- 作者:Jason D. Roberts ; MDa ; Thomas A. Dewland ; MDa ; David V. Glidden ; PhDb ; Thomas J. Hoffmann ; PhDb ; c ; Dan E. Arking ; PhDd ; Lin Y. Chen ; MD ; MSe ; Bruce M. Psaty ; MD ; PhDf ; g ; h ; Jeffrey E. Olgin ; MDa ; Alvaro Alonso ; MD ; PhDi ; Susan R. Heckbert ; MD ; PhDf ; h ; j ; Gregory M. Marcus ; MD ; MASa ;
- 刊名:American Heart Journal
- 出版年:2016
- 出版时间:May 2016
- 年:2016
- 卷:175
- 期:Complete
- 页码:9-17
- 全文大小:525 K
Methods
We performed SNP-RAS inhibitor interaction testing with unadjusted and adjusted Cox proportional hazards models using a discovery (Cardiovascular Health Study) and a replication (Atherosclerosis Risk in Communities) cohort. Additive genetic models were used for the SNP analyses, and 2-tailed P values <.05 were considered statistically significant.
Results
Among 2,796 Cardiovascular Health Study participants, none of the 9 a priori identified candidate SNPs exhibited a significant SNP-drug interaction. Two of the 9 SNPs, rs2106261 (16q22) and rs6666258 (1q21), revealed interaction relationships that neared statistical significance (with point estimates in the same direction for angiotensin-converting enzyme inhibitor only and angiotensin II receptor blocker only analyses), but neither association could be replicated among 8,604 participants in Atherosclerosis Risk in Communities.
Conclusions
Our study failed to identify AF-associated SNP genetic subtypes of AF that derive increased benefit from upstream RAS inhibition for AF prevention. Future studies should continue to investigate the impact of genotype on the response to AF treatment strategies in an effort to develop personalized approaches to therapy and prevention.