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CCR5和CCR2基因变异对哥伦比亚血清学不一致夫妇中HIV耐药性/易感性的影响。

Influence of CCR5 and CCR2 genetic variants in the resistance/susceptibility to HIV in serodiscordant couples from Colombia.

作者信息

Zapata Wildeman, Aguilar-Jiménez Wbeimar, Pineda-Trujillo Nicolás, Rojas Winston, Estrada Hernando, Rugeles María T

机构信息

1 Grupo Inmunovirología, Universidad de Antioquia , Medellín, Colombia .

出版信息

AIDS Res Hum Retroviruses. 2013 Dec;29(12):1594-603. doi: 10.1089/aid.2012.0299. Epub 2013 Nov 9.

Abstract

The main genetic factor related to HIV-1 resistance is the CCR5-Δ32 mutation; however, the homozygous genotype is uncommon. The CCR5-Δ32 mutation along with single nucleotide polymorphisms (SNPs) in the CCR5 promoter and the CCR2-V64I mutation have been included in seven human haplogroups (HH) previously associated with resistance/susceptibility to HIV-1 infection and different rates of AIDS progression. Here, we determined the association of the CCR5 promoter SNPs, the CCR5-Δ32 mutation, CCR2-V64I SNP, and HH frequencies with resistance/susceptibility to HIV-1 infection in a cohort of HIV-1-serodiscordant couples from Colombia. Seventy HIV-1-exposed, but seronegative (HESN) individuals, 57 seropositives (SP), and 112 healthy controls (HC) were included. The CCR5-Δ32 mutation and CCR2-V64I SNP were identified by PCR, and the CCR5 promoter SNPs were evaluated by sequencing. None of the individuals exhibited a homozygous Δ32 genotype; the CCR2-I allele was more frequent in HESN (34%) than HC (23%) (p=0.039, OR=1.672). The frequency of the 29G allele was higher in SP than HC (p=0.003, OR=3). HHF2 showed a higher frequency in HC (19%) than SP (9%) (p=0.027), while HHG1 was more frequent in SP (11.1%) than in HC (4.2%) (p=0.019). The AGACCAC-CCR2-I-CCR5 wild-type haplotype showed a higher frequency in SP (14.2%) than in HC (3.7%) (p=0.001). In conclusion, the CCR5-Δ32 allele is not responsible for HIV-1 resistance in this HESN group; however, the CCR2-I allele could be protective, while the 29G allele might increase the likelihood of acquiring HIV-1 infection. HHG1 and the AGACCAC-CCR2-I-CCR5 wild-type haplotype might promote HIV-1 infection while HHF2 might be related to resistance. However, additional studies are required to evaluate the implications of these findings.

摘要

与HIV-1耐药性相关的主要遗传因素是CCR5-Δ32突变;然而,纯合基因型并不常见。CCR5-Δ32突变以及CCR5启动子中的单核苷酸多态性(SNP)和CCR2-V64I突变已被纳入先前与HIV-1感染的耐药性/易感性以及不同艾滋病进展率相关的七个人类单倍群(HH)中。在此,我们在一组来自哥伦比亚的HIV-1血清学不一致的夫妇中确定了CCR5启动子SNP、CCR5-Δ32突变、CCR2-V64I SNP和HH频率与HIV-1感染的耐药性/易感性之间的关联。纳入了70名暴露于HIV-1但血清学阴性(HESN)的个体、57名血清学阳性(SP)个体和112名健康对照(HC)。通过PCR鉴定CCR5-Δ32突变和CCR2-V64I SNP,并通过测序评估CCR5启动子SNP。所有个体均未表现出纯合Δ32基因型;CCR2-I等位基因在HESN中(34%)比在HC中(23%)更常见(p=0.039,OR=1.672)。29G等位基因在SP中的频率高于HC(p=0.003,OR=3)。HHF2在HC中的频率(19%)高于SP(9%)(p=0.027),而HHG1在SP中的频率(11.1%)高于HC(4.2%)(p=0.019)。AGACCAC-CCR2-I-CCR5野生型单倍型在SP中的频率(14.2%)高于HC(3.7%)(p=0.001)。总之,CCR5-Δ32等位基因对该HESN组中的HIV-1耐药性无作用;然而,CCR2-I等位基因可能具有保护作用,而29G等位基因可能增加感染HIV-1的可能性。HHG1和AGACCAC-CCR2-I-CCR5野生型单倍型可能促进HIV-1感染,而HHF2可能与耐药性有关。然而,需要进一步研究来评估这些发现的意义。

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