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Association of Y chromosome haplogroup I with HIV progression, and HAART outcome.

机译:Y染色体单倍体I与HIV进展和HAART结果的关联。

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The host genetic basis of differential outcomes in HIV infection, progression, viral load set point and highly active retroviral therapy (HAART) responses was examined for the common Y haplogroups in European Americans and African Americans. Accelerated progression to acquired immune deficiency syndrome (AIDS) and related death in European Americans among Y chromosome haplogroup I (Y-I) subjects was discovered. Additionally, Y-I haplogroup subjects on HAART took a longer time to HIV-1 viral suppression and were more likely to fail HAART. Both the accelerated progression and longer time to viral suppression results observed in haplogroup Y-I were significant after false-discovery-rate corrections. A higher frequency of AIDS-defining illnesses was also observed in haplogroup Y-I. These effects were independent of the previously identified autosomal AIDS restriction genes. When the Y-I haplogroup subjects were further subdivided into six I subhaplogroups, no one subhaplogroup accounted for the effects on HIV progression, viral load or HAART response. Adjustment of the analyses for population stratification found significant and concordant haplogroup Y-I results. The Y chromosome haplogroup analyses of HIV infection and progression in African Americans were not significant. Our results suggest that one or more loci on the Y chromosome found on haplogroup Y-I have an effect on AIDS progression and treatment responses in European Americans.
机译:针对欧美人和非裔美国人中常见的Y单倍型,研究了HIV感染,进展,病毒载量设定点和高活性逆转录病毒治疗(HAART)反应差异结果的宿主遗传基础。发现在Y染色体单倍体I(Y-I)受试者中,欧洲人加速发展为获得性免疫缺陷综合症(AIDS)和相关死亡。此外,接受HAART的Y-I单倍型受试者接受HIV-1病毒抑制的时间更长,并且更有可能失败HAART。假发现率校正后,在单倍型Y-1中观察到的加速进展和更长的病毒抑制时间均很显着。在Y-I单倍型人群中也发现了更多的艾滋病定义疾病。这些作用独立于先前确定的常染色体AIDS限制基因。当将Y-1单倍型受试者进一步细分为6个I单倍型时,没有一个单倍型可以解释对HIV进展,病毒载量或HAART反应的影响。人口分层分析的调整发现显着和一致的单倍型Y-1结果。非裔美国人对HIV感染和进展的Y染色体单倍群分析不显着。我们的结果表明,单倍体Y-1上Y染色体上的一个或多个基因座对欧洲裔美国人的AIDS进展和治疗反应有影响。

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