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产生人γ干扰素的T细胞亚群的鉴定。

Identification of the T cell subset that produces human gamma interferon.

作者信息

O'Malley J A, Nussbaum-Blumenson A, Sheedy D, Grossmayer B J, Ozer H

出版信息

J Immunol. 1982 Jun;128(6):2522-6.

PMID:6176643
Abstract

Positive and negative selection procedures combined with cytofluorographic analysis and lysis with monoclonal antibodies were utilized to identify the T lymphocyte subset that produces human gamma interferon (gamma-IFN) (formerly referred to as "immune" or "type II" interferon) in response to mitogen stimulation. Lymphocytes were separated on the basis of their Fc receptors for IgG or IgM, their nonreactivity with IgM or IgG antibodies, and their reactivity with the monoclonal antibodies OKT4, OKT8, OKT11a, and OKM1. Isolated T cell subsets were incubated with the gamma-IFN inducer, phytohemagglutinin. Three days after induction, the cell supernatants were harvested and assayed for interferon. The T cell subset that produces gamma-IFN was identified as E rosette positive with the phenotype: T gamma, T non-micro, OKM1+, OKT4-, OKT8- and OKT11a+. gamma-IFN production by cells was resistant to doses of x-irradiation that abrogate mitogen-induced T suppressor function but was highly sensitive to low doses of 4-hydroperoxycyclophosphamide. These data demonstrate that gamma-IFN is produced by the T gamma, OKM1+ lymphocyte subset, but these cells may also require the presence of accessory monocytes for elaboration of gamma-IFN. The anti-proliferative activity of gamma-IFN may be responsible for the previously described suppressor function of this subset, and gamma-IFN production by T gamma cells may distinguish this subset from the suppressor/cytotoxic functions of the OKT8+ subset or the mitogen-induced OKT4+ suppressor.

摘要

采用阳性和阴性选择程序,结合细胞荧光分析和单克隆抗体裂解技术,以鉴定在有丝分裂原刺激下产生人γ干扰素(γ-IFN)(以前称为“免疫”或“II型”干扰素)的T淋巴细胞亚群。淋巴细胞根据其对IgG或IgM的Fc受体、与IgM或IgG抗体的无反应性以及与单克隆抗体OKT4、OKT8、OKT11a和OKM1的反应性进行分离。将分离的T细胞亚群与γ-IFN诱导剂植物血凝素一起孵育。诱导三天后,收集细胞上清液并检测干扰素。产生γ-IFN的T细胞亚群被鉴定为E花环阳性,其表型为:Tγ、T非微小、OKM1+、OKT4-、OKT8-和OKT11a+。细胞产生γ-IFN对能消除有丝分裂原诱导的T抑制功能的X射线剂量具有抗性,但对低剂量的4-氢过氧环磷酰胺高度敏感。这些数据表明γ-IFN由Tγ、OKM1+淋巴细胞亚群产生,但这些细胞可能还需要辅助单核细胞的存在才能产生γ-IFN。γ-IFN的抗增殖活性可能是该亚群先前所述抑制功能的原因,Tγ细胞产生γ-IFN可能使该亚群与OKT8+亚群的抑制/细胞毒性功能或有丝分裂原诱导的OKT4+抑制因子区分开来。

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