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Controlling immune responses by targeting antigens to dendritic cell subsets and B cells

机译:通过将抗原靶向树突状细胞亚群和B细胞来控制免疫反应

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摘要

Delivering antigens in vivo by coupling them to mAbs specific for unique receptors on antigenpresenting cells (APCs) is a promising approach for modulating immune responses. Antigen delivery to receptors found on myeloid dendritic cell (DC) subsets, plasmacytoid DCs and B cells has shown them all to be viable targets to stimulate either the cellular or humoral arms of the immune system. It is now evident that antigen-targeting approaches can also be used to invoke antigenspecific inhibition of immune responses. The outcome of activation versus inhibition is determined by a combination of factors that include the choice of APC, the receptor that is targeted, whether to include an adjuvant and, if so, which adjuvant to employ. In addition to their use as a means to modulate immune responses, antigen-targeting systems are also a useful method to investigate the function of DC subsets and the early mechanistic events that underlie the initiation of both cellular and humoral immune responses. In this review, we focus on the literature surrounding the control of B-cell responses when antigen is delivered to various APC subsets.
机译:通过将抗原与对抗原呈递细胞(APC)上的独特受体具有特异性的mAb偶联,在体内递送抗原是调节免疫反应的一种有前途的方法。抗原传递到髓样树突状细胞(DC),浆细胞样DC和B细胞上发现的受体已显示它们都是刺激免疫系统细胞或体液的可行靶标。现在很明显,抗原靶向方法也可以用来引起免疫应答的抗原特异性抑制。激活与抑制的结果由多种因素决定,这些因素包括选择APC,靶向受体,是否包含佐剂,以及是否使用佐剂。除了将它们用作调节免疫应答的手段外,抗原靶向系统还是一种有用的方法,可用于研究DC亚群的功能以及构成细胞和体液免疫应答启动的早期机制事件。在这篇综述中,我们专注于当抗原被递送到各种APC子集时围绕B细胞反应控制的文献。

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