LIVER - Normal histology - Cirrhosis 8
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Transcript LIVER - Normal histology - Cirrhosis 8
LIVER
- Normal histology
- Cirrhosis
8th November 2007
Dr. Cynthia Heffron
Clinical Lecturer in Histopathology
INTRODUCTION
1.
2.
3.
Normal liver weight 1400 - 1600g.
Architecture of liver:
Divided into lobules oriented around the terminal tributaries of
the hepatic vein.
Sheets of hepatocytes with portal triads at the corner of each
lobule.
Portal triad/tract:
Bile duct
Portal vein
Hepatic artery
The functional unit of the liver parenchyma is the hepatic
acinus with zones 1,2 & 3. Zone 1 is periportal, zone 3 is
perivenular, zone 2 intermediate.
1. Parenchyma
Liver cells (hepatocytes) trabeculae 1 cell thick in
adults
Kupffer cells in sinusoids are phagocytes
Hepatic stellate cells (also called Ito cells) in
space of Disse (an extrasinusoidal space)
Cells of mesenchymal origin
Store vitamin A
Transform into collagen-producing myofibroblasts when
there is inflammation and fibrosis of the liver
Regulate blood flow in sinusoids
Liver-associated lymphocytes.
2. Biliary drainage system
Canaliculi (between abutting hepatocytes)
Canals of Hering & cholangioles
1-2um in diameter
Canaliculi join to form these larger structures
Intra-hepatic bile ducts
Extra-hepatic bile ducts
3. Vasculature
Incoming blood to the liver at the porta hepatis:
Within the liver:
Portal vein supplies 70% of the blood flow.
Hepatic artery supplies 30% of the blood flow.
Sinusoids lined by fenestrated endothelium.
Blood leaving the liver:
Hepatic venules
Hepatic veins drain into the IVC.
Functions of liver
The liver is important for
Metabolism of carbohydrate, protein, lipids.
Protein synthesis, albumin, coagulation factors,
complement factors etc.
Storage of iron, copper, vitamins A, D, B12.
Detoxification/drug metabolism.
Bile production.
Investigation of liver diseases
Biochemical - enzymes, proteins, bilirubin.
Haematological - coagulation factors among others.
Immunological - antibodies (viruses, autoimmune).
Imaging - ultrasound, CT, MRI, ERCP, MRCP.
Liver biopsy:
percutaneous needle biopsy, transjugular biopsy, wedge
biopsy at laparoscopy or open surgery.
Useful in providing information as to the aetiology and severity
of the liver disease, ruling out the presence of other
concomitant disease, monitoring response to therapy.
Focal lesions require US or CT guidance.
Morphological patterns of liver injury
1.
Degeneration
2.
Ballooning degeneration (hydropic change)
Feathery degeneration (bile-induced damage).
Intracellular accumulations
Fat (steatosis)
Iron
Copper
Bile
Mallory’s hyaline
Haemosiderosis
Steatosis
Mallory’s hyaline
Bile
Morphological patterns of liver injury
1.
Degeneration
2.
Intracellular accumulations
3.
Ballooning degeneration (hydropic change)
Feathery degeneration (bile-induced damage).
Fat (steatosis)
Iron
Copper
Bile
Mallory’s hyaline
Necrosis
Coagulative or lytic and apoptosis.
Necrosis may be:
randomly focal (spotty necrosis),
zonal eg zone 3
bridging (bridging hepatic necrosis, eg portal to venular), involve most
or almost all of the liver (submassive and massive respectively).
Zone 3 is most prone to injury as it is farthest from the blood supply and
is the area containing most drug-metabolising enzymes.
Morphological patterns of liver injury
4. Inflammation
Acute, chronic or granulomatous.
May be portal, periportal (interface hepatitis) or
acinar (focal, or panacinar)
Chronic inflammation
• Viral hepatitis
Granulomatous inflammation
• Foreign material
• Organisms
• Drugs
Morphological patterns of liver injury
5. Regeneration
Hepatocytes have great ability to regenerate.
Regeneration occurs in many diseases.
Bile duct proliferation is seen in the portal tracts in
cirrhosis.
6. Fibrosis
• Forms in response to inflammation or direct toxic injury.
• Irreversible form of liver injury.
• Can be portal, perivenular, form bridging fibrosis, finally cirrhosis.
The great variety of liver diseases and the
liver’s limited patterns of response means
that close clinicopathological correlation is
required for their diagnosis.
CIRRHOSIS
Definition:
Degenerative disease in an organ of the body, esp. the liver,
marked by excess formation of connective tissue and, usually,
subsequent painful swelling
Etymology: ModL < Gr kirrhos, tawny + -osis: so named by R. T.
H. Laënnec (1781-1826), Fr physician, because of the orangeyellow appearance of the diseased liver
Among the top 10 causes of death in the Western world.
End stage of liver disease.
Characterised by:
1.
2.
3.
Bridging fibrous septa
Parenchymal nodules
Disruption of the architecture of the entire liver
Characterised by:
1.
Bridging fibrous septa:
2.
Fibrosis is usually irreversible.
Regression observed rarely.
Parenchymal nodules:
Regenerative nodules surrounded by fibrosis are necessary
for diagnosis.
< 3mm = Micronodular cirrhosis
•
> 3mm = Macronodular cirrhosis
•
3.
Bile duct obstruction or alcohol
Other causes
Disruption of the architecture of the entire liver
Vasculature affected in particular with formation of abnormal
interconnections between vascular inflow and hepatic vein
outflow
Classification of Cirrhosis?
Generally classified by Aetiology
Aetiology of Cirrhosis
Infections:
Viral hepatitis (10%).
Toxins and drugs:
Alcohol (60-70%)
Therapeutic drugs.
Autoimmune:
Hepatitis
Primary biliary cirrhosis.
Metabolic:
Haemochromatosis (5%).
Wilson disease.
Alpha-1-antitrypsin deficiency.
Glycogen storage disease and many others.
Biliary diseases (5-10%):
Congenital atresia.
Sclerosing cholangitis.
Hepatic outflow obstruction.
Cryptogenic (10-15%).
Aetiology of cirrhosis
The aetiology of cirrhosis varies throughout the world.
In the Western world, alcohol is the most common factor
at 60% and viral hepatitis 10%.
Viral hepatitis is the most common factor in Asia and
Africa.
Cryptogenic cirrhosis (cause unknown) forms 10%.
Once cirrhosis has developed and become established,
it is usually not possible to determine the aetiology
by morphology alone and results of other
investigations are required.
Biopsy
Used for primary diagnosis and monitoring
disease.
Percutaneous, transjugular, wedge biopsies.
One study has shown that biopsy was a
significant aid in establishing the diagnosis in
approx 75% of cases.
Accurate interpretation of the biopsy requires
clinical and laboratory data.
Mallory bodies
• Characteristic of alcoholic hepatitis but not specific
• Composed of tangled cytokeratin intermediate filaments and other proteins
Alcoholic liver disease
Fatty liver
Alcoholic hepatitis
Cirrhosis (10-20% of
alcoholics develop
cirrhosis)
Gross:
Enlarged fatty liver
Microscopic:
Hepatocyte swelling
and necrosis
Mallory bodies
Neutrophilic reaction
Fibrosis
• Individual hepatocytes are affected by viral hepatitis.
• Viral hepatitis A rarely leads to signficant necrosis, but hepatitis B can result
in a fulminant hepatitis with extensive necrosis.
• A large pink cell undergoing "ballooning degeneration" is seen below the
right arrow.
• At a later stage, a dying hepatocyte is seen shrinking down to form an
eosinophilic "councilman body" below the arrow on the left.
Histological features of viral hepatitis
Acute
Ground-glass hepatocytes
(HBV)
Balloon degeneration of
hepatocytes
Fatty change (HCV)
Macrophage aggregates
Apoptosis (councilman
bodies, spotty necrosis)
Bridging necrosis
Portal tract inflammation
Chronic
Lymphoid aggregates
Interface hepatitis
Fibrosis
Periportal
Bridging
Cirrhosis
• Hereditary Haemochromatosis: autosomal recessive, chromosome 6
• Defect in intestinal absorption of iron leading to excessive absorption
• Normal amount of Iron in liver – 0.5g, in haemochromatosis up to 50g
• Men > women
Secondary haemochromatosis:
Most common cause = Haemolytic anaemias
Others: transfusions, alcohol
Clinically:
Main manifestations are hepatomegaly, abdominal
pain, skin pigmentation, deranged glucose
homeostasis or frank diabetes mellitus, cardiac
dysfunction and atypical arthritis.
High risk of developing hepatocellular carcinoma.
The periportal red hyaline globules seen here with periodic acid-Schiff (PAS)
stain are characteristic for alpha-1-antitrypsin (AAT) deficiency.
α1- antitrypsin (AAT) deficiency
AAT deficiency is an autosomal recessive disorder
(chromosome 14) marked by abnormally low serum
levels of this major protease inhibitor.
Most people with AAT deficiency are likely to develop
chronic obstructive pulmonary disease with panlobular
emphysema.
The globules are collections of alpha-1-antitrypsin not
being excreted from hepatocytes.
This may eventually lead to chronic hepatitis and
cirrhosis.
Liver disease is more likely to occur in children with
AAT deficiency, while lung disease occurs in adults.
• This is a case of primary biliary cirrhosis, a rare autoimmune disease.
• Seen here in a portal tract is an intense chronic inflammatory infiltrate with loss
of bile ductules.
Primary biliary cirrhosis
• Autoimmune cholestatic liver disease mostly of
middle-aged women.
• Characterized by destruction of bile ductules
within the triads of the liver.
• This destruction is granulomatous and destroys
medium sized intrahepatic bile ducts.
• Antimitochondrial antibody can be detected in
serum.
• Micronodular cirrhosis ensues.
Pathogenesis of Cirrhosis
Liver injury results in chronic inflammation and activation of Kupffer cell,
and other endogenous liver cells with the production of cytokines.
These, together with disruption of the extracellular matrix activates
hepatic stellate cells (HSC). Toxins may activate HSCs. These
transform into myofibroblasts which produce collagen and constrict
sinusoids.
Collagen in the space of Disse leads to “capillarisation” of the sinusoids
and loss of endothelial fenestrations, hindering exchange of solutes.
New vascular channels in fibrous bands link inflow of blood (venous &
arterial) with outflow (hepatic venules) thus by- passing parenchyma.
Existing vascular channels and biliary channels may be obliterated.
The results are internal vascular shunts and portal hypertension.
The hepatocytes in the regenerative nodules may appear normal
microscopically but are unable to adequately fulfill their functions.
Function will be further reduced if there is continuing liver cell damage.
CLINICAL FEATURES
Cirrhosis may be asymptomatic.
When symptomatic:
Non specific symptoms: weakness, fatigue, weight loss, anorexia, nausea,
gaseous abdominal distension, upper abdominal discomfort.
Symptoms and signs secondary to liver failure: encephalopathy,
hypoglycaemia, bleeding, ascites, overwhelming infection
Symptoms and signs secondary to portal hypertension: ascites,
portosystemic venous shunts (varices), congestive splenomegaly, hepatic
encephalopathy.
The liver may be enlarged, hard and irregular or smaller than normal.
Decompensated cirrhosis manifests as signs of liver failure or
complications of portal hypertension.
Deterioration in liver function can be an indication of the development
of hepatocellular carcinoma.
Complications of Cirrhosis
1.
2.
3.
4.
Hepatic failure
Hepatic encephalopathy
Hepatorenal syndrome
Hepatocellular carcinoma
Complications of cirrhosis (continued)
5. Portal hypertension
Portal venous pressure > 10mmHg
Causes
Prehepatic – obstructive thrombosis
Hepatic - cirrhosis
Posthepatic – right sided heart failure, constrictive pericarditis, hepatic vein outflow
obstruction
Manifestations
Ascites
Transudate (<3gm/dL protein),straw coloured or pale green, a few mononuclear cells.
Risk of spontaneous infection when polymorphs predominate.
Is due to aldosterone-induced retention of Na & water, low oncotic pressure (low
albumin), and portal hypertension.
Excess hepatic lymph and intestinal fluid leakage also contributes to ascites.
Portosystemic shunts
oesophageal varices
periumbilical caput medusae
haemorrhoids
Congestive splenomegaly
Hepatic encepaholopathy
Other complications due to impaired parenchymal function:
Disturbed glucose homeostasis
Impaired bile salt prodcution
Malabsortpion
Decreased albumin
Unbound drugs and metatbolites in plasma
Jaundice
Clotting factors
Oestrogen metabolism impaired
Spider naevi
Finger clubbing
Renal failure
Infections
The ultimate mechanism of most cirrhotic
deaths is:
Progressive liver failure.
Complication related to portal hypertension.
Development of hepatocellular carcinoma.