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Pharmacokinetic Changes in Hepatic Dysfunction

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Title: Pharmacokinetic Changes in Hepatic Dysfunction

1
Pharmacokinetic Changes in Hepatic Dysfunction

Jennifer Dugan, Pharm.D., BCPS

2
Liver Physiology

Receives blood from hepatic artery and portal
vein
Between cords of hepatocytes are sinusoids
Blood is collected into hepatic vein, flows into
inferior vena cava
Bile flows in opposite direction of blood
System allows for rapid exchange of drugs and
metabolites between plasma and hepatocytes,
hepatocytes and bile.

3
Factors Affecting Movement

Blood flow
Protein Binding
Mechanism of transfer
Diffusion
Carrier-mediated

4
Biotransformation

Phase I (nonsynthetic/functionalization)
Oxidation
Reduction
Hydrolysis
Phase II (synthetic/conjugation)
Links to endogenous substrate (glucuronic acid,
sulfate, glycine)
Methylation
Acetylation

5
Oxidation

Enzyme systems primarily in hepatocytes near
central vein
Enzymes
Cytochrome P450
NADPH-dependent P450 reductase

6
Conjugation

Frequently preserved in liver disease
Most drugs undergoing Phase II biotransformation
are conjugated with glucuronic acid
Low-affinity, high capacity pathway

7
Sulfation

Occurs near portal vein
High affinity, low capacity
Need ATP to get cofactor to transfer inorganic
sulfate to drug molecules
Limited availability of inorganic sulfate
This is reason you get nonlinear PK with
acetaminophen

8
Extrahepatic Metabolism

Kidney
GI
Intestinal bacteria or enzyme systems in
epithelial cells
Lung
Many pulmonary toxicities may be from local toxic
or reactive metabolites
Skin

9
Hepatic Excretion

Some drug molecules are not metabolized before
excretion
May see decreased metabolites or accumulation of
metabolites if excretion impaired
To be eliminated, the drug must cross sinusoidal
membrane and return to blood as it flows toward
central vein, or be transported into bile
Biliary transport, like active secretion in the
kidneys, may be inhibited competitively

10
Other Liver Functions

Protein synthesis
Glucose homeostasis
Lipid and lipoprotein synthesis
Vitamin storage
Clotting factor synthesis
Bile acid synthesis

11
Hepatic Extraction Ratio (EH)

Extraction Ratio tells of efficiency, not extent
EH Ca (pv ha) Cv (just venous)
Ca
Factors affecting EH
Blood flow
Protein binding
Hepatic intrinsic clearance (ability of
hepatocytes to remove drug from liver water when
blood flow, protein binding, and translocation to
the site of metabolism or elimination are not
rate-limiting)

12
Hepatic Clearance

Volume of blood from which drug is removed
completely per unit time
CLH QH EH
Hepatic clearance is not equal to systemic
clearance

13
Bioavailability

F? 1- EH
Fraction of the absorbed dose that reaches the
systemic circulation
Will approximate 1.0 for dugs that are not
extracted efficiently
If extracted efficiently, hepatic disease
alterations in first pass extraction may
significantly alter systemic availability

14
Volume of Distribution

Vd VB VT (fub/fut)
May or may not be affected by liver disease,
depending on extravascular distribution and
tissue binding

15
Drugs Exhibiting gt20 Decrease in Clearance in
Chronic Liver Disease

Lidocaine
Meperidine
Metoprolol
Propranolol
Verapamil

Caffeine
Diazepam
Erythromycin
Metronidazole
Theophylline

16
Extraction Ratios

Low Extraction Ratio
Dosage adjustment only necessary when intrinsic
clearance changes (ie cirrhosis)
If total drug changes, unbound concentration
should remain constant
Examples- phenytoin, warfarin, diazepam,
chlordiazepoxide, naproxen, sulindac, valproic
acid, theophylline, bumetanide, triamterene

17
Low Extraction Ratio Drugs in Normal Patients
Total
Conc
Free (unbound)
time
Drug displaced
18
Low Extraction Ratio Drugs in Liver Disease
19
Low Extraction Ratio Drugs in Liver Disease

Decreased intrinisic clearance (hepatic cell mass
and function ).
Often increased fu ( serum albumin).
No significant change in F.
Overall, total Cl is generally reduced two to
four-fold (increasing plasma levels).However,
free (active) plasma levels may be increased by
much more
Therefore, highly bound drugs may need gt 2 or
4-fold dosage reduction

20
Extraction Ratios

High Extraction Ratio
Hepatic clearance rate-limited by liver blood
flow
Protein binding doesnt change clearance but
changes amount unbound
No change in hepatic clearance as fraction
unbound increases

21
High Extraction Ratio Drugs in Liver Disease

Increased plasma level of drug (especially if
taken orally)
Decreased hepatic blood flow leads to decreased
clearance
Intra-hepatic and extra-hepatic shunting of blood
leads to decreased first pass effect, thereby
increasing oral bioavailability

22
High Extraction Ratio Drugs in Liver Disease
23
PK Factors influencing clearance

Thyroid
Pituitary
Pancreas
Gender
Pregnancy
Race
Nutritional Status

24
Drug Interactions

Interaction has to exceed intrapatient clearance
variability
Induction increases intrinsic clearance of
unbound drug
Inhibition decreases intrinsic clearance of
unbound drug
Interaction usually results in a lt50 change in
clearance

25
Drug interactions

Total clearance has an inverse relationship to
Css
If drug clearance increases from 10 to 15, Css
will decrease 33
If drug clearance decreases from 10 to 5, Css
will increase 100

26
Drug interactions

Magnitude of interaction based on
Fraction of clearance due to metabolism
Hepatic extraction ratio
Route of administration
For a high EH drug, cimetidine inhibits oral
clearance by 30-50, but inhibits systemic
clearance 15-30
Patients with chronic liver disease are likely
more sensitive to inhibition

27
Pharmacodynamic Changes in Liver Disease

sensitivity to oral anticoagulants
CNS sensitivity to depressants
risk of hypokalemia with some loop diuretics

28
Chronic Liver Disease

gt50 decrease in P450 content
High extraction drugs are more affected in
portosystemic shunting
Low extraction drugs are more sensitive to
intrinsic clearance changes
Bioavailability may be significantly ? secondary
to ? first pass in highly extracted drugs
Vd increased in pts with ? albumin or ascites

Inflammation
Fibroblasts secrete collagen while damaged cells
replaced
Collagen accumulates in sinusoidal space
Basement membrane w/o microvilli forms
Interferes with exchange
Hepatocytes regenerate
Clustered formations form nodules
Distorted liver architecture increases portal
pressure and promoting shunts

30
Progression

Alcohol can cause fatty infiltration
Microsomal enzyme induction
Increased conversion to hepatotoxic metabolites
May be asymptomatic
Alcoholic Hepatitis (Steatonecrosis)
Not all alcoholics have cirrhosis

31
Signs and Symptoms of Cirrhosis

Anorexia
Nausea
Abdominal Discomfort
Weakness
Weight loss
Fatigability

Hepatosplenomegaly
Jaundice
Ascites
Peripheral Edema
Spider angiomas

32
Portal Hypertension

Portal vein collects blood from abdominal portion
of digestive tract, pancreas, and spleen
transports to liver
Blood must pass through capillary system under
high pressure
Blood flow can be blocked by nodules that
compress and distort hepatic veins, ot thrombosis
or obstruction

33
Portal Hypertension

Portal hypertension facilitates formation of
collateral blood vessels and intrahepatic shunts
Low pressure veins in esophagus, anterior
abdominal wall, splenic veins, rectum
Esophageal and gastric varices, ascites,
hemorrhoids, splenic enlargement

34
Pharmacokinetic and Pharmacodynamic Changes