首页> 外文期刊>Immunobiology: Zeitschrift fur Immunitatsforschung >Induction of ssDNA-binding autoantibody secreting B cell immunity during murine malaria infection is a critical part of the protective immune responses
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Induction of ssDNA-binding autoantibody secreting B cell immunity during murine malaria infection is a critical part of the protective immune responses

机译:鼠疟疾感染过程中诱导ssDNA结合的自身抗体分泌B细胞免疫是保护性免疫反应的关键部分

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Although it has been hypothesized that autoimmune-like phenomena may play a critical role in the protective immune responses to both human and animal malaria, there are still no evidence-based data to support this view. In this study we demonstrate that the majority of anti-single stranded (ss) DNA autoantibody secreting B cells were confined to B220+CD21+CD23- cells and that these cells expanded significantly in the spleen of C57BL/6 mice infected with Plasmodium yoelii 17X non-lethal (PyNL). To determine the role of ssDNA-binding autoantibody secreting B cell responses in murine malaria, we conjugated generation 6 (poly) amidoamine dendrimer nanoparticles with ssDNA to deplete ssDNA-binding autoreactive B cells in vivo. Our data revealed that 55.5% of mice died after DNA-coated nanoparticle-mediated in vivo depletion of ssDNA-specific autoreactive B cells and subsequent challenge using PyNL. Adoptive transfer of B cells with ssDNA specificity to mice, followed by PyNL infection, caused a later appearance and inhibition of parasitemia. The possible mechanism by which the ssDNA-binding autoantibody secreting B cells is involved in the protection against murine malaria has also been demonstrated.
机译:尽管已经假设类似自身免疫的现象可能在对人类和动物疟疾的保护性免疫反应中起关键作用,但仍然没有基于证据的数据来支持这种观点。在这项研究中,我们证明了大多数分泌抗单链(ss)DNA自身抗体的B细胞均局限于B220 + CD21 + CD23-细胞,并且这些细胞在感染了约氏疟原虫17X的C57BL / 6小鼠的脾脏中显着扩增非致命(PyNL)。为了确定分泌ssDNA的自身抗体分泌B细胞应答在鼠类疟疾中的作用,我们将6代(聚)酰胺基胺树枝状大分子纳米粒子与ssDNA结合,以在体内消耗ssDNA结合的自身反应性B细胞。我们的数据显示55.5%的小鼠在DNA包覆的纳米粒子介导的ssDNA特异性自身反应性B细胞体内耗竭以及随后使用PyNL攻击后死亡。将具有ssDNA特异性的B细胞过继转移给小鼠,然后感染PyNL,导致其后出现并抑制寄生虫病。还已经证明了分泌ssDNA的自身抗体分泌B细胞参与针对鼠类疟疾的保护的可能机制。

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