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干扰素-γ不是一种抗病毒物质,而是T淋巴细胞的生长促进因子。

Interferon-gamma is not an antiviral, but a growth-promoting factor for T lymphocytes.

作者信息

Landolfo S, Gariglio M, Gribaudo G, Jemma C, Giovarelli M, Cavallo G

机构信息

Department of Microbiology, Medical School, University of Torino, Italy.

出版信息

Eur J Immunol. 1988 Apr;18(4):503-9. doi: 10.1002/eji.1830180403.

Abstract

The effects of interferon (IFN)-gamma or IFN-alpha/beta on virus yield, (2'-5')oligo(A) synthetase activation, H-2 antigen expression and proliferation of T lymphocytes have been investigated. Under the culture conditions used, vesicular stomatitis virus or Semliki Forest virus replication in T cells was not impaired by the addition of IFN-gamma, whereas it was completely inhibited by the addition of IFN-alpha/beta. In contrast, B cell lines, macrophage-transformed cell lines and fibroblasts were fully protected by both IFN-gamma as well as IFN-alpha/beta following virus infection. The lack of sensitivity of T lymphocytes to the antiviral effects of IFN-gamma was not due to absence of specific membrane receptors, since in saturation binding experiments with 125I-labeled murine IFN-gamma most T cell lines displayed a number of binding sites and a degree of affinity comparable to those found on B cells, which are fully sensitive to IFN-gamma antiviral activity. Analysis of IFN-induced dsRNA-dependent (2'-5')oligo(A) synthetase activity, one of the biochemical markers for cellular responses to IFN, showed that it was not induced in T lymphocytes after IFN-gamma treatment, whereas IFN-alpha/beta induced high levels. Both IFN-gamma and IFN-alpha/beta enhanced H-2 antigen expression on T cells as well as on cells of different histological type. Moreover, when IFN-gamma was tested for its antiproliferative activity on T cells, it was found to consistently potentiate the response of these cells to mitogens or growth factors, rather than inhibit their proliferation. Taken as a whole these results suggest that on T lymphocytes IFN-gamma should not be regarded as an antiviral agent, but rather as a modulator of T cell growth and functional differentiation, transducing intracellular signals dissimilar to those observed with target cells of different origin.

摘要

已经研究了干扰素(IFN)-γ或IFN-α/β对病毒产量、(2'-5')寡聚腺苷酸合成酶激活、H-2抗原表达以及T淋巴细胞增殖的影响。在所使用的培养条件下,添加IFN-γ不会损害水疱性口炎病毒或Semliki森林病毒在T细胞中的复制,而添加IFN-α/β则会完全抑制其复制。相反,病毒感染后,B细胞系、巨噬细胞转化细胞系和成纤维细胞受到IFN-γ以及IFN-α/β的完全保护。T淋巴细胞对IFN-γ抗病毒作用缺乏敏感性并非由于缺乏特异性膜受体,因为在使用125I标记的鼠IFN-γ进行的饱和结合实验中,大多数T细胞系显示出的结合位点数量和亲和力程度与对IFN-γ抗病毒活性完全敏感的B细胞上发现的相当。对IFN诱导的依赖双链RNA的(2'-5')寡聚腺苷酸合成酶活性(细胞对IFN反应的生化标志物之一)的分析表明,IFN-γ处理后T淋巴细胞中该酶未被诱导,而IFN-α/β可诱导高水平表达。IFN-γ和IFN-α/β均增强了T细胞以及不同组织学类型细胞上的H-2抗原表达。此外,当检测IFN-γ对T细胞的抗增殖活性时,发现它始终增强这些细胞对有丝分裂原或生长因子的反应,而不是抑制其增殖。总体而言,这些结果表明,对于T淋巴细胞,IFN-γ不应被视为抗病毒剂,而应被视为T细胞生长和功能分化的调节剂,它转导的细胞内信号与不同来源的靶细胞所观察到的信号不同。

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