首页> 美国卫生研究院文献>The Journal of Experimental Medicine >A novel antigen-processing-defective phenotype in major histocompatibility complex class II-positive CIITA transfectants is corrected by interferon-gamma
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A novel antigen-processing-defective phenotype in major histocompatibility complex class II-positive CIITA transfectants is corrected by interferon-gamma

机译:干扰素-γ纠正主要组织相容性复合体II类阳性CIITA转染子中的新型抗原加工缺陷型。

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摘要

Presentation of exogenous protein antigens to T lymphocytes is based on the intersection of two complex pathways: (a) synthesis, assembly, and transport of major histocompatibility complex (MHC) class II-invariant chain complexes from the endoplasmic reticulum to a specialized endosomal compartment, and (b) endocytosis, denaturation, and proteolysis of antigens followed by loading of antigenic peptides onto newly synthesized MHC class II molecules. It is believed that expression of MHC class II heterodimers, invariant chain and human leukocyte antigen-DM is both necessary and sufficient to reconstitute a functional MHC class II loading compartment in antigen-presenting cells. Expression of each of these essential molecules is under the control of the MHC class II transactivator CIITA. Unexpectedly, however, whereas interferon gamma stimulation does confer effective antigen-processing function to nonprofessional antigen presenting cells, such as melanoma cells, expression of the CIITA transactivator alone is not sufficient. Activation of antigen-specific T cells thus requires additional CIITA-independent factor(s), and such factor(s) can be induced by interferon gamma.
机译:将外源蛋白抗原呈递给T淋巴细胞是基于两个复杂途径的相交:(a)合成,组装和运输主要组织相容性复合物(MHC)II类不变链复合物从内质网到专门的内体区室, (b)抗原的内吞,变性和蛋白水解,然后将抗原性肽装载到新合成的II类MHC分子上。据信,MHC II类异二聚体,不变链和人白细胞抗原-DM的表达对于在抗原呈递细胞中重构功能性II类MHC加载区室而言既必要又充分。这些必需分子中的每一个的表达均受MHC II类反式激活因子CIITA的控制。但是,出乎意料的是,尽管干扰素γ刺激确实将有效的抗原加工功能赋予了非专业的抗原呈递细胞,例如黑素瘤细胞,但仅CIITA反式激活因子的表达还不够。因此,抗原特异性T细胞的活化需要另外的CIITA非依赖性因子,并且这种因子可以被干扰素γ诱导。

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