Liver Pathophysiology and Disease Study Guide PDF

Summary

This document provides a study guide on liver pathophysiology and diseases, covering classifications, acute and chronic conditions, infections, and causes. It details various aspects including drug toxicity, infections, and pregnancy-related issues.

Full Transcript

- Liver Pathophysiology / Diseases

- Liver diseases are classified into:

- Parenchymal (Hepatocellular) or Obstructive

- Acute or Chronic

- Pre-Hepatic (increased unconjugated bilirubin)

- Hemolysis

- Hematoma reabsorption

- Hepatocellular (Parenchymal) Injury (increased conjugated
bilirubin, ALT/AST, PT, and AP; decreased albumin if chronic)

- Acute:

- Drug toxicity - "tylenol is the \#1 cause of acute liver
failure"

- Other drugs that are toxic to the liver: NSAIDs,
amiodarone, anabolic steroids, long-term
glucocorticoids, carbon tetrachloride, TPN, cancer
chemotherapeutic agents, some herbal remedies

- Halothane (Fluothane) Hepatitis

- Acetaminophen is not the only drug that can
cause acute liver failure

- Halothane: VA introduced in 1950's

- Found to cause ALF (hepatic necrosis) -
incidence 1:35,000 ("extremely rare")

- Reactive TFA (trifluoroacetyl)
metabolite (halothane is 20% metabolized
this way)

- Can occur with Enflurane (2%) \> Iso
(0.2%) \> Des (0.01%)

- Halothane is not longer available in the
US - still used in developing countries

- Two distinct suspected manifestations:

- Elevated LFTs without evidence of liver
failure - due to combination of
halothane and hypoxia?

- Severe ALF - immune mediated process?

- Infection (presumably Hepatitis A and B)

- Alcoholic hepatitis

- Pregnancy-related

- Hyperemesis Gravidarum - 1st trimester, emesis that
warrants IVFs; elevated liver enzymes in up to 50%

- Intrahepatic Cholestasis - 2md or 3rd trimester;
impaired bile acid transport in lobule; high-risk
pregnancy

- Preeclampsia (HTN, Edema and Proteinuria) - 3rd
trimester; "treatment is to deliver the baby"

- Elevated aminotransferases = severe preeclampsia

- HELLP syndrome: Hemolysis, Elevated Liver Enzymes,
Low Platelet Count; treatment is to deliver the baby

- AFLP: Acute Fatty Liver of Pregnancy - 3rd
trimester; fatty infiltration of the liver that
causes portal HTN and hepatic encephalopathy;
treatment is to deliver the baby

- Chronic:

- Alcoholic liver disease

- Non-alcoholic fatty liver disease

- Caused by excessive fatty deposits in the liver

- Ranges in severity from steatosis (simple fat
deposits) → steatohepatitis/NASH (hepatocellular
necrosis)

- Associated with metabolic syndrome

- Insulin resistance

- Obesity

- Central Adiposity

- Type-II Diabetes

- HTN

- Elevated triglycerides

- Most common cause of elevated liver enzymes in
adults

- NASH: Liver biopsy shows steatosis with inflammation
and fibrosis

- Treatment: weight loss (bariatric surgery)

- Acute vs Chronic Hepatitis:

- Acute Hepatitis -

- Hepatocellular injury due to viral infection, drug
reaction or exposure to hepatotoxin

- Acetaminophen

- Alcohol

- Mushrooms

- Chronic Hepatitis -

- Lasting \>6 months

- Lab values do not correlate with disease severity

- Liver biopsy -\> classification into one of three
types

- Chronic Persistent Hepatitis

- Chronic Lobular Hepatitis

- Chronic Active Hepatitis- \*assume cirrhosis

- "Hepatitis C - most likely to develop into chronic
liver failure"

- Hepatocellular Carcinoma

- Most common primary liver malignancy

- 3rd most common cause of death globally

- Men \> women

- Risk:

- Treatment:

- Treatment for non surgical patients:

- "Typically have an ultrasound every 6 months"

- Cholestatic / Post-Hepatic (increased conjugated bilirubin;
AST/ALT if late dx; AP, GGTP, and 5'-NT; decreased albumin
late dx)

- Biliary disease - affects \> 20 million in the U.S.

- Causes:

- Biliary obstruction

- Cholestatic disease

- Chronic:

- Impaired bile flow increases biliary
pressure and backflow into liver →
hepatocyte destruction

- If bacteria in bile → ascending
cholangitis, hepatic abscess, sepsis,
and acute kidney injury can occur

- Deficiencies in Vitamin K-dependent
clotting factors (II, VII, IX, X)

- Hypercoagulability

- S&S: fatigue, pruritus, dark urine, pale
stools

- Diagnosis: Abdominal US to determine
extrahepatic vs. intrahepatic cause

- Extrahepatic causes: bile duct
obstruction by stone, stricture, mass

- Intrahepatic causes: immune-mediated,
infectious, drug-induced,
paraneoplastic, ischemic

- Labs: Elevated serum AP and GT; may have
elevated bilirubin

- Check AMA (antimicrobial antibody)
titers to rule out Primary Biliary
Cholangitis

- Treatment: Endoscopic Retrograde
Pancreatography (ERCP)

- Primary biliary cholangitis (PBC) - autoimmune "no
test questions"

- Primary sclerosing cholangitis (PSC) - autoimmune
"no test questions"

- Sepsis

- Cirrhosis

- **End-result** of chronic liver diseases

- Lobules are replaced with fibrosis and regenerative nodules

- "What zone cells are most susceptible to ischemia? Zone 3 →
these are responsible for glycolysis, lipogenesis, and
detoxification / biotransformation"

- Disrupts blood flow thru liver → leading to shunt formation →
"blood backs up into portal venous circulation" → Portal HTN,
Esophageal Varices, Ascites Hepato-renal syndrome (HRS), Pulm
HTN

- Increased hepatic resistance and intrahepatic
vasoconstriction- portal pressure continues to increase →
portal HTN

- Body responds with splanchnic vasodilation → causes a
decreased effective arterial circulation

- Now the SNS and RAAS get activated → leads to sodium and
water retention, hypervolemia, increased CO - viscous cycle

- S&S:

- Jaundice, thrombocytopenia, bleeding, endocrine
abnormalities, diabetes, hepatocellular carcinoma

- Labs:

- Increased ALT, AST, AP, GGT, bilirubin, PT,

- Decreased albumin

- Causes:

- Alcoholic Liver Disease

- Chronic Hepatitis

- Nonalcoholic Steatohepatitis Hemochromatosis

- Wilson's Disease

- Primary Biliary Cirrhosis

- Primary Sclerosing Cholangitis

- Alpha-1 Antitrypsin Deficiency Prolonged Cholestasis

- Toxins / Drugs

- Hepatic Venous Outflow Obstruction

- Cystic Fibrosis

- Treatment: depends on disease severity

- Multiple Systems are affected:

- Coagulation

- Hemostasis - mechanisms at play affecting both intrinsic
and extrinsic pathways

- \*\*\*Leads to disrupted balance between bleeding
and clotting\*\*\*

- Decreased synthesis of both clotting and inhibiting
factors

- Decreased synthesis of Vitamin-K dependent
clotting factors (II, VII, IX, X)

- Especially in cholestatic diseases (bile
salts are needed for absorption of
Vitamin K)

- Liver synthesizes all procoagulant and
anticoagulant factors EXCEPT: III
(thromboplastin), IV (calcium), and VIII
(VWB)

- Liver is also how activated clotting factors
are cleared from the body

- Vitamin K administration can correct this

- Decreased synthesis of thrombopoietin → leads to
thrombocytopenia → low and dysfunctional platelets

- Decreased synthesis of inhibiting factors (protein
C, protein S, antithrombin III,)

- Increased consumption of platelets and clotting
factors

- Decreased clearance of activated factors

- Hyperfibrinolysis

- Accelerated intravascular coagulation/DIC

- Renal dysfunction / Hepatorenal Syndrome

- Sodium and water retention

- Renal hypoperfusion and decreased GFR

- Increased prostaglandin levels help maintain renal
perfusion - "caution w/ meds that affect
prostaglandins - no NSAIDS"

- Increased sensitivity to nephrotoxic drugs:

- Aminoglycosides

- ACE-Inhibitors

- ARBs

- Definitive treatment: Transplant (in severe cases -
combined liver and kidney transplants)

- Hepatic encephalopathy

- Seen with both acute and chronic liver disease

- Result of accumulated neurotoxins (commonly ammonia, but
can occur without it)

- Neuropsychologic and neuromotor symptoms

- Neuropsychological Symptoms:

- Impaired LOC and attention

- Impaired ability to follow commands

- Altered affect

- Neuromotor Symptoms:

- Hyper-reflexiveness (Asterixis, Clonus, Babinski)

- Nystagmus

- Decerebrate posturing

- Cirrhotic cardiomyopathy

- Liver disease patients (cirrhosis) have hyperdynamic
circulation - "take home message"

- High cardiac output

- Low BP (systolic and diastolic dysfunction) -
"especially post induction"

- Low SVR (from release of nitric oxide)

- Increased overall fluid volume with decreased
circulating volume

- Decreased responsiveness to beta-adrenergic stimulation

- Prolonged Q-T interval

- Dr. Schlesinger's Notes: portal HTN causes release of
vasodilators (esp. NITRIC OXIDE)... "overproduction of
vasodilators" means sympathetic responsiveness is less
effective

- Pulmonary complications

- Hepatopulmonary Syndrome (HPS)

- Affects up to 20% of liver transplant patients

- **Triad** of liver dysfunction, unexplained
hypoxemia and intrapulmonary vascular dilation

- Intrapulmonary vascular dilation (IPVD)

- Type I lesions: precapillary dilations =
functional shunts

- Type II lesions: larger dilations in central
lungs = anatomic shunts

- Post Pulmonary HTN

- Affects 4-6% of liver transplant patients

- Pulmonary HTN in a patient with portal HTN

- Increased risk in female patients and autoimmune
hepatitis

- Hepatic Hydrothorax (HH)

- Ascites fluid passes from peritoneal cavity into
pleural space thru defects in the diaphragm

- Dr. Schlesinger's Notes:

- Other causes: **Cystic fibrosis and A1 Antitrypsin
Disease -** metabolic syndrome (Lung and Liver
consequences)

- Ascites - "Remember they are 'puff balls' and seem fluid
overloaded but are intravascularly dry"

- Associated with a 50% mortality within 3 years

- Infections common

- Treatment:

- Paracentesis + slow correction of hyponatremia

- Needed with serum Na+ is \< 120-125

- If corrected too quickly: central pontine
myelinolysis

- Sodium restriction

- Diuretics

- Albumin replacement if \> 6-8 L drained by
paracentesis

- Varices

- End result of portal HTN

- Treated with beta-blockers to decrease portal pressure
and endoscopic ligation

- Decrease portal pressure by: decreasing CO and
decreasing splanchnic vasoconstriction