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Mast Cell-Derived Exosomes Induce Phenotypic and Functional Maturation of Dendritic Cells and Elicit Specific Immune Responses In Vivo

机译:肥大细胞衍生的外泌体诱导树突状细胞表型和功能成熟,并引起体内特异性免疫反应。

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Mast cells (MCs) are considered major players in IgE-mediated allergic responses, but have also recently been recognized as active participants in innate as well as specific immune responses. Recent work provided evidence that MCs are able to activate B and T lymphocytes through the release of vesicles called exosomes. Here we demonstrate that exosomes, which are located in the endocytic pathway, harbor exogenous Ags that associate with other molecules endowed with immunomodulatory functions, including 60- and 70-kDa heat shock proteins. Administration to naive mice of Ag-containing exosomes in the absence of conventional adjuvants elicits specific Ab responses across the MHC II haplotype barrier. We demonstrate that MC-exosomes induce immature dendritic cells (DCs) to up-regulate MHC class II, CD80, CD86, and CD40 molecules and to acquire potent Ag-presenting capacity to T cells. Uptake and processing of Ag-associated exosomes by endogenous DCs were also demonstrated. Finally, exosome-associated heat shock proteins are critical for the acquisition by DCs of the Ag-presenting function. This work demonstrates a heretofore unrecognized collaborative interaction between MCs and DCs leading to the elicitation of specific immune responses.
机译:肥大细胞(MCs)被认为是IgE介导的过敏反应的主要参与者,但最近也被公认是先天性和特异性免疫反应的活跃参与者。最近的工作提供了证据,表明MC能够通过释放称为囊泡的囊泡来激活B和T淋巴细胞。在这里,我们证明了位于胞吞途径中的外泌体具有与其他具有免疫调节功能的分子(包括60 kDa和70 kDa热激蛋白)结合的外源Ag。在没有常规佐剂的情况下,对初生小鼠施用含Ag的外泌体会引起跨MHC II单倍型障碍的特异性Ab反应。我们证明,MC外泌体诱导未成熟的树突状细胞(DCs)上调MHC II类,CD80,CD86和CD40分子,并获得有力的Ag呈现能力的T细胞。还证明了内源性DC对Ag相关外泌体的吸收和加工。最后,与外泌体相关的热休克蛋白对于DC获得Ag呈递功能至关重要。这项工作证明了迄今为止无法识别的MC和DC之间的协作相互作用导致特定的免疫反应的引发。

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