4 = CA. | last5 = Boparai | first5 = N. | last6 = Younossi | first6 = ZM. | title = Pathologic features associated with fibrosis in nonalcoholic fatty liver disease. | journal = Hum Pathol | volume = 35 | issue = 2 | pages = 196-9 | month = Feb | year = 2004 | doi =  | PMID = 14991537 }}</ref>
 
===Grading steatohepatitis===
Grading inflammation:<ref name=pmid10484010>Nonalcoholic steatohepatitis: a proposal for grading and staging the histological lesions. Brunt EM, Janney CG, Di Bisceglie AM, Neuschwander-Tetri BA, Bacon BR. Am J Gastroenterol. 1999 Sep;94(9):2467-74. PMID 10484010.</ref>
*Grade 1 - steatosis, occ. ballooning degen., PMNs.
*Grade 2 - obvious ballooning, obvious PMNs, chronic inflammation.
*Grade 3 - panacinar steatosis.


=Autoimmune=
==Autoimmune hepatitis==
==Autoimmune hepatitis==
===General===
*Abbreviated ''AIH''.
*Abbreviated ''AIH''.
*Several criteria exist to diagnose.
{{Main|Autoimmune hepatitis}}


===Diagnosis===
==Primary biliary cirrhosis==
Simplifed diagnostic criteria (2008):<ref name=pmid19675998>Scoring systems for the diagnosis of autoimmune hepatitis: past, present, and future. Wiegard C, Schramm C, Lohse AW. Semin Liver Dis. 2009 Aug;29(3):254-61. Epub 2009 Aug 12. PMID 19675998</ref>
*Abbreviated PBC.
#Antibody titer.
{{Main|Primary biliary cirrhosis}}
#Elevated IgG.
#Liver pathology.
#Exclusion of viral hepatitis.


Details (scoring):<ref name=pmid19675998/>
==Autoimmune hepatitis with obstruction - combined changes==
*ANA or SMA 1:40 1 point.
A. [[File:1 AIH OBS 1.tif|Low power shows inflammation; portal triads, lobules, central veins cannot be distinguished (40X).]]
*ANA or SMA 1:80 2 points.
<br>
*LKM 1:40 2 points.
B. [[File:2 AIH OBS 1.tif|Trichrome shows central venous sclerosis (red arrowhead), periportal fibrosis (green arrowhead), & space of Disse collagenization (yellow arrowhead); juxtaposition of central vein & portal tract indicates collapse, no definite bridging was seen (100X)]]
*IgG upper normal 1 point.
<br>
*IgG 1.1x upper limit 2 points.
C. [[File:3 AIH OBS 1.tif|Central vein is inflamed with a rare plasma cell (cyan arrowhead) (400X).]]
*Histology compatible 1 point.
<br>
*Typical AIH histo. 2 points.
D. [[File:4 AIH OBS 1.tif|Interface hepatitis with plasma cells (yellow arrows) and ballooned hepatocytes (red arrows).  Lobule is disorganized (400X).]]
*No viral hepatsis 2 points.
<br>
E. [[File:5 AIH OBS 1.tif|Proliferating bile ductules (blue arrows) with occasional neutrophils (fucsia arrows), indicative of obstruction, but not acute cholangitis, which requires inflamed bile duct itself, best diagnosed with associated blood vessel (400X).]]
<br>
F. [[File:6 AIH OBS 1.tif|Rare distorted rosettes with greenish brown strands of bile (left arrow) or bile plugs (right arrow) (400X).]]
<br>
Patient with SLE and obstructive jaundice that resolved with apparent passage of stone. A. Low power shows inflammation; portal triads, lobules, central veins cannot be distinguished. B. Trichrome shows central venous sclerosis (red arrowhead), periportal fibrosis (green arrowhead), & space of Disse collagenization (yellow arrowhead); juxtaposition of central vein & portal tract indicates collapse, no definite bridging was seen. C. Central vein is inflamed with a rare plasma cell (cyan arrowhead). D. Interface hepatitis with plasma cells (yellow arrows) and ballooned hepatocytes (red arrows). Lobule is disorganized. E. Proliferating bile ductules (blue arrows) with occasional neutrophils (fucsia arrows), indicative of obstruction, but not acute cholangitis, which requires inflamed bile duct itself, best diagnosed with associated blood vessel. F. Rare distorted rosettes with greenish brown strands of bile (left arrow) or bile plugs (right arrow).


Interpretation:
==Autoimmune hepatitis-primary biliary cirrhosis overlap syndrome==
Definite >= 7.
*Abbreviation ''AIH-PBC OS''.
Probable = 6.
===General===
Epidemiology:
*Rare.


Notes:
Serology:<ref name=pmid19491855>{{Cite journal  | last1 = Muratori | first1 = P. | last2 = Granito | first2 = A. | last3 = Pappas | first3 = G. | last4 = Pendino | first4 = GM. | last5 = Quarneti | first5 = C. | last6 = Cicola | first6 = R. | last7 = Menichella | first7 = R. | last8 = Ferri | first8 = S. | last9 = Cassani | first9 = F. | title = The serological profile of the autoimmune hepatitis/primary biliary cirrhosis overlap syndrome. | journal = Am J Gastroenterol | volume = 104 | issue = 6 | pages = 1420-5 | month = Jun | year = 2009 | doi = 10.1038/ajg.2009.126 | PMID = 19491855 }}</ref>
*Autoantibodies may be seen in HCV.<ref name=pmid19675998/>
*AMA +ve.
*A normal IgG is very unusual in AIH - but may be seen in atypical variants with zone III involvment.
*Anti-dsDNA +ve.


Abbreviations:
===Microscopic===
*ANA = anti-nuclear antibody.
:See: ''[[autoimmune hepatitis]]'' and ''[[primary biliary cirrhosis]]''.
*SMA = smooth muscle antibody.
A. [[File:1 AIH PBC 1 680x512px.tif|Expanded portal tracts with fuzzy edges (40X).]]
*LKM-1 = liver kidney microsomal type 1 antibody.
<br>
B. [[File:2 AIH PBC 1 680x512px.tif|Interface hepatitis with plasma cells (400X).]]
<br>
C. [[File:3 AIH PBC 1 680x512px.tif|Loose granuloma (400X).]]
<br>
D. [[File:4 AIH PBC 1 680x512px.tif|Damaged bile duct (400X).]]
<br>
AIH/PBC overlap. AMA & ANA positive with Alkaline phosphatase > 2 upper limit of normal & one ALT > 5 times upper limit of normal. A. Expanded portal tracts with fuzzy edges. B. Interface hepatitis with plasma cells. C. Loose granuloma. D. Damaged bile duct.


===Histology===
==Primary sclerosing cholangitis==
Classification:<ref name=pmid19675998/>
*Abbreviated ''PSC''.
*Typical:
{{Main|Primary sclerosing cholangitis}}
**Interface hepatitis (zone 1).
***Lymphocytic/lymphoplasmacytic infiltration of portal tracts + lobule.
**Emperipolesis - one cell penetrates into another one.
**Hepatic rosette.
*Compatible
**Chronic hepatitis - with lymphocytic dominant.
*Atypical:
**Signs of other disease.


Notes:
=Hereditary=
*PAS may be useful - find plasma cells. (???)
==Caroli disease==
*Atypical Autoimmune hepatitis may have zone III involvment (lymphoplasmacytic infiltrate)<ref name=pmid19452572>Non-classical phenotypes of autoimmune hepatitis and advances in diagnosis and treatment. Czaja AJ, Bayraktar Y. World J Gastroenterol. 2009 May 21;15(19):2314-28. Review. PMID 19452572.</ref> and a normal IgG.<ref>FW. 21 September 2009.</ref>
===General===
*Genetic disease.
**Frequently associated with [[autosomal recessive polycystic kidney disease]] (ARPKD).<ref name=omim263200>{{OMIM|263200}}</ref>
**May be seen in isolation.<ref name=omim600643>{{OMIM|600643}}</ref>


Micrographs:
Clinical:<ref name=pmid17461493>{{Cite journal  | last1 = Yonem | first1 = O. | last2 = Bayraktar | first2 = Y. | title = Clinical characteristics of Caroli's syndrome. | journal = World J Gastroenterol | volume = 13 | issue = 13 | pages = 1934-7 | month = Apr | year = 2007 | doi =  | PMID = 17461493 }}</ref>
*[http://www.ajronline.org/cgi/content/full/185/4/971/FIG3 Emperipolesis (ajronline.org)]
*Recurrent [[cholangitis]].
*[http://moon.ouhsc.edu/kfung/jty1/Com07/Com07Image/Com705-05b.gif Emperipolesis (ouhsc.edu)]
*Recurrent [[cholelithiasis]].
*[[Cholangiocarcinoma]]<ref name=pmid17461492>{{Cite journal  | last1 = Yonem | first1 = O. | last2 = Bayraktar | first2 = Y. | title = Clinical characteristics of Caroli's disease. | journal = World J Gastroenterol | volume = 13 | issue = 13 | pages = 1930-3 | month = Apr | year = 2007 | doi =  | PMID = 17461492 }}</ref> - seen in ~7% of cases.<ref name=pmid15347876>{{Cite journal  | last1 = Karim | first1 = AS. | title = Caroli's disease. | journal = Indian Pediatr | volume = 41 | issue = 8 | pages = 848-50 | month = Aug | year = 2004 | doi =  | PMID = 15347876 }}</ref>


===Treatment===
Note:
*Immunosuppresants (prednisone, azathioprine).<ref name=pmid19452572>Non-classical phenotypes of autoimmune hepatitis and advances in diagnosis and treatment. Czaja AJ, Bayraktar Y. World J Gastroenterol. 2009 May 21;15(19):2314-28. Review. PMID 19452572.</ref>
*''Caroli syndrome'' = Caroli disease + congenital hepatic fibrosis.<ref name=pmid15888616>{{Cite journal  | last1 = Brancatelli | first1 = G. | last2 = Federle | first2 = MP. | last3 = Vilgrain | first3 = V. | last4 = Vullierme | first4 = MP. | last5 = Marin | first5 = D. | last6 = Lagalla | first6 = R. | title = Fibropolycystic liver disease: CT and MR imaging findings. | journal = Radiographics | volume = 25 | issue = 3 | pages = 659-70 | month =  | year =  | doi = 10.1148/rg.253045114 | PMID = 15888616 | URL = http://radiographics.rsna.org/content/25/3/659.long }}</ref>


==Primary biliary cirrhosis==
===Gross===
*Abbreviated PBC.
*Dilated bile ducts.<ref name=omim263200/>
 
===Microscopic===
Features:<ref name=pmid17461493/>
*Dilated bile ducts.
*Periductal fibrosis. (???)
*+/-Fibrosis.


===Epidemiology===
Image:
*Female>male (~9:1).<ref>DCHH P.162.</ref>
*[http://www.meddean.luc.edu/lumen/MedEd/orfpath/11-3-10.jpg Caroli disease (meddean.luc.edu)].<ref>URL: [http://www.meddean.luc.edu/lumen/MedEd/orfpath/develop.htm http://www.meddean.luc.edu/lumen/MedEd/orfpath/develop.htm]. Accessed on: 1 December 2011.</ref>
*Usually middle age.
*Associated with other autoimmune conditions (Sjogren's syndrome, progressive systemic sclerosis, celiac).


===Etiology===
==Hereditary hemochromatosis==
*Autoimmune.
:''For secondary causes see [[secondary hemochromatosis]]''.
{{Main|Hereditary hemochromatosis}}


===Serology===
==Wilson disease==
*AMA+.
{{Main|Wilson's disease}}


===Classic presentation===
==Alpha-1 antitrypsin deficiency==
*Pruritis.
*[[AKA]] ''alpha1-antiprotease inhibitor deficiency''.
{{Main|Alpha-1 antitrypsin deficiency }}


===Pathophysiology===
=Other=
*Septal bile duct attacked.
==Primary Systemic Sclerosis==
[[File:5 05168051 sl 1.png |Primary systemic sclerosis in the liver]]
[[File:5 05168051 sl 2.png |Primary systemic sclerosis in the liver]]
[[File:5 05168051 sl 3.png |Primary systemic sclerosis in the liver]]
[[File:5 05168051 sl 4.png |Primary systemic sclerosis in the liver]]
[[File:5 05168051 sl 5.png |Primary systemic sclerosis in the liver]]
[[File:5 05168051 sl 6.png |Primary systemic sclerosis in the liver]]
<br>
Primary systemic sclerosis in a 67 year old White, non-Hispanic man who had undergone renal transplantation for idiopathic nodular glomerusclerosis, which had recurred in 2013. He had been scheduled to receive a second transplantation, but had not yet received one.  The patient had a positive anti-nuclear antigen study, with a positive scleroderma antibody (SCL-70), a high SCL-70 antibody index of 3.9, and negative DNA, Chromatin, Anti-Riboscomal P, SS-A, SS-B, anti Smith, RNP, JO-1, anticentromere antibody and rheumatoid factor serologic studies.  Hepatitis A, B, and C serologic studies were negative. Liver function tests showed normal albumin and total bilirubin levels with alkaline phosphatase of 712 IU/L (35-129 normal range), alanine aminotransferase 59 IU/L (5-41 normal range), and aspartate aminotransferase 68 IU/L (5-37 normal range). This case provisions many of the features known to be present in primary systemic sclerosis as seen in the skin. A. At low power, triads appear almost as white ghosts against a relatively normal set of hepatocyte lobules. B. Closer examination reveals some triads to be expanded, with peripheral bile ductular proliferation and modest associated chronic inflammation without interface hepatitis. C. Portal arterioles had thick walls; inflammation included lymphocytes and occasional plasma cells. D. Trichrome failed to stain the material in the triads blue, but did show space of Disse collagenization. E. PAS with diastase showed positive staining of the material with emphasis on the arteriole walls. F. Hemosiderosis was seen on iron stain.  


===Histopathology===
*Intraepithelial lymphocytes - in bile duct '''key feature'''.
*Bile duct epithelial cells with eosinophilic cytoplasm.<ref>OA. 11 September 2009.</ref>
*Plasma cells.
*Granulomas - close to bile duct.
**Seen in classic presentation -- often not present or poorly formed.
*Focal damage (may be missed on biopsy -- due to sampling).
*"Garland" cirrhosis -- has irregular border (unlike in EtOH).
**''Garland'' originally "wreath of flowers" (in French).<ref>[http://dictionary.reference.com/browse/garland http://dictionary.reference.com/browse/garland]</ref>


Images:
==Budd-Chiari syndrome==
*[http://commons.wikimedia.org/wiki/File:Primary_biliary_cirrhosis_low_mag.jpg PBC - low magnification (WC)].
*[[AKA]] ''hepatic vein obstruction''.
*[http://commons.wikimedia.org/wiki/File:Primary_biliary_cirrhosis_intermed_mag.jpg PBC - intermediate magnification (WC)].
===General===
*[http://www.gidesigns.net/images/MC-copper-flower-garland-L.jpg Garland - wreath of flowers (gidesigns.net)].
*Hepatic outflow obstruction.


DDx:<ref>DCHH P.163.</ref>
Clinical triad:<ref name=pmid21573256>{{Cite journal  | last1 = Fox | first1 = MA. | last2 = Fox | first2 = JA. | last3 = Davies | first3 = MH. | title = Budd-Chiari syndrome--a review of the diagnosis and management. | journal = Acute Med | volume = 10 | issue = 1 | pages = 5-9 | month =  | year = 2011 | doi =  | PMID = 21573256 }}</ref>
*Sarcoidosis (if granulomas present).
*Ascites.
*PSC, viral hepatitis, AIH, drugs, Hodgkin's lymphoma<ref name=pmid19131796>Vanishing bile duct syndrome and Hodgkin disease: a case series and review of the literature. Pass AK, McLin VA, Rushton JR, Kearney DL, Hastings CA, Margolin JF. J Pediatr Hematol Oncol. 2008 Dec;30(12):976-80. PMID 19131796.</ref>
*Abdominal pain.
*Hepatomegaly.


===Staging===
Etiology:
PBC is staged according to Ludwig:<ref>PBC. eMedicine.com. URL: [http://emedicine.medscape.com/article/171117-diagnosis http://emedicine.medscape.com/article/171117-diagnosis]. Accessed on: 22 September 2009.</ref>
*~50% have a [[myeloproliferative disease]].<ref name=pmid18814079>{{Cite journal  | last1 = Plessier | first1 = A. | last2 = Valla | first2 = DC. | title = Budd-Chiari syndrome. | journal = Semin Liver Dis | volume = 28 | issue = 3 | pages = 259-69 | month = Aug | year = 2008 | doi = 10.1055/s-0028-1085094 | PMID = 18814079 }}</ref>
*Stage 1: Portal - inflammation or bile duct abnormalities.
*May be due to mass effect from a tumour.
*Stage 2: Periportal - periportal fibrosis (enlargement of portal tracts) +/- inflammation.
*Stage 3: Septal - septal fibrosis +/-inflammation in septa.
*Stage 4: Cirrhosis - nodules of hepatocytes +/- inflammation.


Notes:
Clinical DDx:
*There can be significant variation in staging on biopsy - due to variability of fibrosis in a PBC liver.<ref>J Clin Pathol. 1996 July; 49(7): 556-559. Available at: [http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=500569 http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=500569]. Accessed on: September 22, 2009.</ref>
*[[Hepatic veno-occlusive disease]].
**"Worst area" in biopsy specimen is used to determine stage.


===Treatment===
===Microscopic===
*Ursodeoxycholic acid.
Features:<ref name=pmid17569137>{{Cite journal  | last1 = Aydinli | first1 = M. | last2 = Bayraktar | first2 = Y. | title = Budd-Chiari syndrome: etiology, pathogenesis and diagnosis. | journal = World J Gastroenterol | volume = 13 | issue = 19 | pages = 2693-6 | month = May | year = 2007 | doi =  | PMID = 17569137 | url=http://www.wjgnet.com/1007-9327/full/v13/i19/2693.htm }}</ref>
*May be indication for transplant.
*Sinusoidal dilation in zone III (congestion).
*+/-Hepatocyte drop-out.
*+/-Centrilobular fibrosis.


DDx congestion:
*Congestive heart failure ([[congestive hepatopathy]]).
*Constrictive pericarditis.


==Autoimmune hepatitis-primary biliary cirrhosis overlap syndrome (AIH-PBC OS)==
==Vanishing bile duct syndrome==
===Epidemiology===
*[[AKA]] ''bile duct loss'', [[AKA]] ''ductopenia''.<ref name=pmid11521176/>
*Rare.
===General===
*Fatal.


===Serology===
DDx:<ref name=pmid18242505/>
*AMA+, anti-dsDNA+.<ref name=pmid19491855>The serological profile of the autoimmune hepatitis/primary biliary cirrhosis overlap syndrome. Muratori P, Granito A, Pappas G, Pendino GM, Quarneti C, Cicola R, Menichella R, Ferri S, Cassani F, Bianchi FB, Lenzi M, Muratori L. Am J Gastroenterol. 2009 Jun;104(6):1420-5. Epub 2009 Apr 28. PMID 19491855.</ref>
*[[Primary biliary cirrhosis]].
*[[Primary sclerosing cholangitis]].
*[[GVHD]].<ref name=pmid7994249>{{Cite journal  | last1 = Yeh | first1 = KH. | last2 = Hsieh | first2 = HC. | last3 = Tang | first3 = JL. | last4 = Lin | first4 = MT. | last5 = Yang | first5 = CH. | last6 = Chen | first6 = YC. | title = Severe isolated acute hepatic graft-versus-host disease with vanishing bile duct syndrome. | journal = Bone Marrow Transplant | volume = 14 | issue = 2 | pages = 319-21 | month = Aug | year = 1994 | doi =  | PMID = 7994249 }}</ref>
*[[Drug-induced liver disease|Drugs]].<ref name=pmid11352118>{{Cite journal  | last1 = Chitturi | first1 = S. | last2 = Farrell | first2 = GC. | title = Drug-induced cholestasis. | journal = Semin Gastrointest Dis | volume = 12 | issue = 2 | pages = 113-24 | month = Apr | year = 2001 | doi =  | PMID = 11352118 }}</ref>
*Chronic rejection.<ref name=pmid11521176>{{Cite journal  | last1 = Inomata | first1 = Y. | last2 = Tanaka | first2 = K. | title = Pathogenesis and treatment of bile duct loss after liver transplantation. | journal = J Hepatobiliary Pancreat Surg | volume = 8 | issue = 4 | pages = 316-22 | month =  | year = 2001 | doi = 10.1007/s0053410080316 | PMID = 11521176 }}</ref>


===Microscopic===
Features:<ref name=pmid18242505>{{Cite journal  | last1 = Reau | first1 = NS. | last2 = Jensen | first2 = DM. | title = Vanishing bile duct syndrome. | journal = Clin Liver Dis | volume = 12 | issue = 1 | pages = 203-17, x | month = Feb | year = 2008 | doi = 10.1016/j.cld.2007.11.007 | PMID = 18242505 }}</ref>
*Loss of intrahepatitic bile ducts - '''key feature'''.
*Cholestasis.


==Primary sclerosing cholangitis==
Note:
*Abbreviated ''PSC''.
*May occur without fibrosis and inflammation; thus, can be easy to miss.
*Strongly associated with [[ulcerative colitis]]; 75-90% of PSC patients have [[inflammatory bowel disease]] (IBD).<ref name=emed_psc_over>Khurana V, Singh T. Primary sclerosing cholangitis. eMedicine.com. URL: [http://emedicine.medscape.com/article/187724-overview http://emedicine.medscape.com/article/187724-overview]. Accessed on: 29 November 2009.</ref>
*Risk for [[cholangiocarcinoma]].<ref name=pmid19668124>{{Cite journal  | last1 = Jesudian | first1 = AB. | last2 = Jacobson | first2 = IM. | title = Screening and diagnosis of cholangiocarcinoma in patients with primary sclerosing cholangitis. | journal = Rev Gastroenterol Disord | volume = 9 | issue = 2 | pages = E41-7 | month =  | year = 2009 | doi =  | PMID = 19668124 }}</ref>


===Diagnosis===
===IHC===
*Diagnosed radiologically.
*[[CK7]] -ve.
*Liver biopsy is rarely useful diagnostically<ref name=emed_psc>Khurana V, Singh T. Primary sclerosing cholangitis. eMedicine.com. URL: [http://emedicine.medscape.com/article/187724-diagnosis http://emedicine.medscape.com/article/187724-diagnosis]. Accessed on: 29 November 2009.</ref> - as the disease may be patchy.
**Marks bile ducts.
**The utility of the biopsy is staging.
==Hepatic Graft versus Host Disease (L-GVHD)==
[[File:3 579232643 sl 1.png| Hepatic graft versus host disease (L-GVHD)]]
[[File:3 579232643 sl 2.png| Hepatic graft versus host disease (L-GVHD)]]
[[File:3 579232643 sl 3.png| Hepatic graft versus host disease (L-GVHD)]]
[[File:3 579232643 sl 4.png| Hepatic graft versus host disease (L-GVHD)]]
[[File:3 579232643 sl 5.png| Hepatic graft versus host disease (L-GVHD)]]
[[File:3 579232643 sl 6.png| Hepatic graft versus host disease (L-GVHD)]]
[[File:3 579232643 sl 7.png| Hepatic graft versus host disease (L-GVHD)]]
<br>
Hepatic graft versus host disease (L-GVHD) in a 22 yo man who underwent bone marrow transplantation after developing ALL. A. Low power view shows brownish discoloration in triad, but is otherwise of little interest. B. Arterioles in triads were accompanied by bile ducts in only 30% of cases; this image shows an arteriole without a bile duct. Note the pigment and the accompanying macrophage/lymphocyte inflammation, not extreme. The added chronic inflammation is a feature of chronic L-GVHD. C. Bile ducts, when shown, showed extensive damage, here seen as loss of cytoplasm,  and nuclear pleomorphism and hyperchromasia (other degenerative changes, not seen here, include nuclear dropout or necrosis, cytoplasmic eosinophilia, loss of duct lumen). Lymphocytosis into the ducts was not seen. D. Ballooned hepatocytes and dilated canaliculi were seen. E. Pigment was present, but mostly in Kupffer cells, not hepatocytes or as bile plugs. F. Up to two foci of spotty necrosis were seen in a 100X field (field shown is 200X); not shown are rare apoptotic hepatocytes. G. An iron stain showed the pigment represented extemsive iron deposition, with emphasis on Kupffer cells and portal triad macrophages, frustrating definite assessment of bile plugs in canaliculi. The hemosiderosis resulted from the many blood transfusions the patient had received.


===Treatment===
==Extrahepatic biliary obstruction==
*None very good.
A. [[File:1 OBS 3 680x512px.tif|Sinusoidal dilatation, circular spaces of hepatocytes, small portal triads(40X).]]
*May be indication for transplant.
<br>
B. [[File:2 OBS 3 680x512px.tif|Bile in hepatocytes about central vein & in plugs in canaliculi [yellow arrowhead] (400X).]]
<br>
C. [[File:3 OBS 3 680x512px.tif|Trichrome shows fibrosis about central vein (400X).]]
<br>
D. [[File:4 OBS 3 680x512px.tif|PAS with diastase shows portal triads with mild edema and chronic inflammation, without tortuous bile duct (400X).]]
<br>
Early extrahepatic biliary obstruction, demonstrated radiographically, transient, with rise in bilirubin, alkaline phosphatase, and transaminases. Pure canalicular cholestasis near terminal hepatic venules also seen in acute hepatitis, drug reactions, benign recurrent cholestasis, pregnancy, sepsis, & lymphomas. A. Sinusoidal dilatation, circular spaces of hepatocytes, small portal triads. B. Bile in hepatocytes about central vein & in plugs in canaliculi [yellow arrowhead]. C. Trichrome shows fibrosis about central vein. D. PAS with diastase shows portal triads with mild edema and chronic inflammation, without tortuous bile duct.
<br>
A. [[File:1 OBS 2 680x512px.tif|Expanded inflamed portal triads, swollen hepatocytes (40X)]]
<br>
B. [[File:2 OBS 2 680x512px.tif|Edematous stroma, proliferating ductules [yellow arrowheads], PAS-D macrophages [red arrowhead] (PAS with diastasse, 200X)]]
<br>
C. [[File:3 OBS 2 680x512px.tif|Disordered, often swollen hepatocytes,some with feathery degeneration (net like spaces in cytoplasm [blue arrowhead], rare Councilman body [green arrowhead] (400X)]]
<br>
D. [[File:4 OBS 2 1360x1024px.tif|Bile in hepatocytes [cyan arrrowhead] & in canaliculi [purple arrowheads]. Empty acinar spaces bounded by hepatocytes [orange arrowhead] (400X, higher pixel),]]
<br>
Changes of extrahepatic biliary obstruction, months duration. A. Expanded inflamed portal triads, swollen hepatocytes. B. Edematous stroma, proliferating ductules [yellow arrowheads], PAS-D macrophages [red arrowhead]. C. Disordered, often swollen hepatocytes,some with feathery degeneration (net like spaces in cytoplasm)  [blue arrowhead], rare Councilman body [green arrowhead]. D. Bile in hepatocytes [cyan arrrowhead] & in canaliculi [purple arrowheads]. Empty acinar spaces bounded by hepatocytes [orange arrowhead].
<br>
A. [[File:1 Bd obs 4 680x512px.tif|Expanded, light colored portal triads (arrows)(20X).]]
<br>
B. [[File:2 Bd obs 4 680x512px.tif|Proliferating bile ductules (cyan arrows) with neutrophils (yellow arrows), not specific for acute cholangitis, of assistance with large bile duct obstruction (400X)..]]
<br>
C. [[File:3 Bd obs 4 680x512px.tif|Uninflamed interlobular duct (yellow arrow) with, accompanying blood vessel (red arrow) (400X)]]
<br>
D. [[File:4 Bd obs 4 680x512px.tif|Bile infarct with pyknotic nuclei (arrows)(400X).]]
<br>
E. [[File:5 Bd obs 4 680x512px.tif|Bile (arrow) in interlobular bile duct with disordered nuclei (400X).]]
<br>
F. [[File:6 Bd obs 4 680x512px.tif|Bile plugs in cannaliculi (red arrows), feathery degeneration producing foamy macrophage like hepatocytes (yellow arrows)(400X).]]
<br>
Large bile duct obstruction. A. Expanded, light colored portal triads (arrows). B. Proliferating bile ductules (cyan arrows) with neutrophils (yellow arrows), not specific for acute cholangitis, of assistance with large bile duct obstruction. C. Uninflamed interlobular duct (yellow arrow) with, accompanying blood vessel (red arrow). D. Bile infarct with pyknotic nuclei (arrows). E. Bile (arrow) in interlobular bile duct with disordered nuclei. F. Bile plugs in cannaliculi (red arrows), feathery degeneration producing foamy macrophage-like hepatocytes (yellow arrows).


===Histopathology===
==Congestive hepatopathy==
*Classic: "onion-skinning" - cells layer around the bile ducts; "onion skin" present in approx. 40% of cases.<ref name=medscape_psc>Steele et al. URL: [http://www.medscape.com/viewarticle/552500_6 http://www.medscape.com/viewarticle/552500_6]. Accessed on: 29 November 2009.</ref>
{{Main|Congestive hepatopathy}}
**Not pathognomonic for PSC<ref name=medscape_psc/> - but not too much else looks like this on microscopy (ergo good fellowship exam question).
*+/-Ductopenia.
*+/-Ductal proliferation.


DDx:
==Drug-induced liver disease==
*Big.
*[[AKA]] ''drug-induced liver toxicity''.
{{Main|Drug-induced liver disease}}


Micrographs:
==Focal nodular hyperplasia==
*[http://www.pathconsultddx.com/pathCon/largeImage?pii=S1559-8675%2806%2970838-5&figureId=fig1 Onion-skinning (pathconsultddx.com)]
*Abbreviated ''FNH''.
{{Main|Focal nodular hyperplasia}}


====Staging====
==Nodular regenerative hyperplasia==
Features:<ref>Steele et al. URL: [http://www.medscape.com/viewarticle/552500_6 http://www.medscape.com/viewarticle/552500_6]. Accessed on: 29 November 2009.</ref>
===General===
*Stage I - focal portal inflammation, +/- duct abnormalities, no fibrosis.
*Associated with renal transplants, [[bone marrow transplant]]s and [[vasculitides]].<ref name=Ref_PBoD922>{{Ref PBoD|922}}</ref>
*Stage II - portal enlargement (fibrosis), +/- inflammation.
*Can lead to [[portal hypertension]] and many of the associated complications.<ref name=pmid22554152>{{Cite journal  | last1 = Bissonnette | first1 = J. | last2 = Généreux | first2 = A. | last3 = Côté | first3 = J. | last4 = Nguyen | first4 = B. | last5 = Perreault | first5 = P. | last6 = Bouchard | first6 = L. | last7 = Pomier-Layrargues | first7 = G. | title = Hepatic hemodynamics in 24 patients with nodular regenerative hyperplasia and symptomatic portal hypertension. | journal = J Gastroenterol Hepatol | volume = 27 | issue = 8 | pages = 1336-40 | month = Aug | year = 2012 | doi = 10.1111/j.1440-1746.2012.07168.x | PMID = 22554152 }}
*Stage III - bridging fibrosis + necrosis.
</ref>
*Stage IV - cirrhosis.


Notes:
====Etiology====
*Similar to PBC staging.
*Arterial hypervascularity secondary to loss of hepatic vein radicles (loss of central venule in hepatic lobule).<ref name=Ref_PBoD922>{{Ref PBoD|922}}</ref>


==Hereditary hemochromatosis==
ASIDE: radicle = ramulus - smallest branch or vessel or nerve.<ref name=Dorlands2>Dorland's Medical Dictionary. 30th Ed.</ref>
===Epidemiology/General===
*Genetic defect.  
**One mutation (C282Y mutation) in up to 12.5% of people in populations of northern and central European origin<ref name=pmid18192769>{{cite journal |author=Weinberg ED |title=Survival advantage of the hemochromatosis C282Y mutation |journal=Perspect. Biol. Med. |volume=51 |issue=1 |pages=98-102 |year=2008 |pmid=18192769 |doi=10.1353/pbm.2008.0001 |url=}}</ref>
*Onset in males earlier than females (due to menses).
*Mutation thought to confer survival advantage - several theories (increased resistance to TB, S. typhi vs. decr. iron def./incr. iron absorption)<ref name=pmid18192769/>


===Pathophysiology===
===Gross===
*Iron overload --> cirrhosis. (???)
*Diffuse nodularity - whole liver.


===Histopathology===
===Microscopic===
*Periportal changes (early), i.e. no iron centrilobular.
Features:<ref name=Ref_PBoD922>{{Ref PBoD|922}}</ref>
**Late stage disease has diffuse iron deposition.
*"Plump" hepatocytes surrounded by atrophic ones.
*Brown granular -- may look like [[lipofuscin]] on [[H&E]].
*No fibrosis.


Diagnosis suggested by positive ''iron stain''.  
==Sinuosoidal obstruction syndrome==
*Light blue haze is not enough.
*May be referred to as ''Hepatic veno-occlusive disease''.<ref name=pmid11928077>{{Cite journal  | last1 = DeLeve | first1 = LD. | last2 = Shulman | first2 = HM. | last3 = McDonald | first3 = GB. | title = Toxic injury to hepatic sinusoids: sinusoidal obstruction syndrome (veno-occlusive disease). | journal = Semin Liver Dis | volume = 22 | issue = 1 | pages = 27-42 | month = Feb | year = 2002 | doi = 10.1055/s-2002-23204 | PMID = 11928077 }}.</ref>
**NOT siderosis -- in Kupffer cells.
===General===
*Term for obstruction due to toxicity from a chemotherapeutic agent.<ref name=pmid16393276>{{Cite journal  | last1 = Helmy | first1 = A. | title = Review article: updates in the pathogenesis and therapy of hepatic sinusoidal obstruction syndrome. | journal = Aliment Pharmacol Ther | volume = 23 | issue = 1 | pages = 11-25 | month = Jan | year = 2006 | doi = 10.1111/j.1365-2036.2006.02742.x | PMID = 16393276 }}</ref><ref name=pmid17569137>{{Cite journal  | last1 = Aydinli | first1 = M. | last2 = Bayraktar | first2 = Y. | title = Budd-Chiari syndrome: etiology, pathogenesis and diagnosis. | journal = World J Gastroenterol | volume = 13 | issue = 19 | pages = 2693-6 | month = May | year = 2007 | doi =  | PMID = 17569137 | url=http://www.wjgnet.com/1007-9327/full/v13/i19/2693.htm }}</ref>


Notes:  
Clinical DDx:
*Iron in the bile ducts and endothelium used to be though specific of hereditary hemochromatosis.<ref>MG. 17 September 2009.</ref>
*[[Budd-Chiari syndrome]].
**It is now thought to just reflect the severity of iron deposition, i.e. if the bile ducts and endothelium have iron - it is severe.


===DDx===
===Microscopic===
*Myelodysplastic syndrome.
Features:<ref name=pmid17569137>{{Cite journal  | last1 = Aydinli | first1 = M. | last2 = Bayraktar | first2 = Y. | title = Budd-Chiari syndrome: etiology, pathogenesis and diagnosis. | journal = World J Gastroenterol | volume = 13 | issue = 19 | pages = 2693-6 | month = May | year = 2007 | doi =  | PMID = 17569137 | url=http://www.wjgnet.com/1007-9327/full/v13/i19/2693.htm }}</ref>
*Chronic hemolysis.
*Subendothelial swelling in hepatic venules.
*Alcohol.


==Wilson's disease==
Negatives:
===Epidemiology===
*No thrombosis.
*Rare autosomal recessive - mutation in copper-transporting adenosine triphosphatase (ATPase) gene (ATP7B).<ref name=emedicine183456>[http://emedicine.medscape.com/article/183456-overview http://emedicine.medscape.com/article/183456-overview]</ref>
**Heterozygote carrier rate approximately 1/100 persons.<ref name=emedicine183456/>
*Young individuals - usually 12-23 years old.


===Clinical===
==Ascending Cholangitis (Acute Cholangitis)==
*Kayser-Fleischer rings --> on slit-lamp examination (green eyes).
===General===
*May present to psychiatry or appear to be abusing EtOH.
*Term for infection of bile ducts, usually due to obstruction
*Serum ceruloplasmin - lower than normal.


===Etiology===
Clinical DDx:
*Excess copper -- due to genetic defect.


===Histopathology===
*Nothing specific.
*Steatosis.
*Portal fibrosis.


Staining:
===Microscopic===
*Copper staining positive in ONLY 15%.
====Images====
**Other stains: rhodinine, orecin.


A. [[File:1 asc chol 1 680x512px.tif|Rounded, clear (edematous) portal tracts (arrows) separated by hepatocytes with dilated sinusoids (Row 1 Left 40X).]]
<br>
B. [[File:2 asc chol 1 680x512px.tif|Neutrophils about hepatocytes (arrows) have spilled into the lobule from a portal tract (Row 1 Right 200X).]]
<br>
C. [[File:3 asc chol 1 680x512px.tif|Proliferated bile ductules (arrows) bearing neutrophils within epithelium and lumens are features of obstruction that should prompt a search for interlobular ducts with acute inflammation (Row 2 Left 400X).]]
<br>
D. [[File:4 asc chol 1 680x512px.tif|The epithelium of the ducts can be severely degenerated. Neutrophils (cyan arrows) invade epithelium of an interlobular duct that are recognizable mainly as a circle of rounded nuclei; the associated arteriole (red arrow) should be identified to ensure an interlobular duct is being evaluated. Note the proliferated bile ductules (blue arrows)  (Row 2 Right 400X).]]
<br>
E. [[File:5 asc chol 1 680x512px.tif|A PAS without diastase stain colors the arteriole (blue arrow), as well as the rim of the interlobular duct within which lies a neutrophil (cyan arrow) (Row 2 Right 400X). .]]
<br>
F. [[File:6 asc chol 1 680x512px.tif|A PAS with diastase stain colors the arteriole (red arrow), as well as the rim of the interlobular duct within which lies a neutrophil (cyan arrow) (Row 1 Right 400X)]]
<br>
Acute cholangitis in a patient with multiple bile duct procedures. After the biopsy, removal of bile duct stones released pus. A. Rounded, clear (edematous) portal tracts (arrows) separated by hepatocytes with dilated sinusoids. B. Neutrophils about hepatocytes (arrows) have spilled into the lobule from a portal tract. C, Proliferated bile ductules (arrows) bearing neutrophils within epithelium and lumens are features of obstruction that should prompt a search for interlobular ducts with acute inflammation. D. The epithelium of the ducts can be severely degenerated. Neutrophils (cyan arrows) invade epithelium of an interlobular duct that are recognizable mainly as a circle of rounded nuclei; the associated arteriole (red arrow) should be identified to ensure an interlobular duct is being evaluated. Note the proliferated bile ductules (blue arrows). E. A PAS without diastase stain colors the arteriole (blue arrow), as well as the rim of the interlobular duct within which lies a neutrophil (cyan arrow). F. A PAS with diastase stain colors the arteriole (red arrow), as well as the rim of the interlobular duct within which lies a neutrophil (cyan arrow).


==Alpha-1 antitrypsin deficiency==
A.[[File:1 Sep Acu Cho 1 680x512px.tif|Low power shows variably sized inflamed portal tracts (40X)]]
*AKA 'alpha1-antiprotease inhibitor deficiency'.
<br>
B. [[File:2 Sep Acu Cho 1 680x512px.tif|Trichrome shows dilated sinusoids and space of Disse collagenization (200X)]]
<br>
C. [[File:3 Sep Acu Cho 1 680x512px.tif|Inflammatory focus with macrophages and neutrophils (400X).]]
<br>
D. [[File:4 Sep Acu Cho 1 680x512px.tif|PAS with diastase shows proliferated bile ductules at edge of triad with neutrophils, which should not be used to make a definite diagnosis of acute cholangitis (400X).]]
<br>
E. [[File:5 Sep Acu Cho 1 680x512px.tif|PAS without diastase showing acutely inflamed bile duct, with accompanying blood vessel of similar size, diagnostic of acute cholangitis (400X).]]
<br>
F. [[File:6 Sep Acu Cho 1 680x512px.tif|PAS with diastase showing neutrophil in bille duct lumen, diagnostic of acute cholangitis (400X).]]
<br>
Patient with sepsis and acute cholangitis. A. Low power shows variably sized inflamed portal tracts. B. Trichrome shows dilated sinusoids and space of Disse collagenization. C. Inflammatory focus with macrophages and neutrophils. D. PAS with diastase shows proliferated bile ductules at edge of triad with neutrophils, which should not be used to make a definite diagnosis of acute cholangitis. E. PAS without diastase showing acutely inflamed bile duct, with accompanying blood vessel of similar size, diagnostic of acute cholangitis. F. PAS with diastase showing neutrophil in bille duct lumen, diagnostic of acute cholangitis.


===Etiology===
==Polycystic kidney disease and the liver==
*Genetic defect.
{{Main|Cystic kidney disease}}
===General===
Complications of PKD in the liver:<ref>{{Ref MacSween|174-5}}</ref>
#Infected cyst.
#Cholangiocarcinoma.
#Cholestasis/obstruction due to duct compression.<ref>URL: [http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pubmed&pubmedid=9184868 http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pubmed&pubmedid=9184868]. Accessed on: 23 September 2009.</ref>


===Causes===
Cysts:
*Lung and liver injury.
*Cysts in the liver, like the kidney, are thought to enlarge with age.
**Lung -> emphysema.


===Histopathology===
===Microscopic===
*Pink globules in zone 1.
Features:<ref>{{Ref MacSween|176}}</ref>
**Globules not seen in children.
*''Von Meyenburg complexes'' ([[bile duct hamartoma]]):
**May not be present in late stage (cirrhotic).
**Cluster of dilated ducts with "altered" bile.
**Best seen on PAS-diastase.
**Surrounded by collagenous stroma.
**Can be seen on H&E -- if one looks carefully.
**Separate from the portal areas.<ref>Meyenburg complex. Stedman's Medical Dictionary. 27th Ed.</reF>


Images:
*[http://commons.wikimedia.org/wiki/File:Von_Meyenburg_complex_low_mag.jpg Von Meyenburg complex - bile duct hamartoma (WC)].
*[http://commons.wikimedia.org/wiki/File:Bile_duct_hamartoma_intermed_mag.jpg Bile duct hamartoma (WC)].


==Drug toxicity==
Notes:
*Can do almost anything; may include: granulomata, bile duct injury, cholestasis, ischemic type injury.
*Appearance on ultrasound<ref name=pmid17287178>Bile duct hamartomas--the von Meyenburg complex. Salles VJ, Marotta A, Netto JM, Speranzini MB, Martins MR. Hepatobiliary Pancreat Dis Int. 2007 Feb;6(1):108-9. PMID 17287178.</ref> and CT (hypodense)<ref name=pmid19294869>[The von Meyenburg complex] Schwab SA, Bautz W, Uder M, Kuefner MA. Rontgenpraxis. 2008;56(6):241-4. German. PMID 19294869.</ref> - similar to metastases.
*Effects can be delayed -- temporal relationship not always obvious.


Microscopic:
==Peliosis hepatis==
*Non-specific findings.
{{Main|Peliosis hepatis}}
**+/-Eosinophils.<ref>DCHH P.166.</ref>
**+/-Steatosis - periportal macrovesicular, microvesicular.


===Common===
==Total parenteral nutrition==
Acute hepatits:
*Abbreviated ''TPN''.
*Related to Rx - most often antibiotics.


Acetaminophen:
===General===
*Zone 3 necrosis.
*Indication: short gut syndrome, others.


Methotrexate - chronic use:
===Microscopic===
*Histology:<ref>MacSween 5th Ed. P.715.</ref>
Variable - may range from: steatosis, steatohepatitis, cholestasis, fibrosis and cirrhosis.<ref name=pmid16766237>{{cite journal |author=Guglielmi FW, Boggio-Bertinet D, Federico A, ''et al.'' |title=Total parenteral nutrition-related gastroenterological complications |journal=Dig Liver Dis |volume=38 |issue=9 |pages=623–42 |year=2006 |month=September |pmid=16766237 |doi=10.1016/j.dld.2006.04.002 |url=}}</ref>
**Features of steatohepatitis.
***Zone III steatosis.
***Ballooning degeneration.
**Portal inflammation with mixed population (lymphocytes, macrophages, PMNs).
**Nuclear atypia (hyperchromasia, pleomorphism, vacuolation).
***Described as just nuclear size variation by some.<ref>MG. 23 September 2009.</ref>


==Focal nodular hyperplasia==
Features (classic):<ref>{{Cite journal  | last1 = Li | first1 = SJ. | last2 = Nussbaum | first2 = MS. | last3 = McFadden | first3 = DW. | last4 = Gapen | first4 = CL. | last5 = Dayal | first5 = R. | last6 = Fischer | first6 = JE. | title = Addition of glucagon to total parenteral nutrition (TPN) prevents hepatic steatosis in rats. | journal = Surgery | volume = 104 | issue = 2 | pages = 350-7 | month = Aug | year = 1988 | doi =  | PMID = 3135627 }}</ref><ref>{{Cite journal  | last1 = Stanko | first1 = RT. | last2 = Nathan | first2 = G. | last3 = Mendelow | first3 = H. | last4 = Adibi | first4 = SA. | title = Development of hepatic cholestasis and fibrosis in patients with massive loss of intestine supported by prolonged parenteral nutrition. | journal = Gastroenterology | volume = 92 | issue = 1 | pages = 197-202 | month = Jan | year = 1987 | doi =  | PMID = 3096806 }}
*Abbreviated ''FNH''.
</ref>
*Not commonly seen by pathologists.
*[[Steatosis]] (periportal) - early.
*Benign lesions.
*Cholestasis - late.
*Associated with oral contraceptive pill (OCP) use.


===Imaging===
==Giant cell hepatitis==
*FNH enhances on the arterial phase in triphasic imaging, i.e. triphasic CT or MRI.<ref name=emedicine_fnh>[http://emedicine.medscape.com/article/368377-overview http://emedicine.medscape.com/article/368377-overview]</ref>
*[[AKA]] ''neonatal giant cell hepatitis''.


===Gross===
:See: ''[[Giant cell hepatitis]]''.
Features:<ref>PBoD P.922.</ref>
*Well circumscribed, but no capsule.
*Lighter than surrounding parenchyma, may be yellow.
*+/-Stellate central scar with thick vessels.


Note: Usually a solitary lesion.<ref name=emedicine_fnh/>
==Hepatic amyloidosis==
===Histopathology===
{{Main|Amyloidosis}}
Features:<ref>PBoD P.922.</ref>
*[[AKA]] ''liver amyloidosis''.
*Stellate scar has large arteries with fibromuscular hyperplasia.
*[[AKA]] ''amyloidosis of the liver''.
**Thin fibrous septa radiate from the central scar - surrounded by lymphocytes & bile ductules.
===General===
***Normal hepatocytes between fibrous septae.
*Diffuse abundant amyloid within the space of Disse is associated with [[portal hypertension]].<ref name=pmid1864548>{{Cite journal  | last1 = Bion | first1 = E. | last2 = Brenard | first2 = R. | last3 = Pariente | first3 = EA. | last4 = Lebrec | first4 = D. | last5 = Degott | first5 = C. | last6 = Maitre | first6 = F. | last7 = Benhamou | first7 = JP. | title = Sinusoidal portal hypertension in hepatic amyloidosis. | journal = Gut | volume = 32 | issue = 2 | pages = 227-30 | month = Feb | year = 1991 | doi = | PMID = 1864548 | PMC = 1378815 | URL = http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1378815/?tool=pubmed }}</ref>


===DDx===
===Microscopic===
*May be difficult to distinguish from hepatic adenoma if no scar and no ductal proliferation.<ref>STC. 19 Jan 2009.</ref>
Features:
*Amorphous extracellular pink stuff on H&E - see ''[[amyloid]]'' article.


DDx:
*[[Fibrolamellar hepatocellular carcinoma]].


==Nodular regenerative hyperplasia==
====Images====
*Associated with renal transplants, bone marrow transplants and vasculitities.<ref>PBoD P.922.</ref>
<gallery>
*Can lead to portal hypertension and many of the associated complications.
Image:Hepatic_amyloidosis_-_low_mag.jpg | Amyloidosis of the liver - low mag. (WC)
Image:Hepatic_amyloidosis_-_intermed_mag.jpg | Amyloidosis of the liver - intermed. mag. (WC)
Image:Hepatic_amyloidosis_-_high_mag.jpg | Amyloidosis of the liver - high mag. (WC)
Image:Hepatic_amyloidosis_-_very_high_mag.jpg | Amyloidosis of the liver - very high mag. (WC)
</gallery>
A. [[File:1 AMY 1 680x512px.tif|Amorphous material replaces hepatic parenchyma [4X]]]
<br>
B. [[File:2 AMY 1 680x512px.tif|Material barely stains blue on trichrome [10X]]]
<br>
C. [[File:3 AMY 1 680x512px.tif|Material stains red on unpolarized Congo Red [40X]]]
<br>
D. [[File:4 AMY 1 680x512px.tif|Material stains apple green on polarized Congo Red [40X]]]
<br>
Amyloidosis. A. Amorphous material replaces hepatic parenchyma. B. Material barely stains blue on trichrome. C. Material stains red on unpolarized Congo Red. D. Material stains apple green on polarized Congo Red.


===Etiology===
===Stains===
*Arterial hypervascularity secondary to loss of hepatic vein radicles (loss of central venule in hepatic lobule).<ref>PBoD P.922.</ref>
*[[Congo red]] +ve.


ASIDE: radicle = ramulus - smallest branch or vessel or nerve.<ref>Dorlands2</ref>
==Fulminant hepatic necrosis==
===Gross===
{{Main|Fulminant hepatic necrosis}}
*Diffuse nodularity - whole liver.


===Histopathology===
==Secondary hemochromatosis==
Features:<ref>PBoD P.922.</ref>
:''For the hereditary one see [[hereditary hemochromatosis]]''.
*"Plump" hepatocytes surrounded by atrophic ones.
===General===
*No fibrosis.
*Iron overload secondary to blood transfusions for hereditary or acquired anemia.<ref name=pmid19727383/>
**Primary hemochromatosis due to a defect in iron processing - called ''[[hereditary hemochromatosis]]''.
*Imaging considered the best test, as iron deposition is patchy.<ref name=pmid19727383/>


Selected hereditary causes:<ref name=pmid19727383>{{Cite journal  | last1 = Gattermann | first1 = N. | title = The treatment of secondary hemochromatosis. | journal = Dtsch Arztebl Int | volume = 106 | issue = 30 | pages = 499-504, I | month = Jul | year = 2009 | doi = 10.3238/arztebl.2009.0499 | PMID = 19727383 | PMC = 2735704 | URL = http://www.ncbi.nlm.nih.gov.myaccess.library.utoronto.ca/pmc/articles/PMC2735704/?tool=pubmed}}</ref>
*Thalassemia.
*[[Sickle cell anemia]].
*Hereditary sideroblastic anemia.


==Sinuosoidal obstruction syndrome==
Selected acquired causes:<ref name=pmid19727383/>
*Term for obstruction due to toxicity from a chemotherapeutic agent.<ref name=pmid16393276>Review article: updates in the pathogenesis and therapy of hepatic sinusoidal obstruction syndrome. Helmy A. Aliment Pharmacol Ther. 2006 Jan 1;23(1):11-25. Review. PMID 16393276.</ref>
*[[Myelodysplastic syndromes]]
*May be referred to as ''Hepatic veno-occlusive disease''.<ref name=pmid11928077>Toxic injury to hepatic sinusoids: sinusoidal obstruction syndrome (veno-occlusive disease). DeLeve LD, Shulman HM, McDonald GB.
*Myelofibrosis
Semin Liver Dis. 2002 Feb;22(1):27-42. Review. PMID 11928077.</ref>
*Aplastic anemia, intractable.


==Polycystic kidney disease and the liver==
===Microscopic===
Complications of PKD in the liver:<ref>MacSween 5th Ed. PP. 174-5.</ref>
:See ''[[hereditary hemochromatosis]]''.
#Infected cyst.
#Cholangiocarcinoma.
#Cholestasis/obstruction due to duct compression.<ref>URL: [http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pubmed&pubmedid=9184868 http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pubmed&pubmedid=9184868]. Accessed on: 23 September 2009.</ref>


Cysts:
==Hepatic sarcoidosis==
*Cysts in the liver, like the kidney, are thought to enlarge with age.
{{Main|Hepatic sarcoidosis}}
==Overlapping Disorders==


===Microscopic===
[[File:1 Mixed Disorder 1 680x512px.tif|Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed.]]
Features:<ref>MacSween 5th Ed. P.176.</ref>
[[File:2 Mixed Disorder 1 680x512px.tif|Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed.]]
*''Von Meyenburg complexes'' (bile duct hamartoma):
[[File:3 Mixed Disorder 1 680x512px.tif|Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed.]]
**Cluster of dilated ducts with "altered" bile.
[[File:4 Mixed Disorder 1 680x512px.tif|Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed.]]
**Surrounded by collagenous stroma.
[[File:5 Mixed Disorder 1 680x512px.tif|Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed.]]
**Separate from the portal areas.<ref>Meyenburg complex. Stedman's Medical Dictionary. 27th Ed.</reF>
[[File:6 Mixed Disorder 1 680x512px.tif|Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed.]]<br>
Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed. A. Low power shows hepatocytes afflicted by steatosis and an inflamed portal tract. B. In a region of fatty change lie cytoplasmic tufts of ballooning degeneration (green arrows) and a lipogranuloma (black arrow). C. At the portal-hepatocyte junction lies interface hepatitis (black arrows), as well as extension of inflammation into the lobule (green arrows). D. Red hepatocytes bounded by inflammation denote piecemeal necrosis [PAS without diastase]. E. Giant cells intermixed with lymphocytes prove a portal granuloma [PAS without diastase]. F. A blue fibrous bridge extends from a triad [Trichrome].


Images:
[[File:4 95599552608917 sl 1.png|Acute obstructive changes and changes of recurrent acute injury]]
*[http://commons.wikimedia.org/wiki/File:Von_Meyenburg_complex_low_mag.jpg Von Meyenburg complex - bile duct hamartoma (WC)].
[[File:4 95599552608917 sl 2.png|Acute obstructive changes and changes of recurrent acute injury]]
*[http://commons.wikimedia.org/wiki/File:Bile_duct_hamartoma_intermed_mag.jpg Bile duct hamartoma (WC)].
[[File:4 95599552608917 sl 3.png|Acute obstructive changes and changes of recurrent acute injury]]
[[File:4 95599552608917 sl 4.png|Acute obstructive changes and changes of recurrent acute injury]]
[[File:4 95599552608917 sl 5.png|Acute obstructive changes and changes of recurrent acute injury]]
[[File:4 95599552608917 sl 6.png|Acute obstructive changes and changes of recurrent acute injury]]
[[File:4 95599552608917 sl 7.png|Acute obstructive changes and changes of recurrent acute injury]]<br>
Acute obstructive changes and changes of recurrent injury in 46 yo man with Clostridium perfringens positive blood culture, an ERCP that showed duodenal compression by the pancreas with resultant bile duct dilatation. The patient had had and continued to have multiple bouts of acute pancreatitis. At the time of biopsy,  decreased platelet count/hemoglobin/albumin, elevated lipase/amylase/PT/PTT, normal alkaline phosphatase, bilirubin, AST/ALT, AMA, hepatitis virus serology, ANA. A. Fragment biopsy shows inflamed triads and bridges. B. Trichrome shows bridges without nodules, evidence of prior injury; the patient subsequently developed multiple episodes of pancreatitis. C. Reticulin shows piecemeal necrosis, with black lines bounding individual hepatocytes at interface (arrows). D. Collapse is shown by closly approximated thick black lines; one cannot call portal-central collapse without seeing a central vein. Note on this and the other reticulin image that regeneration, two cell thick cords, is not prominent. E. PAS D of two portal triads, far nearer than normal, both expanded. Note increased number of ducts/ductules (red arrows), neutrophils, and PAS-D macrophages. F. PAS D shows collapse extending from a triad to a portion of a lobule with steatosis. No feathery degeneration or bile duct plugs were seen. Neither were foci of spotty necrosis or abscess seen. G. Other triads, again edematous, showed more of a chronic inflammatory response, with occasional plasma cells (black arrows). Also present are neutrophils (red arrows). The bile duct (grey arrow)  near the artery (brown arrow) shows mildly disturbed nuclei. Note early proliferated bile ductules (cyan arrows).


Notes:
[[File:6 17281676469188 sl 1.png| Hepatitis B virus with steatohepatitis]]
*Appearance on ultrasound<ref name=pmid17287178>Bile duct hamartomas--the von Meyenburg complex. Salles VJ, Marotta A, Netto JM, Speranzini MB, Martins MR. Hepatobiliary Pancreat Dis Int. 2007 Feb;6(1):108-9. PMID 17287178.</ref> and CT (hypodense)<ref name=pmid19294869>[The von Meyenburg complex] Schwab SA, Bautz W, Uder M, Kuefner MA. Rontgenpraxis. 2008;56(6):241-4. German. PMID 19294869.</ref> - similar to metastases.
[[File:6 17281676469188 sl 2.png| Hepatitis B virus with steatohepatitis]]
[[File:6 17281676469188 sl 3.png| Hepatitis B virus with steatohepatitis]]
[[File:6 17281676469188 sl 4.png| Hepatitis B virus with steatohepatitis]]
[[File:6 17281676469188 sl 5.png| Hepatitis B virus with steatohepatitis]]
[[File:6 17281676469188 sl 6.png| Hepatitis B virus with steatohepatitis]]<br>
Hepatitis B virus with steatohepatitis in a 36 year old man with hepatitis B surface antigen and hepatitis Be antigen positivity, Hepatitis be QTPC of 1750 cop/mL, an occasionally mildly elevated (42) ALT, and  normal glucose, alkaline phosphatase, bilirubin, and other transaminases. He had a history of alcohol abuse, which became controlled.  A. Triads show scant inflammation without definite interface hepatitis. About one-fourth of the lobule, not pan-acinar, is afflicted by steatosis. B. Occasional tufts are seen (arrow), indicating focal ballooning sufficient for a diagnosis of steatohepatitis. C. Glycogenated nuclei (black arrows) and hepatocytes with feathery degeneration (red arrows) are seen.  D. Very rare foci of spotty necrosis were seen. E. Apart from this triad and the one in the trichrome stain in F, which had moderate inflammation comprising lymphocytes and macrophages, all triads were small, most without any inflammation at all. Neither collapse nor piecemeal necrosis were seen on reticulin stain. F. Trichrome stain showed only portal fibrosis. The interhepatocyte fibrosis required for brunt fibrosis stage I was not seen. Hence, one would grade this as follows: A) Chronic hepatitis (history of hepatitis B), Metavir activity index 1, Piecemeal necrosis 0, Lobular necrosis 1, Metavir fibrosis stage 1, B) Steatohepaitits, Brunt necroinflammatory grade 1, Brunt fibrosis stage 0.


==See also==
=See also=
*[[Pancreas]].
*[[Pancreas]].
*[[Gastrointestinal pathology]].
*[[Gastrointestinal pathology]].
Line 433: Line 715:
*[[Liver]].
*[[Liver]].


==References==
=References=
{{reflist|2}}
{{reflist|2}}


[[Category:Gastrointestinal pathology]]
[[Category:Gastrointestinal pathology]]
[[Category:Liver pathology]]
[[Category:Liver pathology]]
[[Category:Medical liver disease]]

Latest revision as of 14:45, 18 June 2017

Micrograph showing ground glass hepatocytes, as seen in chronic hepatitis B. H&E stain.

This article deals with medical liver disease. An introduction to the liver and approach is found in the liver article.

Every differential in liver pathology has "drugs"[1] -- if it isn't clearly malignancy.

Liver neoplasms are dealt with in the liver neoplasms article.

Medical liver biopsies are often non-specific, as the liver has the same appearance for many mechanisms of injury, especially when the injury is marked. The clinical history, serology and imaging are essential for proper interpretations in this domain of pathology.

Review of liver blood work

Inflammation activity

  • ALT.
  • AST.

Cholestatic markers

  • ALP.
  • GGT - used to assess whether the ALP is an "honest" value, elevated in cirrhosis.

Cirrhosis/decompensation

  • PLT - low is suggestive of dysfunction.
  • INR - high is bad, unless anticoagulated.

Other

  • Bilirubin.
    • Direct (AKA conjugated).
    • Indirect (AKA unconjugated).

A short DDx of elevated:[2]

  • Indirect:
    • Gilbert syndrome.
    • Crigler-Najjar syndrome type 1.
    • Crigler-Najjar syndrome type 2.
  • Direct:
    • Rotor syndrome.
    • Dubin-Johnson syndomre.

Viral hepatitis

  • HBV DNA.
  • HCV RNA.
  • HBs Ag, HBs Ab, HBe Ag, HBe Ab.
  • HCV Ab.

Others:

Hepatitis B

Meaning & utility of the various Hepatitis B tests:[3][4]

Test name Location Positive test Negative test Usual question
HBs Ag Surface Virus active No active infection Active infection?
HBs Ab Surface Exposed OR vaccinated No exposure OR no vaccine OR loss of Ab Immunization status?
HBe Ag Virus core Infect. w/ viral replication No active infection Active infect. w/ viral replication?
HBe Ab Virus core Exposed to virus Infect. w/o antibody response OR not exposed Immune response to infection?
HBV DNA - Active Not active/no exposure Viral load/how active?
HBc Ab Virus core Virus active/previous exposure No exposure Early active infection?

Notes:

  • HBc Ab may test for acute (IgM) or chronic infection - dependent on specific antibody test; it is often used to look for early infection.[4]
  • Carriers of hepatitis B: HBs Ag +ve, HBs Ab -ve, HBc Ag -ve, HBc Ab +ve, HBe Ag -ve, HBe Ab +ve.[5]

Markers for rare liver diseases

  • Ceruloplasm - low think Wilson's disease; typical value for Wilson's ~ 0.12 g/L.
    • <0.20 g/L is a criteria for Wilson's disease.[6]
  • Alpha-1 antitrypsin - if low think deficiency.

Hemosiderosis

  • Ferritin - high.
  • Iron saturation - high.

Causes:

  • Hemochromatosis.
  • Hemolysis, chronic.
  • Cirrhosis.

Medical imaging

Blood flow:[7]

  • Hepatopedal flow = normal portal vein flow.
  • Hepatofugal flow = reversed portal vein flow.

Interventional measurements

Wedged to free hepatic venous pressure:[8]

Liver biopsy

Medical liver biopsy adequacy

Liver biopsy specimens should be:[9]

  • 2.0 cm in length and contain 11-15 portal tracts,
  • The core should be deeper than 1.0 cm from the liver capsule; specimens close to the capsule may lead to over grading of fibrosis.

Reporting

Specimen, procedure:
- Diagnosis.

The diagnosis usually contains grading and staging information, e.g. activity 2 /4, Laennec fibrosis stage 1 /4.

In the context of medical liver disease:

  • Grade = inflammation/activity.
  • Stage = severity of fibrosis/architectural changes.

Notes:

  • The term "acute" is infrequently used in liver pathology.
  • In the liver: neutrophils is not acute -- unlike most elsewhere in the body.[10]

A microscopic checklist

Size of biopsy: Adequate
Fragmentation: Absent
Fibrosis: Stage 2-3/4, mostly stage 2
Fibrous septa: Present
Septa with curved contours: Present – focally only
Large droplet steatosis (% of hepatocytes): Present, moderate 60%
Ballooning of hepatocytes: Present, rare
Mallory-Denk bodies: Present, rare
Portal inflammation: Present
Interface activity: Minimal (0-1/4)
Lobular necroinflammation: Minimal
Ducts: Present in normal numbers
Duct injury: Absent
Ductular reaction: Absent
Cholestasis: Absent
Terminal hepatic venules: Present
Iron stain: Absent
Ground glass cells with routine stains: Absent
PASD for alpha-1 antitrypsin droplets: Negative 

Viral hepatitis

These are common. The diagnoses are based on serology. The serology is covered in the viral hepatitis section in the liver pathology article.

Typically classified as:[11][12]

  1. Acute < 6 months duration.
  2. Chronic > 6 months duration.

Hepatitis A

  • Infection is self-limited, i.e. not persistent.
  • Usually asymptomatic in children.[13]
  • Serology is diagnostic.

Hepatitis B

Hepatitis B virus, abbreviated HBV, redirects here.

Hepatitis C

Other infections

  • Hydatid disease (Hydatid cyst).
  • Ascaris.
  • Fasciola

Hydatid disease

  • AKA hydatid cyst.

General

Microscopic

Features:

Images

www:

Abscess

A. A process replaces most of the liver parenchyma (20X).
B. Fibrinopurulent exudate apposes granulation tissue (200X).
C. Neutrophils lie in widened sinusoids (200X)..
D. Trichrome shows collagenization of spaces of Disse. Scarring about an abscess or other mass lesion should not be interpreted as reflective of the liver in general (200X).
Abscess. A. A process replaces most of the liver parenchyma. B. Fibrinopurulent exudate apposes granulation tissue. C. Neutrophils lie in widened sinusoids. D. Trichrome shows collagenization of spaces of Disse. Scarring about an abscess or other mass lesion should not be interpreted as reflective of the liver in general (LR 200X).

Coccidiomycosis

A. 500x500px Granulomas at low power
B. 500x500px Granulomas with centrally crowded cells & lady slipper macrophage nuclei
C. 500x500px Center of previous granuloma showing pyknotic macrophage nuclei
D. 500x500px Four Coccidiomycotic spherules
Coccidiomycosis. A. Note the granulomas in otherwise undisturbed liver (UL). B. Granuloma with centrally crowded cells & lady slipper macrophage nuclei. C. Center of granuloma with pyknotic macrophage nuclei, "necrotizing". D. Organisms on GMS stain.

Metabolic and toxic

Alcoholic liver disease

General

Classic lab findings in EtOH abusers

  • AST & ALT elevated with AST:ALT=2:1.
  • GGT elevated.
  • MCV increased.

Gross pathology/radiologic findings

  • Classically micronodular pattern.
    • May be macronodular.

Microscopic

See:

Features:

  • Often zone III damage.
  • Cholestatsis common, i.e. yellow staining.
    • NASH (non-alcoholic steatohepatitis) usu. does not have cholestasis.[17]
  • Fibrosis starts at central veins.
  • Neutrophils (often helpful) -- few other things have PMNs. (???)
    • Neutrophils cluster around cells with Mallory hyaline.

Images

A. Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).
B. Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).
C. Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).
D. Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).
E. Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).
F. Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis).

Alcoholic hepatitis with Metavir stage IV fibrosis (advanced fibrosis/cirrhosis). A. Trichrome shows relatively non-inflamed fibrous bands, as well as [between green dots] nodules. The lack of regeneration throughout might have precluded a diagnosis of cirrhosis, but stage IV fibrosis under the Metavir system is justified. B. Reticulin shows regenerative nodules [left] with mostly two or more nuclei between black lines juxtaposed to non-regenerative hepatocytes on the right, without piecemeal necrosis. C. Regenerative nodules show occasional neutrophils [red arrow] and cytoplasmic tufts of ballooned cells, sometimes possibly Mallory hyalin [green arrows]. D. Triads (note vein [green arrow], artery [yellow arrow], and interlobular bile duct [blue arrow]) generally showed little or no interface hepatitis, even when expanded by fibrosis and inflamed. E. Occasional foci of spotty necrosis were seen. F. This edge of an inflamed triads shows neutrophils about proliferated bile ducts [red arrows], as well as Mallory-Denk bodies [blue arrows].
A. Cirrhosis in an alcoholic.
B. Cirrhosis in an alcoholic.
C. Cirrhosis in an alcoholic.
D. Cirrhosis in an alcoholic.
E. Cirrhosis in an alcoholic.
F. Cirrhosis in an alcoholic.
Definite cirrhosis in an alcoholic. A. Hepatocyte free bands parse tissue, with occasional definite islands [arrows]. B. Trichrome establishes blue fibrosis about isles [arrows]. C. Reticulin stain shows nodules with regeneration, wherein a large proportion of them are at least two nuclei thick [arrows]. D. Bile duct proliferation can be difficult, sometimes mimicking cholangiocarcinoma. Follow the double headed arrows to see how the ductules can be seen to proliferate from a single sources, with all ducts being complete, without necrotic epithelial cells. E. PAS with distase can help, as cholangiocarcinoma generally lacks the red rim of proliferating bile ductules [arrows]; again note the connections that can be made between the ductule openings by the blue double headed arrows. The cyan double headed arrows show general parallelism, consistent with uniform directionality induced by extrinsic force, not a neoplastic spread. F. Trichrome shows the most difficult focus. Double headed arrows display the connectivity seen before of the proliferated bile ductules. Note that numerous pairs of adjacent perpendicular glands without a head to foot appearance are not seen that would indicate the disorderly spread of cholangiocarcinoma.
A. Expanded, inflamed triads with increased bile duct/vascular openings. Mild steatosis (40X).
B. Trichrome stain shows periportal fibrosis [red arrowheads] (200X).
C. PAS with diastase stain shows proliferated bile ductules [blue arrowheads] in stroma with mixed inflammatory infiltrate (400X)
D. Neutrophils about ballooned hepatocyte (satellitosis) [yellow arrowheads]. Councilman bodies [green arrowheads] (400X).
Alcoholic hepatitis without cirrhosis. No history of viral disease. AMA negative. A. Expanded, inflamed triads with increased bile duct/vascular openings. Mild steatosis. B. Trichrome stain shows periportal fibrosis [red arrowheads]. C. PAS with diastase stain shows proliferated bile ductules [blue arrowheads] in stroma with mixed inflammatory infiltrate. D. Neutrophils about ballooned hepatocyte (satellitosis) [yellow arrowheads]. Councilman bodies [green arrowheads].

Notes:

  • If portal inflammatory infiltrates more than mild, r/o other causes i.e. viral hepatitis.
  • Mallory bodies once thought to be characteristic; now considered non-specific and generally poorly understood.[18]
  • Some consider alcoholic liver disease a clinical diagnosis, i.e. as a pathologist one does not diagnose it.[19]

Non-alcoholic fatty liver disease

  • Abbreviated NAFLD.
  • Fatty liver that is not due to alcohol; includes obesity-related fatty liver, metabolic disease/diabetes-related fatty liver.

NASH

  • Non-alcoholic steatohepatitis - see steatohepatitis section.
  • Histologically indistinguishable from ASH.
  • NASH is a clinical diagnosis based on exclusion of alcohol.

Steatohepatitis

Autoimmune

Autoimmune hepatitis

  • Abbreviated AIH.

Primary biliary cirrhosis

  • Abbreviated PBC.

Autoimmune hepatitis with obstruction - combined changes

A. Low power shows inflammation; portal triads, lobules, central veins cannot be distinguished (40X).
B. Trichrome shows central venous sclerosis (red arrowhead), periportal fibrosis (green arrowhead), & space of Disse collagenization (yellow arrowhead); juxtaposition of central vein & portal tract indicates collapse, no definite bridging was seen (100X)
C. Central vein is inflamed with a rare plasma cell (cyan arrowhead) (400X).
D. Interface hepatitis with plasma cells (yellow arrows) and ballooned hepatocytes (red arrows). Lobule is disorganized (400X).
E. Proliferating bile ductules (blue arrows) with occasional neutrophils (fucsia arrows), indicative of obstruction, but not acute cholangitis, which requires inflamed bile duct itself, best diagnosed with associated blood vessel (400X).
F. Rare distorted rosettes with greenish brown strands of bile (left arrow) or bile plugs (right arrow) (400X).
Patient with SLE and obstructive jaundice that resolved with apparent passage of stone. A. Low power shows inflammation; portal triads, lobules, central veins cannot be distinguished. B. Trichrome shows central venous sclerosis (red arrowhead), periportal fibrosis (green arrowhead), & space of Disse collagenization (yellow arrowhead); juxtaposition of central vein & portal tract indicates collapse, no definite bridging was seen. C. Central vein is inflamed with a rare plasma cell (cyan arrowhead). D. Interface hepatitis with plasma cells (yellow arrows) and ballooned hepatocytes (red arrows). Lobule is disorganized. E. Proliferating bile ductules (blue arrows) with occasional neutrophils (fucsia arrows), indicative of obstruction, but not acute cholangitis, which requires inflamed bile duct itself, best diagnosed with associated blood vessel. F. Rare distorted rosettes with greenish brown strands of bile (left arrow) or bile plugs (right arrow).

Autoimmune hepatitis-primary biliary cirrhosis overlap syndrome

  • Abbreviation AIH-PBC OS.

General

Epidemiology:

  • Rare.

Serology:[20]

  • AMA +ve.
  • Anti-dsDNA +ve.

Microscopic

See: autoimmune hepatitis and primary biliary cirrhosis.

A. Expanded portal tracts with fuzzy edges (40X).
B. Interface hepatitis with plasma cells (400X).
C. Loose granuloma (400X).
D. Damaged bile duct (400X).
AIH/PBC overlap. AMA & ANA positive with Alkaline phosphatase > 2 upper limit of normal & one ALT > 5 times upper limit of normal. A. Expanded portal tracts with fuzzy edges. B. Interface hepatitis with plasma cells. C. Loose granuloma. D. Damaged bile duct.

Primary sclerosing cholangitis

  • Abbreviated PSC.

Hereditary

Caroli disease

General

Clinical:[23]

Note:

  • Caroli syndrome = Caroli disease + congenital hepatic fibrosis.[26]

Gross

  • Dilated bile ducts.[21]

Microscopic

Features:[23]

  • Dilated bile ducts.
  • Periductal fibrosis. (???)
  • +/-Fibrosis.

Image:

Hereditary hemochromatosis

For secondary causes see secondary hemochromatosis.

Wilson disease

Alpha-1 antitrypsin deficiency

  • AKA alpha1-antiprotease inhibitor deficiency.

Other

Primary Systemic Sclerosis

Primary systemic sclerosis in the liver Primary systemic sclerosis in the liver Primary systemic sclerosis in the liver Primary systemic sclerosis in the liver Primary systemic sclerosis in the liver Primary systemic sclerosis in the liver
Primary systemic sclerosis in a 67 year old White, non-Hispanic man who had undergone renal transplantation for idiopathic nodular glomerusclerosis, which had recurred in 2013. He had been scheduled to receive a second transplantation, but had not yet received one. The patient had a positive anti-nuclear antigen study, with a positive scleroderma antibody (SCL-70), a high SCL-70 antibody index of 3.9, and negative DNA, Chromatin, Anti-Riboscomal P, SS-A, SS-B, anti Smith, RNP, JO-1, anticentromere antibody and rheumatoid factor serologic studies. Hepatitis A, B, and C serologic studies were negative. Liver function tests showed normal albumin and total bilirubin levels with alkaline phosphatase of 712 IU/L (35-129 normal range), alanine aminotransferase 59 IU/L (5-41 normal range), and aspartate aminotransferase 68 IU/L (5-37 normal range). This case provisions many of the features known to be present in primary systemic sclerosis as seen in the skin. A. At low power, triads appear almost as white ghosts against a relatively normal set of hepatocyte lobules. B. Closer examination reveals some triads to be expanded, with peripheral bile ductular proliferation and modest associated chronic inflammation without interface hepatitis. C. Portal arterioles had thick walls; inflammation included lymphocytes and occasional plasma cells. D. Trichrome failed to stain the material in the triads blue, but did show space of Disse collagenization. E. PAS with diastase showed positive staining of the material with emphasis on the arteriole walls. F. Hemosiderosis was seen on iron stain.


Budd-Chiari syndrome

  • AKA hepatic vein obstruction.

General

  • Hepatic outflow obstruction.

Clinical triad:[28]

  • Ascites.
  • Abdominal pain.
  • Hepatomegaly.

Etiology:

Clinical DDx:

Microscopic

Features:[30]

  • Sinusoidal dilation in zone III (congestion).
  • +/-Hepatocyte drop-out.
  • +/-Centrilobular fibrosis.

DDx congestion:

Vanishing bile duct syndrome

General

  • Fatal.

DDx:[32]

Microscopic

Features:[32]

  • Loss of intrahepatitic bile ducts - key feature.
  • Cholestasis.

Note:

  • May occur without fibrosis and inflammation; thus, can be easy to miss.

IHC

  • CK7 -ve.
    • Marks bile ducts.

Hepatic Graft versus Host Disease (L-GVHD)

Hepatic graft versus host disease (L-GVHD) Hepatic graft versus host disease (L-GVHD) Hepatic graft versus host disease (L-GVHD) Hepatic graft versus host disease (L-GVHD) Hepatic graft versus host disease (L-GVHD) Hepatic graft versus host disease (L-GVHD) Hepatic graft versus host disease (L-GVHD)
Hepatic graft versus host disease (L-GVHD) in a 22 yo man who underwent bone marrow transplantation after developing ALL. A. Low power view shows brownish discoloration in triad, but is otherwise of little interest. B. Arterioles in triads were accompanied by bile ducts in only 30% of cases; this image shows an arteriole without a bile duct. Note the pigment and the accompanying macrophage/lymphocyte inflammation, not extreme. The added chronic inflammation is a feature of chronic L-GVHD. C. Bile ducts, when shown, showed extensive damage, here seen as loss of cytoplasm, and nuclear pleomorphism and hyperchromasia (other degenerative changes, not seen here, include nuclear dropout or necrosis, cytoplasmic eosinophilia, loss of duct lumen). Lymphocytosis into the ducts was not seen. D. Ballooned hepatocytes and dilated canaliculi were seen. E. Pigment was present, but mostly in Kupffer cells, not hepatocytes or as bile plugs. F. Up to two foci of spotty necrosis were seen in a 100X field (field shown is 200X); not shown are rare apoptotic hepatocytes. G. An iron stain showed the pigment represented extemsive iron deposition, with emphasis on Kupffer cells and portal triad macrophages, frustrating definite assessment of bile plugs in canaliculi. The hemosiderosis resulted from the many blood transfusions the patient had received.

Extrahepatic biliary obstruction

A. Sinusoidal dilatation, circular spaces of hepatocytes, small portal triads(40X).
B. Bile in hepatocytes about central vein & in plugs in canaliculi [yellow arrowhead] (400X).
C. Trichrome shows fibrosis about central vein (400X).
D. PAS with diastase shows portal triads with mild edema and chronic inflammation, without tortuous bile duct (400X).
Early extrahepatic biliary obstruction, demonstrated radiographically, transient, with rise in bilirubin, alkaline phosphatase, and transaminases. Pure canalicular cholestasis near terminal hepatic venules also seen in acute hepatitis, drug reactions, benign recurrent cholestasis, pregnancy, sepsis, & lymphomas. A. Sinusoidal dilatation, circular spaces of hepatocytes, small portal triads. B. Bile in hepatocytes about central vein & in plugs in canaliculi [yellow arrowhead]. C. Trichrome shows fibrosis about central vein. D. PAS with diastase shows portal triads with mild edema and chronic inflammation, without tortuous bile duct.
A. Expanded inflamed portal triads, swollen hepatocytes (40X)
B. Edematous stroma, proliferating ductules [yellow arrowheads], PAS-D macrophages [red arrowhead] (PAS with diastasse, 200X)
C. Disordered, often swollen hepatocytes,some with feathery degeneration (net like spaces in cytoplasm [blue arrowhead], rare Councilman body [green arrowhead] (400X)
D. Bile in hepatocytes [cyan arrrowhead] & in canaliculi [purple arrowheads]. Empty acinar spaces bounded by hepatocytes [orange arrowhead] (400X, higher pixel),
Changes of extrahepatic biliary obstruction, months duration. A. Expanded inflamed portal triads, swollen hepatocytes. B. Edematous stroma, proliferating ductules [yellow arrowheads], PAS-D macrophages [red arrowhead]. C. Disordered, often swollen hepatocytes,some with feathery degeneration (net like spaces in cytoplasm) [blue arrowhead], rare Councilman body [green arrowhead]. D. Bile in hepatocytes [cyan arrrowhead] & in canaliculi [purple arrowheads]. Empty acinar spaces bounded by hepatocytes [orange arrowhead].
A. Expanded, light colored portal triads (arrows)(20X).
B. Proliferating bile ductules (cyan arrows) with neutrophils (yellow arrows), not specific for acute cholangitis, of assistance with large bile duct obstruction (400X)..
C. Uninflamed interlobular duct (yellow arrow) with, accompanying blood vessel (red arrow) (400X)
D. Bile infarct with pyknotic nuclei (arrows)(400X).
E. Bile (arrow) in interlobular bile duct with disordered nuclei (400X).
F. Bile plugs in cannaliculi (red arrows), feathery degeneration producing foamy macrophage like hepatocytes (yellow arrows)(400X).
Large bile duct obstruction. A. Expanded, light colored portal triads (arrows). B. Proliferating bile ductules (cyan arrows) with neutrophils (yellow arrows), not specific for acute cholangitis, of assistance with large bile duct obstruction. C. Uninflamed interlobular duct (yellow arrow) with, accompanying blood vessel (red arrow). D. Bile infarct with pyknotic nuclei (arrows). E. Bile (arrow) in interlobular bile duct with disordered nuclei. F. Bile plugs in cannaliculi (red arrows), feathery degeneration producing foamy macrophage-like hepatocytes (yellow arrows).

Congestive hepatopathy

Drug-induced liver disease

  • AKA drug-induced liver toxicity.

Focal nodular hyperplasia

  • Abbreviated FNH.

Nodular regenerative hyperplasia

General

Etiology

  • Arterial hypervascularity secondary to loss of hepatic vein radicles (loss of central venule in hepatic lobule).[35]

ASIDE: radicle = ramulus - smallest branch or vessel or nerve.[37]

Gross

  • Diffuse nodularity - whole liver.

Microscopic

Features:[35]

  • "Plump" hepatocytes surrounded by atrophic ones.
  • No fibrosis.

Sinuosoidal obstruction syndrome

  • May be referred to as Hepatic veno-occlusive disease.[38]

General

  • Term for obstruction due to toxicity from a chemotherapeutic agent.[39][30]

Clinical DDx:

Microscopic

Features:[30]

  • Subendothelial swelling in hepatic venules.

Negatives:

  • No thrombosis.

Ascending Cholangitis (Acute Cholangitis)

General

  • Term for infection of bile ducts, usually due to obstruction

Clinical DDx:


Microscopic

Images

A. Rounded, clear (edematous) portal tracts (arrows) separated by hepatocytes with dilated sinusoids (Row 1 Left 40X).
B. Neutrophils about hepatocytes (arrows) have spilled into the lobule from a portal tract (Row 1 Right 200X).
C. Proliferated bile ductules (arrows) bearing neutrophils within epithelium and lumens are features of obstruction that should prompt a search for interlobular ducts with acute inflammation (Row 2 Left 400X).
D. The epithelium of the ducts can be severely degenerated. Neutrophils (cyan arrows) invade epithelium of an interlobular duct that are recognizable mainly as a circle of rounded nuclei; the associated arteriole (red arrow) should be identified to ensure an interlobular duct is being evaluated. Note the proliferated bile ductules (blue arrows) (Row 2 Right 400X).
E. A PAS without diastase stain colors the arteriole (blue arrow), as well as the rim of the interlobular duct within which lies a neutrophil (cyan arrow) (Row 2 Right 400X). .
F. A PAS with diastase stain colors the arteriole (red arrow), as well as the rim of the interlobular duct within which lies a neutrophil (cyan arrow) (Row 1 Right 400X)
Acute cholangitis in a patient with multiple bile duct procedures. After the biopsy, removal of bile duct stones released pus. A. Rounded, clear (edematous) portal tracts (arrows) separated by hepatocytes with dilated sinusoids. B. Neutrophils about hepatocytes (arrows) have spilled into the lobule from a portal tract. C, Proliferated bile ductules (arrows) bearing neutrophils within epithelium and lumens are features of obstruction that should prompt a search for interlobular ducts with acute inflammation. D. The epithelium of the ducts can be severely degenerated. Neutrophils (cyan arrows) invade epithelium of an interlobular duct that are recognizable mainly as a circle of rounded nuclei; the associated arteriole (red arrow) should be identified to ensure an interlobular duct is being evaluated. Note the proliferated bile ductules (blue arrows). E. A PAS without diastase stain colors the arteriole (blue arrow), as well as the rim of the interlobular duct within which lies a neutrophil (cyan arrow). F. A PAS with diastase stain colors the arteriole (red arrow), as well as the rim of the interlobular duct within which lies a neutrophil (cyan arrow).

A.Low power shows variably sized inflamed portal tracts (40X)
B. Trichrome shows dilated sinusoids and space of Disse collagenization (200X)
C. Inflammatory focus with macrophages and neutrophils (400X).
D. PAS with diastase shows proliferated bile ductules at edge of triad with neutrophils, which should not be used to make a definite diagnosis of acute cholangitis (400X).
E. PAS without diastase showing acutely inflamed bile duct, with accompanying blood vessel of similar size, diagnostic of acute cholangitis (400X).
F. PAS with diastase showing neutrophil in bille duct lumen, diagnostic of acute cholangitis (400X).
Patient with sepsis and acute cholangitis. A. Low power shows variably sized inflamed portal tracts. B. Trichrome shows dilated sinusoids and space of Disse collagenization. C. Inflammatory focus with macrophages and neutrophils. D. PAS with diastase shows proliferated bile ductules at edge of triad with neutrophils, which should not be used to make a definite diagnosis of acute cholangitis. E. PAS without diastase showing acutely inflamed bile duct, with accompanying blood vessel of similar size, diagnostic of acute cholangitis. F. PAS with diastase showing neutrophil in bille duct lumen, diagnostic of acute cholangitis.

Polycystic kidney disease and the liver

General

Complications of PKD in the liver:[40]

  1. Infected cyst.
  2. Cholangiocarcinoma.
  3. Cholestasis/obstruction due to duct compression.[41]

Cysts:

  • Cysts in the liver, like the kidney, are thought to enlarge with age.

Microscopic

Features:[42]

  • Von Meyenburg complexes (bile duct hamartoma):
    • Cluster of dilated ducts with "altered" bile.
    • Surrounded by collagenous stroma.
    • Separate from the portal areas.[43]

Images:

Notes:

  • Appearance on ultrasound[44] and CT (hypodense)[45] - similar to metastases.

Peliosis hepatis

Total parenteral nutrition

  • Abbreviated TPN.

General

  • Indication: short gut syndrome, others.

Microscopic

Variable - may range from: steatosis, steatohepatitis, cholestasis, fibrosis and cirrhosis.[46]

Features (classic):[47][48]

  • Steatosis (periportal) - early.
  • Cholestasis - late.

Giant cell hepatitis

  • AKA neonatal giant cell hepatitis.
See: Giant cell hepatitis.

Hepatic amyloidosis

  • AKA liver amyloidosis.
  • AKA amyloidosis of the liver.

General

Microscopic

Features:

  • Amorphous extracellular pink stuff on H&E - see amyloid article.

DDx:

Images

A. Amorphous material replaces hepatic parenchyma [4X]
B. Material barely stains blue on trichrome [10X]
C. Material stains red on unpolarized Congo Red [40X]
D. Material stains apple green on polarized Congo Red [40X]
Amyloidosis. A. Amorphous material replaces hepatic parenchyma. B. Material barely stains blue on trichrome. C. Material stains red on unpolarized Congo Red. D. Material stains apple green on polarized Congo Red.

Stains

Fulminant hepatic necrosis

Secondary hemochromatosis

For the hereditary one see hereditary hemochromatosis.

General

  • Iron overload secondary to blood transfusions for hereditary or acquired anemia.[49]
  • Imaging considered the best test, as iron deposition is patchy.[49]

Selected hereditary causes:[49]

Selected acquired causes:[49]

Microscopic

See hereditary hemochromatosis.

Hepatic sarcoidosis

Overlapping Disorders

Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed. Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed. Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed. Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed. Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed. Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed.
Changes of steatohepatitis and interface hepatitis, with granuloma. Patient with diabetes was ANA, AMA, HCV, HBV negative, without drugs known to produce granulomas or interface hepatitis. This may be a case of AMA negative primary biliary cirrhosis, but studies to determine that with certainty were not performed. A. Low power shows hepatocytes afflicted by steatosis and an inflamed portal tract. B. In a region of fatty change lie cytoplasmic tufts of ballooning degeneration (green arrows) and a lipogranuloma (black arrow). C. At the portal-hepatocyte junction lies interface hepatitis (black arrows), as well as extension of inflammation into the lobule (green arrows). D. Red hepatocytes bounded by inflammation denote piecemeal necrosis [PAS without diastase]. E. Giant cells intermixed with lymphocytes prove a portal granuloma [PAS without diastase]. F. A blue fibrous bridge extends from a triad [Trichrome].

Acute obstructive changes and changes of recurrent acute injury Acute obstructive changes and changes of recurrent acute injury Acute obstructive changes and changes of recurrent acute injury Acute obstructive changes and changes of recurrent acute injury Acute obstructive changes and changes of recurrent acute injury Acute obstructive changes and changes of recurrent acute injury Acute obstructive changes and changes of recurrent acute injury
Acute obstructive changes and changes of recurrent injury in 46 yo man with Clostridium perfringens positive blood culture, an ERCP that showed duodenal compression by the pancreas with resultant bile duct dilatation. The patient had had and continued to have multiple bouts of acute pancreatitis. At the time of biopsy, decreased platelet count/hemoglobin/albumin, elevated lipase/amylase/PT/PTT, normal alkaline phosphatase, bilirubin, AST/ALT, AMA, hepatitis virus serology, ANA. A. Fragment biopsy shows inflamed triads and bridges. B. Trichrome shows bridges without nodules, evidence of prior injury; the patient subsequently developed multiple episodes of pancreatitis. C. Reticulin shows piecemeal necrosis, with black lines bounding individual hepatocytes at interface (arrows). D. Collapse is shown by closly approximated thick black lines; one cannot call portal-central collapse without seeing a central vein. Note on this and the other reticulin image that regeneration, two cell thick cords, is not prominent. E. PAS D of two portal triads, far nearer than normal, both expanded. Note increased number of ducts/ductules (red arrows), neutrophils, and PAS-D macrophages. F. PAS D shows collapse extending from a triad to a portion of a lobule with steatosis. No feathery degeneration or bile duct plugs were seen. Neither were foci of spotty necrosis or abscess seen. G. Other triads, again edematous, showed more of a chronic inflammatory response, with occasional plasma cells (black arrows). Also present are neutrophils (red arrows). The bile duct (grey arrow) near the artery (brown arrow) shows mildly disturbed nuclei. Note early proliferated bile ductules (cyan arrows).

Hepatitis B virus with steatohepatitis Hepatitis B virus with steatohepatitis Hepatitis B virus with steatohepatitis Hepatitis B virus with steatohepatitis Hepatitis B virus with steatohepatitis Hepatitis B virus with steatohepatitis
Hepatitis B virus with steatohepatitis in a 36 year old man with hepatitis B surface antigen and hepatitis Be antigen positivity, Hepatitis be QTPC of 1750 cop/mL, an occasionally mildly elevated (42) ALT, and normal glucose, alkaline phosphatase, bilirubin, and other transaminases. He had a history of alcohol abuse, which became controlled. A. Triads show scant inflammation without definite interface hepatitis. About one-fourth of the lobule, not pan-acinar, is afflicted by steatosis. B. Occasional tufts are seen (arrow), indicating focal ballooning sufficient for a diagnosis of steatohepatitis. C. Glycogenated nuclei (black arrows) and hepatocytes with feathery degeneration (red arrows) are seen. D. Very rare foci of spotty necrosis were seen. E. Apart from this triad and the one in the trichrome stain in F, which had moderate inflammation comprising lymphocytes and macrophages, all triads were small, most without any inflammation at all. Neither collapse nor piecemeal necrosis were seen on reticulin stain. F. Trichrome stain showed only portal fibrosis. The interhepatocyte fibrosis required for brunt fibrosis stage I was not seen. Hence, one would grade this as follows: A) Chronic hepatitis (history of hepatitis B), Metavir activity index 1, Piecemeal necrosis 0, Lobular necrosis 1, Metavir fibrosis stage 1, B) Steatohepaitits, Brunt necroinflammatory grade 1, Brunt fibrosis stage 0.

See also

References

  1. Mitchell, Richard; Kumar, Vinay; Fausto, Nelson; Abbas, Abul K.; Aster, Jon (2011). Pocket Companion to Robbins & Cotran Pathologic Basis of Disease (8th ed.). Elsevier Saunders. pp. 448. ISBN 978-1416054542.
  2. Mitchell, Richard; Kumar, Vinay; Fausto, Nelson; Abbas, Abul K.; Aster, Jon (2011). Pocket Companion to Robbins & Cotran Pathologic Basis of Disease (8th ed.). Elsevier Saunders. pp. 441. ISBN 978-1416054542.
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