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环孢菌素A对特定小鼠T细胞克隆功能的影响:抑制增殖、淋巴因子分泌及细胞毒性。

Effects of cyclosporin A on functions of specific murine T cell clones: inhibition of proliferation, lymphokine secretion and cytotoxicity.

作者信息

Weiss J, Schwinzer B, Kirchner H, Gemsa D, Resch K

出版信息

Immunobiology. 1986 Apr;171(3):234-51. doi: 10.1016/S0171-2985(86)80007-9.

Abstract

Allospecific T lymphocyte clones with different functions were generated from spleen cells of C 57/Bl6 mice following sensitization in vitro by a one-way mixed lymphocyte culture (MLC) with irradiated DBA/2 spleen cells. The clones were propagated in vitro in the presence of interleukin 2 (IL 2) and restimulation with stimulator cells. In these clones Cyclosporin A (CSA) was tested for its suppressive effect on different T lymphocyte functions. The antigen-dependent proliferation of a helper clone (HTL) was totally inhibited by 50 ng/ml CSA. Proliferation induced by simultaneous administration of antigen and IL 2 was partially suppressed in all helper and cytotoxic clones (CTL). The IL 2-driven proliferation in the absence of antigen was also suppressed between 25-70% by the immunosuppressive drug. Secretion of macrophage activating factor (MAF) and interferon (IFN) by HTL and CTL in response to antigen or mitogen was reduced dose dependently by CSA. Concentrations of 50 ng/ml CSA diminished lymphokine secretion to approximately 10% of controls, also when excess IL 2 was present. Cytotoxicity, previously described to be insensitive to the drug, could be suppressed by 50 ng/ml CSA to a various extent, from 40-70%, in different cytotoxic clones when the effector cells were preincubated with CSA for 1 h or more. Conclusively, the data suggest that CSA interferes generally with the activation of T lymphocyte clones.

摘要

通过用经照射的DBA/2脾细胞进行单向混合淋巴细胞培养(MLC)在体外致敏后,从C 57/Bl6小鼠的脾细胞中产生了具有不同功能的同种特异性T淋巴细胞克隆。这些克隆在白细胞介素2(IL-2)存在的情况下于体外增殖,并用刺激细胞进行再刺激。在这些克隆中测试了环孢菌素A(CSA)对不同T淋巴细胞功能的抑制作用。50 ng/ml的CSA完全抑制了辅助性克隆(HTL)的抗原依赖性增殖。在所有辅助性和细胞毒性克隆(CTL)中,同时给予抗原和IL-2诱导的增殖均受到部分抑制。在无抗原的情况下,IL-2驱动的增殖也被这种免疫抑制药物抑制了25%-70%。CSA剂量依赖性地降低了HTL和CTL对抗原或丝裂原反应时巨噬细胞激活因子(MAF)和干扰素(IFN)的分泌。50 ng/ml的CSA浓度也将淋巴因子分泌减少至对照的约10%,即使存在过量的IL-2时也是如此。先前描述为对该药物不敏感的细胞毒性,当效应细胞与CSA预孵育1小时或更长时间时,在不同的细胞毒性克隆中可被50 ng/ml的CSA不同程度地抑制,抑制程度为40%-70%。总之,数据表明CSA通常会干扰T淋巴细胞克隆的激活。

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