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首页> 外文期刊>Scientific reports. >Fetal exposure to HIV-1 alters chemokine receptor expression by CD4+T cells and increases susceptibility to HIV-1
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Fetal exposure to HIV-1 alters chemokine receptor expression by CD4+T cells and increases susceptibility to HIV-1

机译:胎儿暴露于HIV-1会改变CD4 + T细胞的趋化因子受体表达,并增加对HIV-1的敏感性

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Absolute numbers of lymphocytes are decreased in uninfected infants born to HIV-1-infected women (HIV-1-exposed). Although the exact mechanism is unknown, fetal exposure to maternal HIV-1-infection could prime the immune system and affect T cell trafficking. We compared the expression of chemokine receptors on cord blood CD4+ T cells from HIV-1-exposed children and healthy controls. At baseline CD4+ T cells had a largely na?ve phenotype. However, stimulation with cytokines resulted in an upregulation of inflammatory response-related chemokine receptors on CD4+ T cells, with HIV-1-exposed infants having a significantly higher frequency of CD4+ T cells expressing, in particularly Th2 associated chemokine receptors (CCR3 p + CD4+ T cells were reduced (p = 0.01) in HIV-1-exposed infants. We further assessed whether the inflammatory phenotype was associated with susceptibility to HIV-1 and detected higher levels of p24 upon in in vitro infection of stimulated CD4+ T cells of HIV-1-exposed infants. In summary, fetal exposure to HIV-1 primes the immune system in the infant leading to an enhanced immune activation and altered T cell homing, with potential ramifications regarding T cell responses and the acquisition of HIV-1 as an infant.
机译:HIV-1感染妇女(暴露于HIV-1)出生的未感染婴儿的淋巴细胞绝对数量减少。尽管确切的机制尚不清楚,但胎儿暴露于母亲的HIV-1感染可能会引发免疫系统并影响T细胞的运输。我们比较了暴露于HIV-1的儿童和健康对照者脐血CD4 + T细胞上趋化因子受体的表达。在基线时,CD4 + T细胞具有幼稚的表型。但是,用细胞因子刺激导致CD4 + T细胞上与炎症反应相关的趋化因子受体的表达上调,而HIV-1暴露婴儿的CD4 + 在HIV-1中表达T细胞,尤其是表达T h 2相关趋化因子受体(CCR3 p + CD4 + T细胞)的细胞减少(p = 0.01)我们进一步评估了炎症表型是否与HIV-1易感性相关,并在体外感染了HIV-1暴露的婴儿的CD4 + T细胞刺激感染后检测到较高的p24水平总之,胎儿暴露于HIV-1会激发婴儿的免疫系统,从而导致增强的免疫激活和改变的T细胞归巢,并可能对婴儿的T细胞反应和HIV-1的获得产生影响。

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