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大肠杆菌cAMP受体蛋白变构激活时的化学连接

Chemical linkage at allosteric activation of E. coli cAMP receptor protein.

作者信息

Tutar Yusuf

机构信息

Department of Chemistry and Biochemistry, Texas Tech University, Lubbock, TX 79409, USA.

出版信息

Protein J. 2008 Jan;27(1):21-9. doi: 10.1007/s10930-007-9104-1.

Abstract

Cyclic AMP Receptor protein (CRP) regulates transcription initiation in E. coli. The ligand and DNA binding data yields the following results: (1) There are two different types of cAMP binding sites; weak and strong. (2) CRP-DNA-cAMP is the active form of all CRP conformers and this complex prefers to form from CRP-DNA rather than CRP-cAMP form. (3) Binding of additional cAMP(s) to CRP-DNA-cAMP complex greatly reduces DNA binding affinity. (4) Variants showed that ribose moiety of cAMP is important to transmit the signal to the DNA binding domain to activate specific DNA binding. (5) Deconvolution of DNA binding data leads us to propose a model for cAMP's role in transcription initiation process.

摘要

环磷酸腺苷受体蛋白(CRP)调节大肠杆菌中的转录起始。配体与DNA结合数据产生了以下结果:(1)存在两种不同类型的环磷酸腺苷结合位点;弱结合位点和强结合位点。(2)CRP-DNA-环磷酸腺苷是所有CRP构象体的活性形式,并且这种复合物更倾向于由CRP-DNA形成,而非CRP-环磷酸腺苷形式。(3)额外的环磷酸腺苷与CRP-DNA-环磷酸腺苷复合物结合会大大降低DNA结合亲和力。(4)变体表明,环磷酸腺苷的核糖部分对于将信号传递至DNA结合结构域以激活特异性DNA结合很重要。(5)DNA结合数据的反卷积使我们提出了一个关于环磷酸腺苷在转录起始过程中作用的模型。

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