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能够在胚胎癌干细胞中进行转录的莫洛尼氏鼠肉瘤病毒衍生物获得了一个功能性Sp1结合位点。

Derivatives of Moloney murine sarcoma virus capable of being transcribed in embryonal carcinoma stem cells have gained a functional Sp1 binding site.

作者信息

Prince V E, Rigby P W

机构信息

Laboratory of Eukaryotic Molecular Genetics, National Institute for Medical Research, The Ridgeway, London, England.

出版信息

J Virol. 1991 Apr;65(4):1803-11. doi: 10.1128/JVI.65.4.1803-1811.1991.

Abstract

The long terminal repeat (LTR) sequences of Moloney murine leukemia virus and its closely related derivative Moloney murine sarcoma virus (Mo-MSV) are incapable of directing transcription in embryonal carcinoma (EC) stem cells. The myeloproliferative sarcoma virus, a derivative of Mo-MSV, has several point mutations in the LTR and is transcribed more efficiently to allow productive infection of F9 EC cells. One of these mutations, at -166 with respect to the transcriptional start, creates a consensus binding site for the well-characterized mammalian transcription factor Sp1. We used gel retardation assays to demonstrate that F9 EC cell extracts form several complexes with the myeloproliferative sarcoma virus sequence around -166. One of these complexes involves a murine Sp1-like protein, which has immunoreactivity, DNA binding specificity, and electrophoretic mobility equivalent to those of purified human Sp1 protein. An equivalent complex forms on the corresponding Mo-MSV sequence but with a fivefold-lower affinity. Consistent with these observations, introduction of the single point mutation at -166 into the Mo-MSV LTR, creating a consensus Sp1 binding site, increases expression in F9 EC cells sixfold.

摘要

莫洛尼鼠白血病病毒及其密切相关的衍生物莫洛尼鼠肉瘤病毒(Mo-MSV)的长末端重复序列(LTR)无法在胚胎癌细胞(EC)干细胞中指导转录。髓性增殖性肉瘤病毒是Mo-MSV的衍生物,其LTR中有几个点突变,转录效率更高,从而能够有效地感染F9 EC细胞。其中一个位于转录起始位点-166处的突变,形成了一个已被充分研究的哺乳动物转录因子Sp1的共有结合位点。我们使用凝胶阻滞试验证明,F9 EC细胞提取物与-166附近的髓性增殖性肉瘤病毒序列形成了几种复合物。其中一种复合物涉及一种鼠类Sp1样蛋白,其免疫反应性、DNA结合特异性和电泳迁移率与纯化的人Sp1蛋白相当。在相应的Mo-MSV序列上也形成了类似的复合物,但亲和力低五倍。与这些观察结果一致,将-166处的单点突变引入Mo-MSV LTR,形成一个共有Sp1结合位点,可使F9 EC细胞中的表达增加六倍。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bff0/239988/170e28439060/jvirol00047-0149-a.jpg

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