Saturday, August 23, 2008

 

PPI en aspirin

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Proton pump inhibitor use with aspirin secondary prevention 'cost-effective'


19 August 2008

MedWire News: Proton pump inhibitor (PPI) cotherapy in conjunction with low-dose aspirin for secondary cardiovascular disease prevention is cost-effective in average-risk patients at over-the counter (OTC) cost, but only in high risk patients at prescription cost, Markov model findings indicate.

Sameer Saini (University of Michigan, Ann Arbor, USA) and co-authors of the study explain that the risk for upper gastrointestinal bleeding (UGIB) in patients taking aspirin for secondary prevention can be minimized with PPI cotherapy.

To look at whether long-term PPI cotherapy is cost-effective from the perspective of a long-term medical insurance payer such as Medicare, the researchers developed a Markov model to compare the costs of secondary prevention with low-dose aspirin and low-dose aspirin plus PPI in patients with coronary heart disease who were aged at least 50 years.

Assuming patients had a starting age of 65 years, were at average risk for UGIB (had no established risk factors other than age), and that PPI therapy reduces the risk for UGIB by 66% (based on randomized data in high-risk Asian patients), the model indicated that using a PPI with aspirin rather than aspirin alone would reduce the lifetime risk for UGIB events from 9.5% to 3.1% and that for UGIB-related death from 1.4% to 0.4%.

At OTC cost, the authors say that the PPI plus aspirin combination in this scenario was cost effective, at a cost-effectiveness ratio per life-year gained of $40,090.

Patient age, the effectiveness of PPI for reducing UGIB, and the cost of PPI all affected how cost-effective the combination would be, with younger age, lower efficacy, and higher costs making the ratio less favorable.

Cost-effectiveness ratios per life-year gained varied from $35,315 up to $94,578 across starting ages ranging from 50 to 80 years.

And increasing the PPI cost to prescription prices made the strategy cost-ineffective in all but the highest risk patients. The cost-effectiveness ratio per life-year gained for patients at high risk (4-fold higher than average) for UGIB was $100,000 in 50-year-olds, $51,000 in 65-year-olds, and $25,000 in 80-year-olds.

In an accompanying editorial, Michael Pignone (University of North Carolina, Chapel Hill, USA) pointed out that achieving the cost-effectiveness ratios under $50,000 would currently require use of the generic omeprazole magnesium, which has not been evaluated for preventive efficacy.

Also, he said: "We need greater confidence about the risk for adverse effects of PPI from fractures, pneumonia, or other unrecognized conditions."

Arch Intern Med 2008; 168: 1684-1690



© Copyright Current Medicine Group Ltd, 2008

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# posted by roodbont @ 12:40 AM 0 comments

Thursday, August 21, 2008

 

statin myopathy

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Volume 359:789-799 August 21, 2008 Number 8
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SLCO1B1 Variants and Statin-Induced Myopathy — A Genomewide Study
The SEARCH Collaborative Group

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ABSTRACT

Background Lowering low-density lipoprotein cholesterol with statin therapy results in substantial reductions in cardiovascular events, and larger reductions in cholesterol may produce larger benefits. In rare cases, myopathy occurs in association with statin therapy, especially when the statins are administered at higher doses and with certain other medications.

Methods We carried out a genomewide association study using approximately 300,000 markers (and additional fine-mapping) in 85 subjects with definite or incipient myopathy and 90 controls, all of whom were taking 80 mg of simvastatin daily as part of a trial involving 12,000 participants. Replication was tested in a trial of 40 mg of simvastatin daily involving 20,000 participants.

Results The genomewide scan yielded a single strong association of myopathy with the rs4363657 single-nucleotide polymorphism (SNP) located within SLCO1B1 on chromosome 12 (P=4x10–9). SLCO1B1 encodes the organic anion–transporting polypeptide OATP1B1, which has been shown to regulate the hepatic uptake of statins. The noncoding rs4363657 SNP was in nearly complete linkage disequilibrium with the nonsynonymous rs4149056 SNP (r2=0.97), which has been linked to statin metabolism. The prevalence of the rs4149056 C allele in the population was 15%. The odds ratio for myopathy was 4.5 (95% confidence interval [CI], 2.6 to 7.7) per copy of the C allele, and 16.9 (95% CI, 4.7 to 61.1) in CC as compared with TT homozygotes. More than 60% of these myopathy cases could be attributed to the C variant. The association of rs4149056 with myopathy was replicated in the trial of 40 mg of simvastatin daily, which also showed an association between rs4149056 and the cholesterol-lowering effects of simvastatin. No SNPs in any other region were clearly associated with myopathy.

Conclusions We have identified common variants in SLCO1B1 that are strongly associated with an increased risk of statin-induced myopathy. Genotyping these variants may help to achieve the benefits of statin therapy more safely and effectively. (Current Controlled Trials number, ISRCTN74348595 [controlled-trials.com] .)


# posted by roodbont @ 12:39 AM 0 comments

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