Hepatobiliary physiology & disease (DeMonaco) Flashcards
Liver functions
1. protein synthesis
2. nutrient metabolism
3. immune functions
4. excretion
5. storage
Hepatic blood flow
portal vein & hepatic vein & artery
Hepatocytes
- make up 60% of liver mass
- metabolic activities (glucose, albumin, cholesterol, BUN, coagulation factors)
Cholangiocytes
7-10% of liver mass
- biliary secretions & immune response
Kupfer cells
2-5% of liver mass
- phagocytic cells (inflammatory response
Stellate cells
3-5% of liver mass
- lipid & vitamin A storage
- produce collagen -> fibrosis
Liver and CHOs
Storage & release of glucose
- gluconeogenesis (glucose creation)
- glycogenesis (glycogen storage)
- glycogenolysis (glycogen breakdown into glucose, stimualted by glucagon & inhibited by insulin)
glycogen storage/glycogenesis can occur in liver & skeletal muscle
glucagon = peptide hormone synthesized by alpha cells of pancreatic islets of Langerhans in response to low blood sugar
Protein metabolism in the liver
- Ammonia = by-product of protein metabolism that gets transformed/detoxified into urea by the liver -> see decreased urea in liver dysfunction/failure
urea eventually gets transformed into ureic acid then excreted in urine
Lipid processing in the liver
- In duodenal lumen, bile salts break down fats -> enter into enterocytes, transforemd into chylomicrons -> transported to lymphatics via lacteals -> enter circulation thru subclavian vein via thoracic duct -> heart -> aorta -> celiac a. -> hepatic a. -> liver for further processing:
- liver makes triglycerides, cholesterol, lipoproteins (VLDL, LDL, HDL); performs beta oxidation of fatty acids to create ketones for energy (anaerobic glycolysis)
- Clinical scenarios: DKA, hepatic lipidosis; hypocholesterolemia (liver failure)
Albumin
- synthesized in the liver
- functions: transports hormones, FA; maintains oncotic pressure
- hypoalbuminemia: cavitary effusions & edema
Evidence of liver dysfunction/failure:
1. Coagulopathies (decr. production of clotting factors)
2. Hypoalbuminemia (edema, cavitary effusions)
3. Hypoglycemia, Hypocholesterolemia
4. Iron deficiency (liver makes transport and storage proteins for iron transport/storage – transferrin/ferritin)
5. Cholestasis (intra or extrahepatic)
6. Septicemia (failure of liver to process/clear out enteric organisms from entering hepatic vein/systemic circ.)
7. Toxicity (failure of liver to detoxify xenobiotics/other toxins into less lipophilic metabolites to bet excreted in bile or urine for elimination)
8. Decreased urea // ammonia toxicity
9. Jaundice/Icterus (Hepatic – failure of metabolism of bilirubin from unconjugated to conjugated; Post-Hepatic – decr. excretion, cholestasis)
Pre-hepatic hyperbilirubinemia usually due to RBC instability
Cholestasis will lead to a lack of bile acid in SI to absorb fat-soluble vitamins like VitK)
Describe the 3 jaundice classifications
1. Prehepatic: Overproduction of unconnjugated bilirubin -> excess RBC lysis -> impaired uptake of bilirubin by the liver
2. Hepatic: failureof liver to conjugate bilirubin -> excess unconjugated bilirubin
3. Posthepatic: decreased excretion of conjugated bilirubin (intra or extrahepatic obstruction – bile duct obstruction)
unconjugated = indirect, conjugated = direct
Copper hepatopathies
Normal animal: liver absorbs takes up any dietary copper in the SI thru portal circulation, and then utilizes it for its own function, transports to other tissues for use, or excretes it
Copper hepatopathies: Copper builds up -> toxic to hepatocytes elevated liver enzymes-> liver damage/disease
Describe the hepatobiliary system with regards to order of bile flow
Hepatocytes produce bile -> bile flows down canaliculi -> bile ductules -> intralobular ducts -> interlobular ducts -> hepatic ducts -> into gallbladder via cystic duct for storage
Food digestion: gallbladder stimulated to contract by CCK release -> bile flows back out and down into common bile duct, spincter of oddi relaxes, and bile flows out, through major duodenal papilla and into duodenum
Bile acids test: feed animal either a fatty meal or a drug that can induce GB contractions (erythromycin)
Bile modification in the gallbladder
Hepatic bile becomes concentrated 10-to-15 fold in the gallbladder via absorption & secretion of water and electrolytes -> concentrated bile can aid in digestion/absorption of fats
Where do bile acids get reabsorbed?
In the distal ileum via enterohepatic circulation (90% first-pass hepatic extraction, < 5% in fecal losses)
Leptospirosis
Infectious disease that can cause acute liver injury
- AKI with or without elevated hepatic enzymes (hepatocellular or cholestasis)
Common toxins that can cause acute hepatic injury
- xylitol
- amanita mushroom
- Sago palms, blue green algae, aflatoxins
Common drugs that can cause acute heaptic injury or cholestasis
