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SNF5转录因子基因的失活消除了HIV-1整合酶在酵母中表达所诱导的致死表型。

Inactivation of the SNF5 transcription factor gene abolishes the lethal phenotype induced by the expression of HIV-1 integrase in yeast.

作者信息

Parissi V, Caumont A, Richard de Soultrait V, Dupont C H, Pichuantes S, Litvak S

机构信息

CNRS UMR-5097. IFR 66 'Pathologies Infectieuses', Université Victor Segalen Bordeaux 2. 146 rue Leo Saignat, 33076, Bordeaux, France.

出版信息

Gene. 2000 Apr 18;247(1-2):129-36. doi: 10.1016/s0378-1119(00)00108-6.

Abstract

The ubiquitous human transcription factor Ini1 has been shown to interact with HIV-1 integrase (IN) and to stimulate in vitro the reactions catalyzed by this enzyme. We have previously used a yeast model to study the effect of HIV-1 IN expression (Caumont, A.B., Jamieson, G.A., Pichuantes, S., Nguyen, A.T., Litvak, S., Dupont, C. -H., 1996. Expression of functional HIV-1 integrase in the yeast Saccharomyces cerevisiae leads to the emergence of a lethal phenotype: potential use for inhibitor screening. Curr. Genet. 29, 503-510). Here, we describe the effect of the inactivation of the gene encoding for SNF5, a yeast transcription factor homologous to Ini1, on the lethality induced by the expression of HIV-1 IN in yeast. We observed that the retroviral IN was unable to perform its lethal activity in cells where the SNF5 gene has been disrupted, suggesting that SNF5 may play a role in the lethal effect induced by IN in yeast. SNF5 inactivation affects neither yeast viability nor expression of HIV-1 IN. Given the homology between SNF5 and its human counterpart Ini1, our results suggest that this factor may be important for IN activity in infected cells. Moreover, given the important role proposed for this transcription factor in the integration step and the fact that it is dispensable for cell viability, the interaction between Ini1/ySNF5 and HIV-1 IN should become a potential target in the search for new antiretroviral agents.

摘要

普遍存在的人类转录因子Ini1已被证明可与HIV-1整合酶(IN)相互作用,并在体外刺激该酶催化的反应。我们之前使用酵母模型研究了HIV-1 IN表达的影响(Caumont, A.B., Jamieson, G.A., Pichuantes, S., Nguyen, A.T., Litvak, S., Dupont, C. -H., 1996. 在酿酒酵母中功能性HIV-1整合酶的表达导致致死表型的出现:抑制剂筛选的潜在用途。《当代遗传学》29, 503 - 510)。在此,我们描述了编码SNF5(一种与Ini1同源的酵母转录因子)的基因失活对HIV-1 IN在酵母中表达所诱导的致死性的影响。我们观察到,在SNF5基因已被破坏的细胞中,逆转录病毒IN无法发挥其致死活性,这表明SNF5可能在IN诱导的酵母致死效应中起作用。SNF5失活既不影响酵母活力,也不影响HIV-1 IN的表达。鉴于SNF5与其人类对应物Ini1之间的同源性,我们的结果表明该因子可能对感染细胞中IN的活性很重要。此外,鉴于该转录因子在整合步骤中所起的重要作用以及它对细胞活力是可有可无的这一事实,Ini1/ySNF5与HIV-1 IN之间的相互作用应成为寻找新型抗逆转录病毒药物的潜在靶点。

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