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人类热休克转录因子对5碱基对DNA序列基序的模块化识别

Modular recognition of 5-base-pair DNA sequence motifs by human heat shock transcription factor.

作者信息

Cunniff N F, Wagner J, Morgan W D

机构信息

Department of Biology, McGill University, Montreal, Quebec, Canada.

出版信息

Mol Cell Biol. 1991 Jul;11(7):3504-14. doi: 10.1128/mcb.11.7.3504-3514.1991.

Abstract

We investigated the recognition of the conserved 5-bp repeated motif NGAAN, which occurs in heat shock gene promoters of Drosophila melanogaster and other eukaryotic organisms, by human heat shock transcription factor (HSF). Extended heat shock element mutants of the human HSP70 gene promoter, containing additional NGAAN blocks flanking the original element, showed significantly higher affinity than the wild-type promoter element for human HSF in vitro. Protein-DNA contact positions were identified by hydroxyl radical protection, diethyl pyrocarbonate interference, and DNase I footprinting. New contacts in the mutant HSE constructs corresponded to the locations of additional NGAAN motifs. The pattern of binding indicated the occurrence of multiple DNA binding modes for HSF with the various constructs and was consistent with an oligomeric, possibly trimeric, structure of the protein. In contrast to the improved binding, the extended heat shock element mutant constructs did not exhibit dramatically increased heat-inducible transcription in transient expression assays with HeLa cells.

摘要

我们研究了人类热休克转录因子(HSF)对保守的5碱基重复基序NGAAN的识别情况,该基序存在于黑腹果蝇和其他真核生物的热休克基因启动子中。人HSP70基因启动子的扩展热休克元件突变体,在原始元件两侧含有额外的NGAAN块,在体外对人HSF的亲和力明显高于野生型启动子元件。通过羟基自由基保护、焦碳酸二乙酯干扰和DNase I足迹法确定了蛋白质与DNA的接触位置。突变型热休克元件(HSE)构建体中的新接触点与额外NGAAN基序的位置相对应。结合模式表明HSF与各种构建体存在多种DNA结合模式,并且与该蛋白质的寡聚体结构(可能是三聚体)一致。与结合改善相反,在HeLa细胞的瞬时表达试验中,扩展热休克元件突变体构建体并未表现出显著增加的热诱导转录。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3325/361086/42ea25337ad5/molcellb00031-0119-a.jpg

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