The AHA Guidelines and Scientifi c Statements Handbook
some authorities routinely employ non-HDL-C as a
secondary target in all patients. One advantage of
non-HDL-C is that its measurement does not
require a fasting state for accuracy. Two modalities
of therapy can be employed to achieve the goals of
cholesterol-lowering therapy. These are therapeutic
lifestyle changes (TLC) and drug therapy. Lifestyle
therapies should be employed in all patients. Drug
therapy, however, is often required to achieve the
goals of therapy, particularly in persons at higher
risk.Therapeutic lifestyle changes
ATP III [1] recommends a multifaceted lifestyle
approach to reduce risk for CHD. This approach is
designated therapeutic lifestyle changes (TLC). Its
essential features are:Table 10.5 Drugs affecting lipoprotein metabolism
Drug class, agents
and daily doses
Lipid/lipoprotein
effects Side effects Contraindications Clinical trial resultsHMG CoA reductase
inhibitors (statins)*
LDL-C ↓ 18–55%
HDL-C ↑ 5–15%
TG ↓ 7–30%Myopathy
Increased liver enzymesAbsolute:- Active liver disease
Relative: - Concomitant use of certain
drugs‡ - Chronic liver disease (e.g.
fatty liver, hepatitis C)
Reduced major coronary
events, CHD deaths, need
for coronary procedures,
stroke, and total mortalityBile acid
Sequestrants†
LDL-C ↓ 15–30%
HDL-C ↑ 3–5%
TG No change or
increaseGastrointestinal distress
Constipation
Decreased absorption
of other drugsAbsolute:- Dysbeta-lipoproteinemia
- TG >400 mg/dL
Relative: - TG >200 mg/dL
Reduced major coronary
events and CHD deathsEzetimibe LDL-C ↓ 15–25% Few Benefi t not demonstrated
with controlled trials
Nicotinic acid¥ LDL-C ↓ 5–25%
HDL-C ↑ 15–35%
TG ↓ 20–50%
Flushing
Hyperglycemia
Hyperuricemia (or gout)
Upper GI distress
HepatotoxicityAbsolute:- Chronic liver disease
- Severe gout
Relative: - Diabetes (requires close
monitoring) - Hyperuricemia
- Peptic ulcer disease
Reduced major coronary
events, and possibly total
mortalityFibric acids§ LDL-C ↓ 5–20%
(may be increased in
patients with high TG)
HDL-C ↑ 10–20%
TG ↓ 20–50%
Dyspepsia
Gallstones
MyopathyAbsolute:- Severe renal disease
- Severe hepatic disease
Reduced major coronary
events
Suggestion of increased
non-CHD mortality- Lovastatin (20–80 mg), pravastatin (20–40 mg), simvastatin (20–80 mg), fl uvastatin (20–80 mg), atorvastatin (10–80 mg), resuvastatin (5–40 mg).
† Cholestyramine (4–16 g), colestipol (5–20 g), colesevelam (2.6–3.8 g) Ezetimibe (10 mg).
‡ Cyclosporine, gemfi brozil (or niacin), macrolide antibiotics, various anti-fungal agents and cytochrome P-450 inhibitors.
¥ Immediate release (crystalline) nicotinic acid (1.5–3 g), extended release nicotinic acid (Niaspan®) (1–2 g), sustained release nicotinic acid (1–2 g).
§ Gemfi brozil (600 mg BID), fenofi brate (48–200 mg), clofi brate (1000 mg BID).