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Pharmacogenomic application of the haptoglobin genotype in the treatment of HDL dysfunction

机译:触珠蛋白基因型在HDL功能障碍治疗中的药物基因组学应用

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摘要

An emerging paradigm of research has suggested that in the setting of diabetes mellitus (DM) the quality or function of high-density lipoprotein (HDL) may be a determinant of cardiovascular disease risk. Specific structural modifications of HDL protein and lipid components, resulting from oxidative modification, have been proposed to mediate HDL’s loss of the ability to promote cholesterol efflux (reverse cholesterol transport), serve as an antioxidant and anti-inflammatory agent. Therefore, inhibiting HDL oxidative modification would be expected to improve its function and provide cardioprotection. Nevertheless, antioxidant strategies to reduce cardiovascular events from atherosclerosis in DM have failed. It has been proposed that this failure may have been due to the inadequate nature of patient selection. High dose antioxidant therapy may only provide benefit to a subset of DM individuals with oxidatively modified HDL. We will review evidence that haptoglobin (Hp) identifies such individuals who can be successfully treated with vitamin E. These data will suggest that a pharmacogenomic approach utilizing the Hp genotype may be useful in identifying individuals who will benefit from antioxidant therapy.
机译:新兴的研究范例表明,在糖尿病(DM)的情况下,高密度脂蛋白(HDL)的质量或功能可能是心血管疾病风险的决定因素。已经提出了通过氧化修饰对HDL蛋白和脂质成分进行特定的结构修饰,以介导HDL丧失促进胆固醇外排(胆固醇逆向转运)的能力,用作抗氧化剂和消炎药。因此,抑制HDL的氧化修饰有望改善其功能并提供心脏保护作用。然而,减少DM中由动脉粥样硬化引起的心血管事件的抗氧化剂策略已失败。已经提出,这种失败可能是由于患者选择的性质不足引起的。高剂量抗氧化剂治疗可能仅对具有氧化修饰的HDL的部分DM个体提供益处。我们将审查证据,以结合珠蛋白(Hp)识别可以成功用维生素E治疗的个体。这些数据将表明,利用Hp基因型的药物基因组学方法可能有助于鉴定将受益于抗氧化剂治疗的个体。

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