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高碘酸钠诱导的T细胞有丝分裂:对Ia和白细胞介素1需求的分析

Sodium periodate-induced T cell mitogenesis: an analysis of the requirement for Ia and IL 1.

作者信息

Smith L A, Cohen D A, Lachman L B, Kaplan A M

出版信息

J Immunol. 1985 Aug;135(2):1137-44.

PMID:2989361
Abstract

T lymphocytes oxidized with the mitogen sodium periodate undergo a proliferative response when cultured in the presence of Ia+ accessory cells. However, the exact role(s) the accessory cells play in such a response has not been clearly defined. We have evaluated the role of Ia and the requirement for interleukin 1 (IL 1) in periodate mitogenicity by using the Ia+ cloned tumor cell lines P388AD (Ia+, IL 1 inducible) and P388NA (Ia+, IL 1 noninducible) as accessory cells. P388AD but not P388NA was able to supply accessory cell function to periodate-treated T cells, suggesting that Ia expression alone was not sufficient to reconstitute a response. Monoclonal anti-I-Ad and anti-I-Ed antibody blocked the accessory cell function of P388AD. In addition, monoclonal antibody GK 1.5, directed against the T cell determinant L3T4a, blocked the P388AD/periodate-treated T cell interaction, confirming that this interaction was restricted by class II molecules. Although Ia expression was required, the response was not major histocompatibility complex (MHC) restricted, because allogeneic as well as syngeneic macrophages were capable of supplying accessory cell function to periodate-treated T cells. Exogenous IL 1 alone was able to trigger periodate-treated T cells, suggesting that Ia was required for the induction of IL 1 synthesis by the accessory cells. Furthermore, purified IL 2, devoid of IL 1 activity, was able to fully reconstitute the proliferative response of accessory cell-depleted oxidized T cells to a level equal to that of whole spleen accessory cells or P388AD. These data suggest that periodate-treated T cells can proliferate with IL 1 alone and that Ia+ accessory cells in periodate-mediated T cell mitogenicity may function in the release of IL 1 and the induction of IL 2 synthesis by the T cells.

摘要

用促有丝分裂剂高碘酸钠氧化的T淋巴细胞,在Ia⁺辅助细胞存在的情况下培养时会发生增殖反应。然而,辅助细胞在这种反应中所起的确切作用尚未明确界定。我们通过使用Ia⁺克隆肿瘤细胞系P388AD(Ia⁺,可诱导白细胞介素1(IL-1))和P388NA(Ia⁺,不可诱导IL-1)作为辅助细胞,评估了Ia的作用以及对白细胞介素1(IL-1)在高碘酸钠促有丝分裂活性中的需求。P388AD而非P388NA能够为经高碘酸钠处理的T细胞提供辅助细胞功能,这表明仅Ia表达不足以重建反应。单克隆抗I-Ad和抗I-Ed抗体阻断了P388AD的辅助细胞功能。此外,针对T细胞决定簇L3T4a的单克隆抗体GK 1.5阻断了P388AD/经高碘酸钠处理的T细胞相互作用,证实这种相互作用受II类分子限制。尽管需要Ia表达,但该反应不受主要组织相容性复合体(MHC)限制,因为同种异体以及同基因巨噬细胞都能够为经高碘酸钠处理的T细胞提供辅助细胞功能。单独的外源性IL-1能够触发经高碘酸钠处理的T细胞,这表明Ia是辅助细胞诱导IL-1合成所必需的。此外,不含IL-1活性的纯化IL-2能够完全重建辅助细胞缺失的氧化T细胞的增殖反应,使其达到与全脾辅助细胞或P388AD相当的水平。这些数据表明,经高碘酸钠处理的T细胞仅与IL-1一起就能增殖,并且在高碘酸钠介导的T细胞促有丝分裂活性中,Ia⁺辅助细胞可能在释放IL-1以及诱导T细胞合成IL-2中发挥作用。

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