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疱疹病毒萨米里原癌基因stpC在生长转化的人T淋巴细胞中的调控,类似于T细胞激活基因的调控。

Regulation of the herpesvirus saimiri oncogene stpC, similar to that of T-cell activation genes, in growth-transformed human T lymphocytes.

作者信息

Fickenscher H, Biesinger B, Knappe A, Wittmann S, Fleckenstein B

机构信息

Institut für Klinische und Molekulare Virologie, Friedrich-Alexander-Universität Erlangen-Nürnberg, Germany.

出版信息

J Virol. 1996 Sep;70(9):6012-9. doi: 10.1128/JVI.70.9.6012-6019.1996.

Abstract

Herpesvirus saimiri strain C488, a T-cell tumor virus of New World primates, transforms human T lymphocytes to stable interleukin-2-dependent growth without need for further stimulation by antigen or mitogen. The transformed cell lines show the phenotype of activated mature T cells and retain many essential features of the primary parental cells, e.g., antigen specificity. In contrast to transformed New World monkey T cells, the human lines do not support lytic growth of the virus, even after chemical stimulation. Here we show that many viral genes remain silent during episomal persistence. However, the viral oncogene stpC is predominantly transcribed and translated to a stable cytoplasmic protein of 20 kDa that is heterogeneously expressed in individual cells. This 1.7-kb mRNA is bicistronic, encoding also Tip, a viral protein interacting with the T-cell-specific tyrosine kinase Lck. stpC/tip transcripts are heavily induced upon stimulation by mitogen or phorbol ester. Block of protein synthesis does not abolish transcription: treatment with cycloheximide greatly induces stpC/tip mRNA levels. Thus, this gene complex is regulated similarly to early T-cell activation genes. Constitutive and induced expression engage different transcription start sites. The T-cell regulation of the viral genes stpC and tip may contribute to the T-cell tropism of growth transformation by herpesvirus saimiri.

摘要

赛氏疱疹病毒C488株是一种新大陆灵长类动物的T细胞肿瘤病毒,可将人T淋巴细胞转化为稳定的依赖白细胞介素-2的生长状态,无需抗原或有丝分裂原的进一步刺激。转化后的细胞系表现出活化成熟T细胞的表型,并保留了原代亲代细胞的许多基本特征,如抗原特异性。与转化后的新大陆猴T细胞不同,即使经过化学刺激,人源细胞系也不支持病毒的裂解生长。我们在此表明,许多病毒基因在游离持续存在期间保持沉默。然而,病毒癌基因stpC主要转录并翻译成一种20 kDa的稳定细胞质蛋白,该蛋白在单个细胞中呈异质性表达。这种1.7 kb的mRNA是双顺反子的,还编码Tip,一种与T细胞特异性酪氨酸激酶Lck相互作用的病毒蛋白。stpC/tip转录本在有丝分裂原或佛波酯刺激后大量诱导。蛋白质合成的阻断并不消除转录:用放线菌酮处理可大大诱导stpC/tip mRNA水平。因此,这种基因复合体的调控方式与早期T细胞活化基因类似。组成型和诱导型表达涉及不同的转录起始位点。病毒基因stpC和tip的T细胞调控可能有助于赛氏疱疹病毒生长转化的T细胞嗜性。

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