Hyperlipidemia Flashcards
What are the steps in the pathogenesis of atherosclerosis?
- endothelial injury
- LDL accumulation and oxidation
- monocytes adhere –> become macrophages that phagocytose oxidized LDL –>
- foam cells
- platelets adhere
- smooth muscle cell migration deposits collagen
- necrosis, plaque lysis
What is the 1st step in treatment of all forms of primary hyperlipidemia?
diet modification
What are 3 ways in which HDL is anti-atherogenic?
- reverse cholesterol transport
- protections against endothelial dysfunction
- inhibits oxidative stress
Which drug is the best agent to increase HDL? What 2 other effects does this drug have and how does it achieve them?
Niacin–>
- increased HDL: reduced hepatic clearance of ApoAI (important HDL lipoprotein);
- decreases triglycerides: decreases lipolysis in adipose tissue, leading to lowered FFA transport to liver;
- decreaess LDL: Reduction of liver triglyceride synthesis, leading to less hepatic VLDL (thus, LDL) production
Name 4 less serious side effects and 3 medically serious side effects of Niacin that limits its use to only 50% of eligible patients
Less Serious:
flushing/pruritis face & upper trunk; rash; acanthosis nigricans; dyspepsia
More Serious:
hepatotoxicity, hyperglycemia, hyperuricemia
In which patients is Niacin contraindicated?
patients with diabetes mellitus and/or gout
may cause hyperglycemia and hyperuricemia
Name 3 Fibric Acid derivatives (fibrates). Which of these is no longer used due to increased bile lithogenicity?
Clofibrate (not used anymore - causes gallstone formation)
Gemfibrozil
Fenofibrate
In what subtype of hyperlipidemic patients is Gemfibrozil and those in its class used? Possible mechanism of action?
(fibrates)
used mostly in patients with severe hypertriglyceridemias
–> may interact w/peroxisome proliferator-activated receptor (esp. PPARα) to stimulate LPL synthesis (enhance TG-rich lipoprotein clearance)
What are 2 adverse effects of Fenofibrate and those in its class?
(Fibrates)
- Potentiates oral anticoagulants (displace from albumin)
- myositis flu-like syndrome in 5% [Combination w/statin inadvisable due to higher myositis risk]
What is the only hypolipidemic class indicated for use in children? Why?
Bile Acid Sequestrants –>
VERY safe- not absorbed from intestine
Name 3 Bile Acid Sequestrants. What other drug may they be combined with for standard treatment of hyperlipidemia?
Cholestyramine
Colestipol
Colesevelam
[last 2 are combined with statins in standard treatment]
What is the mechanism of action of Colestipol and others in its class?
(bile acid sequestrants)
Very positively charged resins binds negative charged bile acids–> The large size inhibits reabsorption and increasing bile/cholesterol excretion–> depletion in liver stores of bile acid leads to increase in LDL receptors in liver (to make more cholesterol/bile), decreasing LDL in blood by ~25%
What are 4 adverse effects of Colesevelam and those in its class?
(bile acid sequestrants)
- impairs fat soluble vitamin absorption
- binds other drugs (e.g., cardiac glycosides, coumarins) and interferes with their absorption
- GI effects: bloating, dyspepsia, constipation
- causes slight increase in TGs [contraindicated in hypertriglyceridemia]
Name 7 statins. Which 2 are prodrugs that must be modified in the liver to active form?
Mevastatin (Compactin) Lovastatin (Mevacor) - prodrug Simvastatin (Zocor) - prodrug Pravastatin (Pravachol) Fluvastatin (Lescol) Atorvastatin (Lipitor) Rosuvastatin (Crestor)
What is the mechanism of action of Mevastatin and others in its class?
HMG-CoA Reductase competitive inhibitors:
Inhibits cholesterogenesis in liver–> less free cholesterol leads to activation of SREBP, a membrane-bound transcription factor that increases LDL-R synthesis and lessens degradation–> increased removal of LDL from blood (25-60%)
reduced cholesterol synthesis decreases VLDL synthesis–> lowers TG (25%)
