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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >HIV-1 Viral Escape in Infancy Followed by Emergence of a Variant-Specific CTL Response.
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HIV-1 Viral Escape in Infancy Followed by Emergence of a Variant-Specific CTL Response.

机译:婴儿期的HIV-1病毒逃逸,随后出现了变异特异性CTL反应。

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Mutational escape from the CTL response represents a major driving force for viral diversification in HIV-1-infected adults, but escape during infancy has not been described previously. We studied the immune response of perinatally infected children to an epitope (B57-TW10) that is targeted early during acute HIV-1 infection in adults expressing HLA-B57 and rapidly mutates under this selection pressure. Viral sequencing revealed the universal presence of escape mutations within TW10 among B57- and B5801-positive children. Mutations in TW10 and other B57-restricted epitopes arose early following perinatal infection of B57-positive children born to B57-negative mothers. Surprisingly, the majority of B57/5801-positive children exhibited a robust response to the TW10 escape variant while recognizing the wild-type epitope weakly or not at all. These data demonstrate that children, even during the first years of life, are able to mount functional immune responses of sufficient potency to drive immune escape.Moreover, our data suggest that the consequences of immune escape may differ during infancy because most children mount a strong variant-specific immune response following escape, which is rarely seen in adults. Taken together, these findings indicate that the developing immune system of children may exhibit greater plasticity in responding to a continually evolving chronic viral infection.
机译:来自CTL反应的突变逃逸代表了HIV-1感染成年人中病毒多样化的主要驱动力,但是婴儿期的逃逸尚未被描述。我们研究了围产期感染儿童对表位(B57-TW10)的免疫反应,该表位在表达HLA-B57的成年人中急性HIV-1感染的早期就被靶向,并在这种选择压力下迅速突变。病毒测序显示,B57和B5801阳性儿童在TW10中普遍存在逃避突变。围产期感染B57阴性母亲所生的B57阳性儿童后,TW10和其他B57限制性表位的突变就开始出现。出乎意料的是,大多数B57 / 5801阳性儿童对TW10逃避变体表现出强大的反应,而对野生型抗原决定簇的识别却很弱或根本没有。这些数据表明,即使在生命的最初几年中,儿童也能够发挥足够的功能性免疫反应来促进免疫逃逸。此外,我们的数据表明,婴儿期免疫逃逸的后果可能会有所不同,因为大多数儿童都具有较强的免疫力。逃跑后的变体特异性免疫反应,这在成年人中很少见。综上所述,这些发现表明,儿童不断发展的免疫系统在应对持续发展的慢性病毒感染时可能表现出更大的可塑性。

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