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可溶性P-选择素、SELP基因多态性与欧美及非裔美国年轻人的动脉粥样硬化风险:年轻人冠状动脉风险发展(CARDIA)研究

Soluble P-selectin, SELP polymorphisms, and atherosclerotic risk in European-American and African-African young adults: the Coronary Artery Risk Development in Young Adults (CARDIA) Study.

作者信息

Reiner Alexander P, Carlson Christopher S, Thyagarajan Bharat, Rieder Mark J, Polak Joseph F, Siscovick David S, Nickerson Deborah A, Jacobs David R, Gross Myron D

机构信息

Departments of Epidemiology, University of Washington, Seattle, WA 98195, USA.

出版信息

Arterioscler Thromb Vasc Biol. 2008 Aug;28(8):1549-55. doi: 10.1161/ATVBAHA.108.169532. Epub 2008 Jun 5.

Abstract

OBJECTIVE

To characterize the genetic and clinical correlates of soluble P-selectin, and the relationship of P-selectin to atherosclerotic risk, in young European-American (EA) and African-American (AA) adults.

METHODS AND RESULTS

We assessed the interrelationships between 25 common SELP polymorphisms, soluble P-selectin, and atherosclerotic risk in 1222 EA and 1072 AA from the longitudinal population-based CARDIA study. Male sex, smoking, blood pressure, and metabolic status were strong cross-sectional correlates of soluble P-selectin among CARDIA subjects aged 33 to 45 years, explaining 13% of the variance. Among EAs, higher soluble P-selectin predicted carotid intima-media thickness (IMT) measured 5 years later, even after accounting for traditional risk factors. Common SELP nucleotide sequence variants explained 11% and 5% of the interindividual variation in soluble P-selectin levels in EAs and AAs, respectively. Four distinct variants contributed to P-selectin phenotype in EAs, including a polymorphism of the 5' SELP haplotype block associated with carotid IMT. Half of the phenotypic variation attributable to SELP in EAs could be explained by the Thr715Pro polymorphism, whereas Val599Leu was more strongly associated with soluble P-selectin among AAs.

CONCLUSIONS

Common SELP polymorphisms were associated with soluble P-selectin and carotid IMT in young adults, but the patterns of association differed between EAs and AAs. These results support the role of P-selectin in the preclinical stages of atherosclerosis.

摘要

目的

在年轻的欧美裔(EA)和非裔美国人(AA)成年人中,对可溶性P-选择素的遗传和临床相关性以及P-选择素与动脉粥样硬化风险的关系进行特征描述。

方法与结果

我们在基于人群的纵向CARDIA研究中的1222名EA和1072名AA中,评估了25种常见的SELP基因多态性、可溶性P-选择素和动脉粥样硬化风险之间的相互关系。在年龄为33至45岁的CARDIA受试者中,男性、吸烟、血压和代谢状态是可溶性P-选择素的强横断面相关因素,可解释13%的变异。在EA中,即使在考虑传统风险因素后,较高的可溶性P-选择素仍可预测5年后测量的颈动脉内膜中层厚度(IMT)。常见的SELP核苷酸序列变异分别解释了EA和AA中可溶性P-选择素水平个体间变异的11%和5%。四个不同的变异体对EA中的P-选择素表型有贡献,包括与颈动脉IMT相关的5'SELP单倍型块的多态性。EA中可归因于SELP的表型变异的一半可由Thr715Pro多态性解释,而Val599Leu在AA中与可溶性P-选择素的相关性更强。

结论

常见的SELP基因多态性与年轻成年人的可溶性P-选择素和颈动脉IMT相关,但EA和AA之间的关联模式不同。这些结果支持P-选择素在动脉粥样硬化临床前期阶段的作用。

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