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The heat shock protein gp96: a receptor-targeted cross-priming carrier and activator of dendritic cells

机译:热休克蛋白gp96:靶向受体的交叉引发载体和树突状细胞的激活剂

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摘要

Heat shock proteins like gp96 (grp94) are able to induce specific cytotoxic T-cell (CTL) responses against cells from which they originate and are currently studied in clinical trials for use in immunotherapy of tumors. We have recently demonstrated that gp96 binds to at least one yet unidentified receptor restricted to antigen-presenting cells (APCs) like dendritic cells (DCs) but not to T cells. Moreover we have shown, that for CTL activation by gp96-chaperoned peptides receptor-mediated uptake of gp96 by APCs is required. Lately, we have discovered a second function of gp96 when interacting with professional APCs. Gp96 is able to mediate maturation of DCs as determined by up-regulation of MHC class II, CD86 and CD83 molecules, secretion of pro-inflammatory cytokines IL-12 and TNF-α and enhanced T-cell simulatory capacity. Furthermore, the gp96 receptor(s) are down-regulated on mature DCs, suggesting that the gp96 receptor(s) behave similar to other endocytic receptors like CD36, mannose receptor etc. Our findings now provide additional evidence for the remarkable immunogenicity of gp96: first, the existence of specific gp96 receptors on APCs and second, the capacity to activate dendritic cells which is strictly required to enable these highly sophisticated APCs to prime CTL responses.
机译:像gp96(grp94)这样的热激蛋白能够诱导针对其起源细胞的特异性细胞毒性T细胞(CTL)反应,目前正在临床试验中进行研究以用于肿瘤的免疫治疗。我们最近已经证明,gp96结合至少一种尚未识别的受体,该受体限于像树突状细胞(DC)那样的抗原呈递细胞(APC),但不与T细胞结合。此外,我们已经表明,对于gp96陪伴肽的CTL激活,APC需要受体介导的gp96摄取。最近,我们发现与专业APC交互时gp96的第二个功能。通过上调MHC II类,CD86和CD83分子,促炎性细胞因子IL-12和TNF-α的分泌以及增强的T细胞模拟能力,Gp96能够介导DC的成熟。此外,gp96受体在成熟的DC上被下调,表明gp96受体的行为与其他内吞受体类似,例如CD36,甘露糖受体等。我们的发现现在为gp96的卓越免疫原性提供了更多证据:首先,APC上存在特定的gp96受体,其次,激活树突状细胞的能力是使这些高度复杂的APC引发CTL反应所必需的。

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