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Target organ damage in African American hypertension: role of APOL1.

机译:非裔美国人高血压中的靶器官损伤:APOL1的作用。

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摘要

Apolipoprotein L1 (APOL1) gene association studies and results of the African American Study of Kidney Disease and Hypertension are disproving the longstanding concept that mild to moderate essential hypertension contributes substantially to end-stage renal disease susceptibility in African Americans. APOL1 coding variants underlie a spectrum of kidney diseases, including that attributed to hypertension (labeled arteriolar or hypertensive nephrosclerosis), focal segmental glomerulosclerosis, and HIV-associated nephropathy. APOL1 nephropathy risk variants persist because of protection afforded from the parasite that causes African sleeping sickness. This breakthrough will lead to novel treatments for hypertensive African Americans with low-level proteinuria, for whom effective therapies are lacking. Furthermore, APOL1 nephropathy risk variants contribute to racially variable allograft survival rates after kidney transplantation and assist in detecting nondiabetic forms of nephropathy in African Americans with diabetes. Discovery of APOL1-associated nephropathy was a major success of the genetics revolution, demonstrating that secondary hypertension is typically present in nondiabetic African Americans with nephropathy.
机译:载脂蛋白L1(APOL1)基因关联研究和非裔美国人肾脏疾病和高血压研究的结果,驳斥了长期存在的观念,即轻度至中度原发性高血压对非裔美国人终末期肾脏疾病的易感性有重大贡献。 APOL1编码变体是一系列肾脏疾病的基础,包括归因于高血压(标记为小动脉或高血压性肾硬化),局灶性节段性肾小球硬化和与HIV相关的肾病。由于引起非洲昏睡病的寄生虫提供了保护,因此APOL1肾病的风险变异仍然存在。这一突破将为缺乏有效疗法的低蛋白尿症高血压非裔美国人带来新疗法。此外,APOL1肾病风险变量有助于肾脏移植后种族差异的同种异体移植存活率,并有助于检测非洲裔美国糖尿病患者的非糖尿病性肾病。与APOL1相关的肾病的发现是遗传学革命的一项重大成功,表明继发性高血压通常存在于患有糖尿病的非糖尿病非裔美国人中。

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