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腺病毒反向末端重复序列在无细胞系统中起增强子的作用。

The adenovirus inverted terminal repeat functions as an enhancer in a cell-free system.

作者信息

Miralles V J, Cortes P, Stone N, Reinberg D

机构信息

Department of Biochemistry, Robert Wood Johnson Medical School, University of Medicine and Dentistry of New Jersey, Piscataway 08875-5635.

出版信息

J Biol Chem. 1989 Jun 25;264(18):10763-72.

PMID:2525131
Abstract

Two binding sites for EivF, a factor involved in transcription from the adenovirus early promoter iv (Eiv), were mapped within the adenovirus inverted terminal repeats (ITR). Consistent with the observation that EivF was required to initiate transcription from the Eiv promoter and with the demonstration that two EivF binding sites were present in the ITR, we show that the inverted terminal repeat region was able to promote transcription from the CAP site of the Eiv promoter in vitro and in an EIa-dependent fashion in vivo. The minimum sequence within the ITR capable of directing EIa-dependent transcription consists of forty nine nucleotides comprising two EivF binding sites and at least one Sp1 binding site. This 49-base pair fragment possesses the characteristics of an enhancer which is induced by EIa. The enhancer is active in HeLa cell nuclear extracts. Transcription directed by the ITR required EivF and the general transcription factors. The addition of purified Sp1 factor specifically stimulated transcription which correlates with the presence of Sp1 binding sites between the two EivF recognition sites.

摘要

EivF是一种参与腺病毒早期启动子iv(Eiv)转录的因子,在腺病毒反向末端重复序列(ITR)中确定了两个EivF结合位点。鉴于观察到从Eiv启动子起始转录需要EivF,且证明ITR中存在两个EivF结合位点,我们发现反向末端重复区域在体外能够促进从Eiv启动子的CAP位点起始转录,并且在体内以依赖EIa的方式促进转录。ITR内能够指导依赖EIa转录的最小序列由49个核苷酸组成,包括两个EivF结合位点和至少一个Sp1结合位点。这个49碱基对的片段具有由EIa诱导的增强子的特征。该增强子在HeLa细胞核提取物中具有活性。由ITR指导的转录需要EivF和通用转录因子。添加纯化的Sp1因子可特异性刺激转录,这与两个EivF识别位点之间存在Sp1结合位点相关。

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