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1型人类免疫缺陷病毒env V3环序列的基因分型分析:初治人群中28对感染母婴共受体使用情况的生物信息学预测

Genotypic analysis of human immunodeficiency virus type 1 env V3 loop sequences: bioinformatics prediction of coreceptor usage among 28 infected mother-infant pairs in a drug-naive population.

作者信息

Duri Kerina, Soko White, Gumbo Felicity, Kristiansen Knut, Mapingure Munyaradzi, Stray-Pedersen Babill, Muller Fredrik

机构信息

Department of Immunology, College of Health Sciences, Parirenyatwa Hospital, University of Zimbabwe, Harare, Zimbabwe.

出版信息

AIDS Res Hum Retroviruses. 2011 Apr;27(4):411-9. doi: 10.1089/aid.2010.0142. Epub 2010 Oct 23.

Abstract

We sought to predict virus coreceptor utilization using a simple bioinformatics method based on genotypic analysis of human immunodeficiency virus types 1 (HIV-1) env V3 loop sequences of 28 infected but drug-naive women during pregnancy and their infected infants and to better understand coreceptor usage in vertical transmission dynamics. The HIV-1 env V3 loop was sequenced from plasma samples and analyzed for viral coreceptor usage and subtype in a cohort of HIV-1-infected pregnant women. Predicted maternal frequencies of the X4, R5X4, and R5 genotypes were 7%, 11%, and 82%, respectively. Antenatal plasma viral load was higher, with a mean log(10) (SD) of 4.8 (1.6) and 3.6 (1.2) for women with the X4 and R5 genotypes, respectively, p = 0.078. Amino acid substitution from the conserved V3 loop crown motif GPGQ to GPGR and lymphadenopathy were associated with the X4 genotype, p = 0.031 and 0.043, respectively. The maternal viral coreceptor genotype was generally preserved in vertical transmission and was predictive of the newborn's viral genotype. Infants born to mothers with X4 genotypes were more likely to have lower birth weights relative to those born to mothers with the R5 genotype, with a mean weight (SD) of 2870 (±332) and 3069 (±300) g, respectively. These data show that at least in HIV-1 subtype C, R5 coreceptor usage is the most predominant genotype, which is generally preserved following vertical transmission and is associated with the V3 GPGQ crown motif. Therefore, antiretroviral-naive pregnant women and their infants can benefit from ARV combination therapies that include R5 entry inhibitors following prediction of their coreceptor genotype using simple bioinformatics methods.

摘要

我们试图使用一种基于基因型分析的简单生物信息学方法,通过对28名孕期感染但未接受过药物治疗的女性及其感染婴儿的人类免疫缺陷病毒1型(HIV-1)env V3环序列进行分析,来预测病毒共受体的利用情况,并更好地了解垂直传播动力学中的共受体使用情况。从血浆样本中对HIV-1 env V3环进行测序,并在一组HIV-1感染的孕妇中分析病毒共受体的使用情况和亚型。预测的X4、R5X4和R5基因型的母亲频率分别为7%、11%和82%。产前血浆病毒载量较高,X4和R5基因型女性的平均log(10)(标准差)分别为4.8(1.6)和3.6(1.2),p = 0.078。从保守的V3环冠基序GPGQ到GPGR的氨基酸替代以及淋巴结病与X4基因型相关,p分别为0.031和0.043。母亲的病毒共受体基因型在垂直传播中通常得以保留,并可预测新生儿的病毒基因型。与R5基因型母亲所生的婴儿相比,X4基因型母亲所生的婴儿出生体重更有可能较低,平均体重(标准差)分别为2870(±332)克和3069(±300)克。这些数据表明,至少在HIV-1 C亚型中,R5共受体使用是最主要的基因型,其在垂直传播后通常得以保留,并与V3 GPGQ冠基序相关。因此,未接受过抗逆转录病毒治疗的孕妇及其婴儿在使用简单生物信息学方法预测其共受体基因型后,可从包括R5进入抑制剂的抗逆转录病毒联合疗法中获益。

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