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Monocyte-derived macrophages exhibit distinct and more restricted HIV-1 integration site repertoire than CD4+ T cells

机译:单核细胞衍生的巨噬细胞表现出明显且更受限制的HIV-1集成位点曲目,而不是CD4 + T细胞

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The host genetic landscape surrounding integrated HIV-1 has an impact on the fate of the provirus. Studies analysing HIV-1 integration sites in macrophages are scarce. We studied HIV-1 integration site patterns in monocyte-derived macrophages (MDMs) and activated CD4(+) T cells derived from seven antiretroviral therapy (ART)-treated HIV-1-infected individuals whose cells were infected ex vivo with autologous HIV-1 isolated during the acute phase of infection. A total of 1,484 unique HIV-1 integration sites were analysed. Their distribution in the human genome and genetic features, and the effects of HIV-1 integrase polymorphisms on the nucleotide selection specificity at these sites were indistinguishable between the two cell types, and among HIV-1 isolates. However, the repertoires of HIV-1-hosting gene clusters overlapped to a higher extent in MDMs than in CD4(+) T cells. The frequencies of HIV-1 integration events in genes encoding HIV-1-interacting proteins were also different between the two cell types. Lastly, HIV-1-hosting genes linked to clonal expansion of latently HIV-1-infected CD4(+) T cells were over-represented in gene hotspots identified in CD4(+) T cells but not in those identified in MDMs. Taken together, the repertoire of genes targeted by HIV-1 in MDMs is distinct from and more restricted than that of CD4(+) T cells.
机译:围绕综合HIV-1的宿主遗传景观对潜意识的命运产生了影响。分析巨噬细胞HIV-1集成位点的研究是稀缺的。我们研究了单核细胞衍生的巨噬细胞(MDMS)中的HIV-1集成位点模式和衍生自七种抗逆转录病毒治疗(ART)的活化的CD4(+)T细胞(ART)-treated HIV-1感染的个体,其细胞被自体HIV感染前体内1在感染的急性期间分离。分析了总共1,484个独特的HIV-1集成站点。它们在人类基因组和遗传特征中的分布,以及HIV-1整合酶多态性对这些位点的核苷酸选择特异性的影响在两种细胞类型和HIV-1分离物之间难以区分。然而,HIV-1宿主基因簇的再胃部簇在MDMS中重叠而不是CD4(+)T细胞。编码HIV-1相互作用蛋白基因中HIV-1集成事件的频率也不同于两种细胞类型。最后,在CD4(+)T细胞中鉴定的基因热点,但不在MDMS中鉴定的基因热点中结合到潜伏的潜在HIV-1感染的CD4(+)T细胞的HIV-1宿主基因。携带在一起,在MDMS中由HIV-1靶向的基因的曲目不同,与CD4(+)T细胞的HIV-1不同。

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