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Absence of H186R Polymorphism in Exon 4 of the AP0BEC3G Gene among North Indian Individuals

机译:北印度人AP0BEC3G基因第4外显子缺乏H186R多态性

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AIDS restriction genes have been defined in which allelic variations have been shown to influence infection or disease progression. Members of the APOBEC family of cellular polynucleotide cytidine deaminases (e.g., APOBEC3G) have been identified as a host factor that inhibits HIV-1 replication. It deaminates cytidine to uridine in nascent minus-strand viral DNA, inducing G-to-A hypermutation in the plus-strand viral DNA. The impact of codon-changing variant APOBEC3G H186R polymorphism on HIV-1 susceptibility and progression is not clear. We conducted genetic risk association study in HIV-1-exposed seronegative (HES; n = 50) individuals, HIV-1 seronegative (HSN; n = 320) healthy control, and HIV-1 seropositive patients (HSP; n = 190). The APO-BEC3G H186R genotypes were identified by polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) method in DNA extracted from peripheral blood and confirmed by direct sequencing the randomly selected 58 samples. Frequency of rare homozygous RR (mutant type) and HR (heterozygous mutant) genotype was 0% while HH (wild type) was 100% among North Indians. In conclusion, we demonstrated that no genetic H186R polymorphism in exon 4 of APOBEC3G gene is found and therefore neither associated with differential susceptibility to HIV-1 infection/progression among North Indians.
机译:已经定义了AIDS限制基因,其中等位基因变异已显示影响感染或疾病进展。细胞多核苷酸胞苷脱氨基酶APOBEC家族成员(例如APOBEC3G)已被鉴定为抑制HIV-1复制的宿主因子。它在新生的负链病毒DNA中将胞苷脱氨化为尿苷,从而在正链病毒DNA中引起G-to-A超突变。尚不清楚改变密码子的变体APOBEC3G H186R多态性对HIV-1易感性和进展的影响。我们对暴露于HIV-1的血清阴性(HES; n = 50)个体,HIV-1血清阴性(HSN; n = 320)健康对照和HIV-1血清阳性患者(HSP; n = 190)进行了遗传风险关联研究。通过聚合酶链反应-限制性片段长度多态性(PCR-RFLP)方法鉴定外周血DNA中的APO-BEC3G H186R基因型,并通过对随机选择的58个样品进行直接测序来确认。在北印度人中,罕见的纯合子RR(突变型)和HR(杂合突变体)基因型的频率为0%,而HH(野生型)的基因型为100%。总之,我们证明在APOBEC3G基因的第4外显子中没有发现遗传的H186R多态性,因此与北印度人对HIV-1感染/进展的易感性没有关系。

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