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T细胞活化所涉及的信号。I.佛波酯增强反应性,但在有丝分裂原刺激的T细胞增殖诱导过程中不能替代完整的辅助细胞。

Signals involved in T cell activation. I. Phorbol esters enhance responsiveness but cannot replace intact accessory cells in the induction of mitogen-stimulated T cell proliferation.

作者信息

Davis L, Lipsky P E

出版信息

J Immunol. 1985 Nov;135(5):2946-52.

PMID:3876369
Abstract

The role of accessory cells (AC) in the initiation of mitogen-induced T cell proliferation was examined by comparing the effect of intact macrophages (M phi) with that of 4-beta-phorbol 12-myristate 13-acetate (PMA). In high-density cultures, purified guinea pig T cells failed to proliferate in response to stimulation with phytohemagglutinin (PHA), concanavalin A (Con A), or PMA alone. The addition of M phi to PHA or Con A but not PMA-stimulated cultures restored T cell proliferation. The addition of PMA to high-density T cell cultures stimulated with PHA or Con A also permitted [3H]thymidine incorporation, but was less effective than intact M phi in this regard. This action of PMA was dependent on the small number of AC contaminating the T cell cultures as evidenced by the finding that PMA could not support mitogen responsiveness of T cells that had been depleted of Ia-bearing cells by planning, even when these cells were cultured at high density. When PMA was added to T cell cultures supported by optimal numbers of M phi, catalase-reversible suppression of responses was noted. Even in cultures containing catalase, PMA failed to enhance responsiveness above that supported by optimal numbers of M phi. A low-density culture system was used to examine in greater detail the possibility that PMA could completely substitute for M phi in promoting T cells activation. In low-density cultures, mitogen-induced T cell proliferation required intact M phi. PMA could not support responses even in cultures supplemented with interleukin 1-containing M phi supernatants or purified interleukin 2 alone or in combination. Similar results were found in high-density cultures of T cells depleted of Ia-bearing cells. These results support a model of T cell activation in which AC play at least two distinct roles. The initiation of the response requires a signal conveyed by an intact M phi, which cannot be provided by either a M phi supernatant factor or PMA. The response can be amplified by additional M phi or M phi supernatant factors. PMA can substitute for M phi in this regard and can provide the signal necessary for amplification of T cell proliferation supported by small numbers of intact AC.

摘要

通过比较完整巨噬细胞(M phi)与4-β-佛波醇12-肉豆蔻酸酯13-乙酸酯(PMA)的作用,研究了辅助细胞(AC)在丝裂原诱导的T细胞增殖起始过程中的作用。在高密度培养中,纯化的豚鼠T细胞对单独用植物血凝素(PHA)、刀豆蛋白A(Con A)或PMA刺激无增殖反应。将M phi添加到PHA或Con A刺激的培养物中可恢复T细胞增殖,但添加到PMA刺激的培养物中则不能。将PMA添加到用PHA或Con A刺激的高密度T细胞培养物中也能使[3H]胸腺嘧啶核苷掺入,但在这方面不如完整的M phi有效。PMA的这种作用依赖于污染T细胞培养物的少量AC,这一发现表明,即使将这些细胞高密度培养,PMA也不能支持经淘选去除Ia阳性细胞的T细胞的丝裂原反应性。当将PMA添加到由最佳数量的M phi支持的T细胞培养物中时,可观察到过氧化氢酶可逆性抑制反应。即使在含有过氧化氢酶的培养物中,PMA也不能将反应增强到超过最佳数量的M phi所支持的水平。使用低密度培养系统更详细地研究了PMA在促进T细胞活化方面能否完全替代M phi的可能性。在低密度培养中,丝裂原诱导的T细胞增殖需要完整的M phi。即使在补充了含白细胞介素1的M phi上清液或单独或联合纯化的白细胞介素2的培养物中,PMA也不能支持反应。在去除Ia阳性细胞的T细胞高密度培养中也发现了类似结果。这些结果支持了一种T细胞活化模型,其中AC至少发挥两种不同作用。反应的起始需要完整M phi传递的信号,而M phi上清液因子或PMA均不能提供该信号。反应可由额外的M phi或M phi上清液因子放大。在这方面PMA可替代M phi,并可为少量完整AC支持的T细胞增殖放大提供必要信号。

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