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在过继转移前的体外培养过程中阻断抗原-抗体复合物对T淋巴细胞的激活。

Blocking antigen-antibody complexes on the T-lymphocyte activation during in vitro incubation before adoptive transfer.

作者信息

Kontiainen S, Mitchison N A

出版信息

Immunology. 1975 Mar;28(3):523-33.

Abstract

Following appropriate immunization of mice with CGG or DNP-CGG spleen cells release antigen upon incubation in vitro. The release can be detected either by 'self-stimulation' of the primed cell population, so that upon adoptive transfer antibodies to CGG and DNP are produced without need for further administration of antigen, or by stimulation of indicator (primed) cells. Boosting mice with antigen in saline following initial immunization with antigen in adjuvant proves the most effective method of loading spleen cells with antigen. A small fraction (10- minus 4- minus 10- minus 5) of the antigen used for boost is retained. The antigen appears to be held on the cell surfaces in the form of antigen-antibody complexes, for it is retained on the cells for up to 13 weeks in the presence of circulating antibody, during which time its capacity to self-stimulate can be inhibited by host serum in vitro. Activated thymus cells take up detectable amounts of antigen-antibody complexes. Complexes obtained by immunization with antigen in adjuvant can be inactivated by trypsinizing spleen cells. Trypsinization of separated T and B cells reveals detectable amounts of complex on the T cells, Complexes detected on T cells in this way are believed to be equivalent to the blocking complexes operative in transplantation and tumour immunity.

摘要

用CGG或DNP - CGG对小鼠进行适当免疫后,脾细胞在体外培养时会释放抗原。这种释放可以通过以下两种方式检测:一是通过致敏细胞群体的“自我刺激”,使得在过继转移后无需进一步给予抗原就能产生针对CGG和DNP的抗体;二是通过刺激指示(致敏)细胞。在用佐剂中的抗原进行初次免疫后,用盐水中的抗原对小鼠进行加强免疫被证明是用抗原加载脾细胞的最有效方法。用于加强免疫的抗原的一小部分(10的负4次方至10的负5次方)会被保留。抗原似乎以抗原 - 抗体复合物的形式附着在细胞表面,因为在存在循环抗体的情况下,它能在细胞上保留长达13周,在此期间其自我刺激的能力在体外可被宿主血清抑制。活化的胸腺细胞会摄取可检测量的抗原 - 抗体复合物。用佐剂中的抗原进行免疫获得的复合物可通过胰蛋白酶处理脾细胞而失活。对分离的T细胞和B细胞进行胰蛋白酶处理后,在T细胞上可检测到一定量的复合物。以这种方式在T细胞上检测到的复合物被认为等同于在移植和肿瘤免疫中起作用的封闭复合物。

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