New cholesterol methods
needed in wake of failed drugs, heart researchers say
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[April 04, 2016]
By Ransdell Pierson
(Reuters) - New ways of controlling
cholesterol, including possibly directly injecting "good" HDL
cholesterol into patients, need to be studied following the failure of
promising treatments from Eli Lilly, Pfizer Inc and Roche Holding AG,
according to top heart researchers.
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Lilly in October halted a 12,000-patient study of its experimental
drug evacetrapib, an oral medication that in smaller earlier studies
slashed "bad" LDL cholesterol and doubled levels of HDL.
But improved cholesterol levels did not prevent heart attacks and
strokes, diminishing hopes for the approach to treating heart
disease - by raising HDL through blockage of a protein called CETP.
Roche in 2012 scrapped its own CETP inhibitor after it also failed
to help patients. Pfizer's similar drug was discontinued in 2006
after being linked to deaths in trials.
Although Merck & Co continues to develop its own CETP inhibitor in a
30,000-patient study expected to be completed next year, researchers
on Sunday said the failures of the Lilly, Roche and Pfizer drugs
bode poorly for it.
"Merck's drug is the fourth shot on goal for CETP inhibitors, but
with disappointment or lack of success for the other agents you have
to be increasingly pessimistic" about the class of drugs, said Dr.
Stephen Nicholls, deputy director of the South Australian Health and
Medical Research Institute in Adelaide, Australia. He was a lead
investigator for the failed trial of Lilly's drug.
Nicholls and Dr. Steve Nissen, the head of cardiology for the
Cleveland Clinic, who co-lead the evacetrapib study, on Sunday
reviewed the baffling evacetrapib data in a presentation at the
annual scientific sessions of the American College of Cardiology in
Chicago.
"This drug lowered LDL by 37 percent and raised HDL by 130 percent
and had absolutely no effect" on preventing deaths and heart
attacks, Nissen said in an interview.
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Although other ways of raising HDL cholesterol might eventually
prove protective, Nissen said all attempts so far have been
fruitless.
Nicholls said he remains hopeful of future HDL therapies and is
testing whether artificial HDL can be made in the laboratory and
injected directly into high-risk heart patients. "There is
enthusiasm it may be able to shrink plaque" in heart arteries, he
said.
He said he is studying variations of that approach with French
drugmaker Cerenis Therapeutics and the Medicines Company.
Nicholls said another possible approach would be to instruct the
liver to make more HDL.
(Reporting by Ransdell Pierson; Editing by Leslie Adler)
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