Anti-Hypercholesterolemic Agents

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Anti-Hypercholesterolemic Agents

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Anti-Hypercholesterolemic Agents. Biosynthesis and ... Typically all statins possess side effects. The most dominant side effect, cited in the withdrawal ... – PowerPoint PPT presentation

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Title: Anti-Hypercholesterolemic Agents

1
Anti-Hypercholesterolemic Agents

Biosynthesis and Metabolism of Cholesterol
What is arteriosclerosis?
- Link between arteriosclerosis and cholesterol
Lipoproteins particles
- Structure and classification of lipoprotein
particles
Hyperlipidemias
- Types and overall strategy to control
hyperlipidemias
Anti-hyperlipidemic Agents
- Classes
Statins
Fibrates
Bile Acid Sequestrants
Nicotinic Acid
Ezetimibe

2
Biosynthesis of Cholesterol
HMG CoA reductase
3
Metabolism of Cholesterol
4
Arteriosclerosis
Arteriosclerosis is excessive formation and
deposition of endogeneous products from blood.
In 1984 a 1 drop in serum cholesterol was found
to reduce the risk to coronary heart disease
(CHD) by nearly 2.
5
Lipoprotein Particles
Structure
6
Lipoprotein Particles
Classification of lipoprotein particles
Composition Density Size

Chylomicrons TG gtgt C, CE Low Large
VLDL TG gt CE
IDL CE gt TG
LDL CE gtgt TG
HDL CE gt TG High Small
7
Transport of Lipoprotein Particles
8
Hyperlipidemia
Types of hyperlipidemias
I IIa IIb III IV V
Lipids
Cholesterol N- N- N- N-
Triglycerides N N-
Lipoproteins
Chylomicrons N N N N
VLDL N- N- N-
LDL N-
HDL N N N N-
N normal, increase decrease
slight increase slight decrease
9
Strategy for Controlling Hyperlipidemia
STATINS
HMG CoA reductase
Ezetimibe
BILE ACID SEQUESTRANTS
FIBRATES
10
Anti-hyperlipidemic Drugs - Statins
11
Anti-hyperlipidemic Drugs - Statins
Atorvastatin Cerivastatin

Fluvastatin
Rosuvastatin
Pitavastatin
12
Anti-hyperlipidemic Drugs - Statins
Rationale competitive binding
13
Anti-hyperlipidemic Drugs - Statins
Pharmacokinetic properties of statins case of
cerivastatin
Bioavail. Dosage (mg) Protein Binding Metabolites
Atorvastatin 14 10 80 gt98 Active
Cerivastatin 60 0.2 0.3 gt99 Active
Fluvastatin 24 10 80 98 Active
Lovastatin 5 10 80 gt95
Pravastatin 17 10 40 50
Simvastatin 5 10 - 80 95
Typically all statins possess side effects. The
most dominant side effect, cited in the
withdrawal of cerivastatin, is rhabdomyolysis
(lysis of rhabdomyose) or weakening of skeletal
muscles.
14
Anti-hyperlipidemic Drugs - Statins
Metabolic properties of statins

Rapid first pass metabolism significantly reduces
bioavailability
Metabolism is complex
Extensive conversion between the lactone and
open-chain forms
Glucuronidated forms as well
Other than these three, many other lesser
metabolites
Inhibitors of cytochrome P450 increase
bioavailability of statins .. Greater incidences
of myopathy .. E.g., cyclosporin, gemfibrozil,
erythromycin, itraconazole, etc.
Rhabdomyolysis . A rare complication of statin
treatment . Characterized by breakdown of
muscles .. Release of myoglobin into blood,
which travels to kidneys and stops working of its
tubules . Also muscle breakdown increase K,
which induces cardiac arrythmias and death

15
Anti-hyperlipidemic Drugs - Fibrates

Older generation drugs introduced in 1981
Second most useful anti-hyperlipidemic drugs
Primarily decrease serum triglycerides
Increase lipoprotein catabolism increase TG
usage by the body
activate PPAR-a (peroxisome proliferator-activat
ed receptor a)
Most used in Type III, IV and V hyperlipidemias

16
Anti-hyperlipidemic Drugs - Fibrates
No longer recommended because of an increase in
overall mortality and adverse events
rhabdomyolysis highest PPAR-a affinity ?
clinical trials stopped in the US
17
Anti-hyperlipidemic Drugs Bile Acid Sequestrants