Dosage Adjustment - Pre Lecture

Question 1

What is the effects of cardiac failure on absorption?

Answer 1

Mucosal edema and reduced GI blood flow will alter absorption of some drugs

Question 2

What is the effects of cardiac failure on distribution?

Answer 2

1. Decreased tissue perfusion and altered fraction of drug distributed the between plasma and tissue compartment
2. Usual dose can elevate plasma concentration to toxic

Quinidine or lidocaine

Question 3

What is the effects of cardiac failure on elimination?

Answer 3

1. Decreased hepatic perfusion accompanies reduced cardiac output
2. Reduces renal elimination of drug from reduced filtration, increasing toxicity (ahminoglycosides and digoxin)
3. High ER drugs (lidocaine) show limited perfusion limited clearance therefore increase concentrations at low cardiac output
4. Decreased hepatic metabolic capacity by tissue hypoxia and cellular damage

Question 4

What is the major route of elimination for parent drugs and metabolites?

Answer 4

Renal excretion

Question 5

How does renal disease affect absorption?

Answer 5

1. Urea is cleaved therefore gastric pH increases
2. Ammonia and buffers are yielded
3. Nephrotic syndrome
4. Reduction of ferrous iron absorption and other drugs

Question 6

What is nephrotic syndrome?

Answer 6

Resistance to oral diuretics and malabsorption of loo[ diuretics through the edematous intestine

Question 7

How does renal disease affect distribution?

Answer 7

1. Accumulation of acidic substances that compete with drug binding sites (albumin)
2. PK of drugs are altered

Question 8

What is the exception of drug PK changes due to renal disease?

Answer 8

Phenytoin, therapy is guided by plasma concnetration

Question 9

Describe phenytoin properties during renal impairment?

Answer 9

Drug protein binding reduction by competition of accumulated molecules normally cleared by kidney (albumin)

Question 10

How does renal disease affect metabolism?

Answer 10

CYP3A4 of phase 2 are reduced, phase 2 is less affected

Question 11

How does renal disease affect excretion?

Answer 11

1. Filtration and secretion fall into step
2. Excretion is related to GFR

Question 12

What is the main site of metabolism?

Answer 12

Liver

Question 13

What is the solution to liver disease’s unpredictable effects on drug handling?

Answer 13

1. Unsuccessful in determining the correlation between PK of drugs and liver function
2. Close clinical monitoring is better

Question 14

How does liver disease affect absorption?

Answer 14

1. Portal hypertension and hypoalbuminia from mucosal edema
2. anastomoses allow bypassing of first-metabolism increasing bioavailability

Question 15

How does liver disease affect distribution?

Answer 15

Reduced albumin binding -> increased apparent Vd

Question 16

How does liver disease affect metabolism?

Answer 16

Phase I drug metabolism mediated by CYP450 drug is generally reduced

Question 17

What are examples of DDIs?

Answer 17

1. Drug drug
2. Food drug
3. Chemical drug

Question 18

What is a DDI?

Answer 18

Modification of action caused by food or drugs

Question 19

What is unintentional DDI?

Answer 19

Produce adverse reactions in the patient

Question 20

What is intentional DDI?

Answer 20

Provide improved therapeutic response or decrease adverse drug effects

Question 21

What are the mechanisms of DDI?

Answer 21

pharmdynamics
Phamocokinetics

Question 22

What is PD DDI?

Answer 22

Directly at the drug target level or at the level of downstream signaling pathways or by cross-talking pathways

Question 23

What is PK DDI?

Answer 23

Changes in drug exposure parameters (AUC changes)

Question 24

What is the common approach to deal with DDI?

Answer 24

Avoid the interacting combinations by choosing alternative drugs

Question 25

In what cases would alternative therapies not work?

Answer 25

1. Alterations in dose
2. Treatment
   3/ Additional monitoring

Question 26

What makes a drug susceptible to DDI?

Answer 26

1. Low TI
2. Nonlinear PK
3. Steep dose response curve
4. Enzyme inhibiting or inducing properties
5. Genetic variations in drug metabolizing enzymes and/or transporters