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李斯特菌 p60 蛋白的一个含 LysM 和 SH3 结构域的区域刺激辅助细胞促进宿主 NK 细胞的激活。

A LysM and SH3-domain containing region of the Listeria monocytogenes p60 protein stimulates accessory cells to promote activation of host NK cells.

机构信息

Integrated Department of Immunology, National Jewish Health and University of Colorado School of Medicine, Denver, Colorado, United States of America.

出版信息

PLoS Pathog. 2011 Nov;7(11):e1002368. doi: 10.1371/journal.ppat.1002368. Epub 2011 Nov 3.

Abstract

Listeria monocytogenes (Lm) infection induces rapid and robust activation of host natural killer (NK) cells. Here we define a region of the abundantly secreted Lm endopeptidase, p60, that potently but indirectly stimulates NK cell activation in vitro and in vivo. Lm expression of p60 resulted in increased IFNγ production by naïve NK cells co-cultured with treated dendritic cells (DCs). Moreover, recombinant p60 protein stimulated activation of naive NK cells when co-cultured with TLR or cytokine primed DCs in the absence of Lm. Intact p60 protein weakly digested bacterial peptidoglycan (PGN), but neither muropeptide recognition by RIP2 nor the catalytic activity of p60 was required for NK cell activation. Rather, the immune stimulating activity mapped to an N-terminal region of p60, termed L1S. Treatment of DCs with a recombinant L1S polypeptide stimulated them to activate naïve NK cells in a cell culture model. Further, L1S treatment activated NK cells in vivo and increased host resistance to infection with Francisella tularensis live vaccine strain (LVS). These studies demonstrate an immune stimulating function for a bacterial LysM domain-containing polypeptide and suggest that recombinant versions of L1S or other p60 derivatives can be used to promote NK cell activation in therapeutic contexts.

摘要

李斯特菌(Lm)感染会迅速而强烈地激活宿主自然杀伤(NK)细胞。在这里,我们定义了大量分泌的 Lm 内肽酶 p60 的一个区域,该区域能够在体外和体内有力但间接刺激 NK 细胞的激活。Lm 表达 p60 导致与经处理的树突状细胞(DC)共培养的幼稚 NK 细胞产生更多的 IFNγ。此外,当与 TLR 或细胞因子预刺激的 DC 共培养时,重组 p60 蛋白在不存在 Lm 的情况下也能刺激幼稚 NK 细胞的激活。完整的 p60 蛋白可弱消化细菌肽聚糖(PGN),但 RIP2 识别肽聚糖 muropeptide 或 p60 的催化活性都不是 NK 细胞激活所必需的。相反,免疫刺激活性映射到 p60 的 N 端区域,称为 L1S。在细胞培养模型中,用重组 L1S 多肽处理 DC 可刺激其激活幼稚 NK 细胞。此外,L1S 处理可在体内激活 NK 细胞,并增加宿主对弗氏柠檬酸杆菌活疫苗株(LVS)感染的抵抗力。这些研究表明,一种含有细菌 LysM 结构域的多肽具有免疫刺激功能,并表明重组 L1S 或其他 p60 衍生物可用于在治疗环境中促进 NK 细胞的激活。

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