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静息和致敏的T淋巴细胞在生长和淋巴因子释放方面表现出对刺激(抗原呈递细胞)的不同需求。

Resting and sensitized T lymphocytes exhibit distinct stimulatory (antigen-presenting cell) requirements for growth and lymphokine release.

作者信息

Inaba K, Steinman R M

出版信息

J Exp Med. 1984 Dec 1;160(6):1717-35. doi: 10.1084/jem.160.6.1717.

DOI:10.1084/jem.160.6.1717
PMID:6239901
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2187515/
Abstract

Previous studies have shown that unprimed or resting T lymphocytes will grow and release lymphokines when stimulated by dendritic cells (DC). We now have examined the stimulatory requirements for antigen-primed or blast-transformed T cells. The latter were derived from dendritic/T cell clusters that developed during the primary mixed leukocyte reaction (MLR). The specificity of the blasts was established by a binding assay in which most T cells aggregated small B lymphocytes of the appropriate haplotype within 2 h at 4 or 37 degrees C. Since unprimed T cells did not aggregate allogeneic B cells, we suggest that DC induce T lymphocytes to express additional functioning receptors for antigen. Lyt-2-T blasts did not grow or release interleukin 2 or B cell helper factors unless rechallenged with specific alloantigen, whereupon growth (generation time of 14-18 h) and lymphokine release rapidly resumed. The blasts could be stimulated by allogeneic macrophages, B cells, and B lymphoblasts, whereas the primary MLR was initiated primarily by DC. responsiveness appeared restricted to the I region of the major histocompatibility complex, and varied directly with the level of Ia antigens on the stimulator cells. The interaction of B cells and T blasts was bidirectional. The T blasts would grow and form B cell helper factors, while the B cells grew and secreted antibody. However, the efficacy of T cell-mediated antibody formation was enhanced some 10-fold by the addition of specific antigen. Therefore, responses of resting helper T cells, then, are initiated by antigen plus DC. Once sensitized, T blasts interact independently with antigen presented by other leukocytes.

摘要

以往的研究表明,未致敏或静止的T淋巴细胞在受到树突状细胞(DC)刺激时会生长并释放淋巴因子。我们现在研究了对抗原致敏或经胚细胞转化的T细胞的刺激需求。后者源自初次混合淋巴细胞反应(MLR)期间形成的树突状/T细胞簇。胚细胞的特异性通过结合试验确定,在该试验中,大多数T细胞在4℃或37℃下2小时内聚集了合适单倍型的小B淋巴细胞。由于未致敏的T细胞不会聚集同种异体B细胞,我们认为DC诱导T淋巴细胞表达额外的功能性抗原受体。Lyt-2-T胚细胞不会生长或释放白细胞介素2或B细胞辅助因子,除非再次用特异性同种异体抗原刺激,此时生长(代时为14 - 18小时)和淋巴因子释放会迅速恢复。胚细胞可被同种异体巨噬细胞、B细胞和B淋巴母细胞刺激,而初次MLR主要由DC启动。反应性似乎局限于主要组织相容性复合体的I区,并与刺激细胞上Ia抗原的水平直接相关。B细胞与T胚细胞的相互作用是双向的。T胚细胞会生长并形成B细胞辅助因子,而B细胞会生长并分泌抗体。然而,通过添加特异性抗原,T细胞介导的抗体形成效率提高了约10倍。因此,静止辅助性T细胞的反应由抗原加DC启动。一旦致敏,T胚细胞会与其他白细胞呈递的抗原独立相互作用。

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Resting and sensitized T lymphocytes exhibit distinct stimulatory (antigen-presenting cell) requirements for growth and lymphokine release.静息和致敏的T淋巴细胞在生长和淋巴因子释放方面表现出对刺激(抗原呈递细胞)的不同需求。
J Exp Med. 1984 Dec 1;160(6):1717-35. doi: 10.1084/jem.160.6.1717.
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