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高血压的药物基因组学与药物遗传学:最新进展与展望——内收蛋白范例

Pharmacogenomics and pharmacogenetics of hypertension: update and perspectives--the adducin paradigm.

作者信息

Manunta Paolo, Bianchi Giuseppe

机构信息

Division of Nephrology, Dialysis, and Hypertension, University Vita-Salute San Raffale, Via Olgettina 60, 20131 Milan, Italy.

出版信息

J Am Soc Nephrol. 2006 Apr;17(4 Suppl 2):S30-5. doi: 10.1681/ASN.2005121346.

Abstract

There is a growing literature on the potential prospective use of genome information to enhance success in finding new medicines. An example of a prospective efficacy of pharmacogenetic and pharmacogenomics is the detection and impact of adducin polymorphism on hypertension. Adducin is a heterodimeric cytoskeleton protein, the three subunits of which are encoded by genes (ADD1, ADD2, and ADD3) that map to three different chromosomes. A long series of parallel studies in the Milan hypertensive rat strain model of hypertension and humans indicated that an altered adducin function might cause hypertension through an enhanced constitutive tubular sodium reabsorption. In particular, six linkage studies, 18 of 20 association studies, and four of five follow-up studies that measured organ damage in hypertensive patients support the clinical impact of adducing polymorphism. As many modulatory genes and environment affect the adducin activity, the context must be taken into account to measure the clinical effect size of adducins. Pharmacogenomics is giving an important contribution to this end. In particular, the selective advantages of diuretics in preventing myocardial infarction and stroke over other antihypertensive therapies that produce a similar BP reduction in carriers of the mutated adducin may support new strategies that aim to optimize the use of antihypertensive agents for the prevention of hypertension-associated organ damage.

摘要

关于利用基因组信息来提高新药研发成功率的潜在前瞻性应用的文献越来越多。药物遗传学和药物基因组学前瞻性疗效的一个例子是内收蛋白多态性对高血压的检测及影响。内收蛋白是一种异二聚体细胞骨架蛋白,其三个亚基由定位于三条不同染色体的基因(ADD1、ADD2和ADD3)编码。在米兰高血压大鼠品系模型和人类中进行的一系列长期平行研究表明,内收蛋白功能改变可能通过增强肾小管钠的固有重吸收导致高血压。特别是,六项连锁研究、20项关联研究中的18项以及五项测量高血压患者器官损伤的随访研究中的四项都支持内收蛋白多态性的临床影响。由于许多调节基因和环境会影响内收蛋白的活性,在衡量内收蛋白的临床效应大小时必须考虑背景因素。药物基因组学为此做出了重要贡献。特别是,在携带突变内收蛋白的人群中,利尿剂在预防心肌梗死和中风方面相对于其他能产生相似血压降低效果的抗高血压疗法具有选择性优势,这可能支持旨在优化抗高血压药物使用以预防高血压相关器官损伤的新策略。

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