CETP inhibitor
Template:Short description Template:Infobox drug class
A CETP inhibitor is a member of a class of drugs that inhibit cholesterylester transfer protein (CETP).[1][2][3][4] They are intended to reduce the risk of atherosclerosis (a cardiovascular disease) by improving blood lipid levels. At least three medications within this class have failed to demonstrate a beneficial effect.[5]
Types
These drugs have generally failed in clinical trials, either causing a marked increase in deaths (torcetrapib), or having no meaningful clinical improvement despite HDL increases (dalcetrapib, evacetrapib).
Failed:
- Torcetrapib: failed in 2006 due to excess deaths in Phase III clinical trials.Script error: No such module "Unsubst".
- Dalcetrapib: development halted in May 2012 when Phase III trials failed to show clinically meaningful efficacy.[6]
- Evacetrapib: development discontinued in 2015 due to insufficient efficacy.[7]
Others:
- Anacetrapib: In 2017, the REVEAL trial based on more than 30,000 participants showed a modest benefit of the addition of anacetrapib to statin therapy.[8] Merck halted the development of the drug in 2017, concluding it wasn't sufficiently effective to be a competitive product.[9][10]
- Obicetrapib (TA-8995, AMG-899): Phase II results were reported in 2015 and Phase III trials beginning in 2023.[11]
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Mechanism
Drugs in this class substantially increase HDL cholesterol, lower LDL cholesterol, and enhance reverse cholesterol transport.Script error: No such module "Unsubst".
CETP inhibitors inhibit cholesterylester transfer protein (CETP), which normally transfers cholesterol from HDL cholesterol to very low density or low density lipoproteins (VLDL or LDL). Inhibition of this process results in higher HDL levels and reduces LDL levels.[12] CETP inhibitors do not reduce rates of mortality, heart attack, or stroke in patients already taking a statin.[13]
Pharmacogenomics
In 2015, a pharmacogenomic sub-study of the dal-OUTCOMES clinical trial on 5,749 individuals identified a genetic variant in the ADCY9 gene which modulates response to dalcetrapib. In patients with the rs1967309 'AA' genotype, there was a significant reduction in the rate of cardiovascular events in the dalcetrapib arm whereas non-carriers were at increased risk.[14] Beginning in 2015, the efficacy of dalcetrapib in the genetic sub-population was being investigated in the dal-GenE trial.[15]Template:Update inline
Chemical structures
References
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