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Cross-linking the B7 Family Molecule B7-DC Directly Activates Immune Functions of Dendritic Cells

机译:B7家族分子B7-DC的交联直接激活树突状细胞的免疫功能。

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摘要

B7-DC molecules are known to function as ligands on antigen-presenting cells (APCs), enhancing T cell activation. In this study, cross-linking B7-DC with the monoclonal antibody sHIgM12 directly potentiates dendritic cell (DC) function by enhancing DC presentation of major histocompatibility complex–peptide complexes, promoting DC survival; and increasing secretion of interleukin (IL)-12p70, a key T helper cell type 1 promoting cytokine. Furthermore, ex vivo treatment of DCs or systemic treatment of mice with sHIgM12 increases the number of transplanted DCs that reach draining lymph nodes and increases the ability of lymph node APCs to activate naive T cells. Systemic administration of the antibody has an equivalent effect on DCs transferred at a distant site. These findings implicate B7-DC expressed on DCs in bidirectional communication. In addition to the established costimulatory and inhibitory functions associated with B7-DC, this molecule can also function as a conduit for extracellular signals to DCs modifying DC functions.
机译:已知B7-DC分子可充当抗原呈递细胞(APC)上的配体,从而增强T细胞活化。在这项研究中,B7-DC与单克隆抗体sHIgM12的交联通过增强主要组织相容性复合物-肽复合物的DC呈递,直接增强树突状细胞(DC)的功能,从而促进DC的存活。并增加白介素(IL)-12p70(一种关键的1型T辅助细胞促进细胞因子)的分泌。此外,DC的离体治疗或用sHIgM12全身性治疗小鼠会增加到达排水淋巴结的已移植DC的数量,并增加淋巴结APC激活幼稚T细胞的能力。抗体的全身性给药对在远处转移的DC具有等效作用。这些发现暗示在双向通信中DC上表达的B7-DC。除了已建立的与B7-DC相关的共刺激和抑制功能外,该分子还可以充当细胞外信号传导至DC的通道,从而修饰DC功能。

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