TRIM5α 136Q, CCR5启动子59029G和CCR264I等位基因影响儿童和青少年HIV的进展

IF 2.6 Q2 GENETICS & HEREDITY Application of Clinical Genetics Pub Date : 2019-11-07 eCollection Date: 2019-01-01 DOI:10.2147/TACG.S205335
Béatrice Dambaya, Céline Nguefeu Nkenfou, Linda Mekue, Georges Této, Nicole Ngoufack, Georgia Ambada, Njiokou Flobert, Vittorio Colizzi, Ndjolo Alexis
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Their blood was collected every 6 months and used for biological and host genetic polymorphism analyses. Five genes were genotyped: <i>Trim5α (R136Q), CCR5</i> promoter <i>59029G, CCR2-64I, SDF 3'A</i> and <i>CCR5-Δ32</i>. Exposed non-infected (HEU) and unexposed HIV negative children (HNEU) were recruited as control groups.</p><p><strong>Results: </strong>Among the 5 genes studied, the protective allele of Trim5α (R136Q) was present in all LTNP and in 72.34% and 2.56% of SP and RP, respectively (p<0.0001). The CCR5 promoter 59029G/G was also more present in LTNP and SP than in RP (p=0.02; p=0.04). The protective CCR2-64I homozygous genotype was almost absent in all groups, only the heterozygous genotype was present with a significant difference between RP vs SP (p=0.0001), and SP vs LTNP (p=0.0002). The CCR2-∆32 was completely absent either as homozygous or heterozygous genotype. It was a monomorphic allele. 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引用次数: 0

摘要

背景儿童在艾滋病毒感染和疾病进展方面表现出不同程度的脆弱性。这种差异对受感染儿童的后续行动提出了挑战。在这里,我们研究了这种变异性背后的原因,重点是一些与宿主相关的HIV基因。方法我们对570名1至19岁的喀麦隆儿童和青少年进行了筛查。其中,137人在2010年至2015年的4年时间里进行了随访。签署代理同意书后,儿童和青少年根据年龄、CD4计数、病毒载量和临床症状分为长期非进展型(LTNP)、缓慢进展型(SP)和快速进展型(RP)。每6个月采集一次他们的血液,用于生物和宿主基因多态性分析。对5个基因进行了基因分型:Trim5α(R136Q)、CCR5启动子59029G、CCR2-64I、SDF 3 A和CCR5-Δ32。暴露的未感染(HEU)和未暴露的HIV阴性儿童(HNEU)被招募为对照组。结果在所研究的5个基因中,保护性等位基因Trim5α(R136Q)在所有LTNP中均存在,在SP和RP中分别存在72.34%和2.56%(p<0.0001)。CCR5启动子59029G/G在LTNP和SP中的存在也高于RP(p=0.02;p=0.04),只有杂合基因型存在,RP与SP(p=0.0001)和SP与LTNP(p=0.0002)之间存在显著差异。CCR2-∆32完全不存在,无论是纯合型还是杂合型。这是一个单态等位基因。SDF 3âA在我们的研究人群中几乎以纯合野生型基因型的形式存在,与疾病获得和疾病进展无关。结论在研究中描述的5个基因中,Trim 5α(R136Q)、CCR5启动子59029G和CCR2V64I等位基因与儿童和青少年HIV感染的进展有关。
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TRIM5α 136Q, CCR5 Promoter 59029G And CCR264I Alleles Impact The Progression Of HIV In Children And Adolescents.

Background: Children show various degrees of vulnerability regarding HIV infection and disease progression. This disparity presents challenges for the follow-up of infected children. Here we investigated reasons behind this variability focusing on some host-related HIV genes.

Methods: We screened 570 Cameroonian children and adolescents, aged 1 to 19 years old. Among them, 137 were followed over 4 years, from 2010 to 2015. Upon signing a proxy consent, children and adolescents were classified according to their age, CD4 count, viral load and clinical symptoms as long-term non-progressors (LTNP), slow progressors (SP) and rapid progressors (RP). Their blood was collected every 6 months and used for biological and host genetic polymorphism analyses. Five genes were genotyped: Trim5α (R136Q), CCR5 promoter 59029G, CCR2-64I, SDF 3'A and CCR5-Δ32. Exposed non-infected (HEU) and unexposed HIV negative children (HNEU) were recruited as control groups.

Results: Among the 5 genes studied, the protective allele of Trim5α (R136Q) was present in all LTNP and in 72.34% and 2.56% of SP and RP, respectively (p<0.0001). The CCR5 promoter 59029G/G was also more present in LTNP and SP than in RP (p=0.02; p=0.04). The protective CCR2-64I homozygous genotype was almost absent in all groups, only the heterozygous genotype was present with a significant difference between RP vs SP (p=0.0001), and SP vs LTNP (p=0.0002). The CCR2-∆32 was completely absent either as homozygous or heterozygous genotype. It was a monomorphic allele. SDF 3'A was almost present as homozygous wild-type genotype in our study population and was associated neither to disease acquisition nor to disease progression.

Conclusion: Among the 5 genes described in the study, Trim 5α (R136Q), CCR5 promoter 59029G and CCR2V64I alleles were associated to the progression of HIV infection in children and adolescents.

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来源期刊
Application of Clinical Genetics
Application of Clinical Genetics Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
5.40
自引率
0.00%
发文量
20
审稿时长
16 weeks
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