| Literature DB >> 29107486 |
Ling Xu1, Lijun Wang1, Junhui Peng1, Fudong Li1, Lijie Wu2, Beibei Zhang1, Mengqi Lv1, Jiahai Zhang1, Qingguo Gong1, Rongguang Zhang3, Xiaobing Zuo4, Zhiyong Zhang1, Jihui Wu1, Yajun Tang5, Yunyu Shi6.
Abstract
CsdA has been proposed to be essential for the biogenesis of ribosome and gene regulation after cold shock. However, the structure of CsdA and the function of its long C-terminal regions are still unclear. Here, we solved all of the domain structures of CsdA and found two previously uncharacterized auxiliary domains: a dimerization domain (DD) and an RNA-binding domain (RBD). Small-angle X-ray scattering experiments helped to track the conformational flexibilities of the helicase core domains and C-terminal regions. Biochemical assays revealed that DD is indispensable for stabilizing the CsdA dimeric structure. We also demonstrate for the first time that CsdA functions as a stable dimer at low temperature. The C-terminal regions are critical for RNA binding and efficient enzymatic activities. CsdA_RBD could specifically bind to the regions with a preference for single-stranded G-rich RNA, which may help to bring the helicase core to unwind the adjacent duplex.Entities:
Keywords: ATPase activity; CsdA; DEAD-box helicase; RNA binding; crystal structure; dimerization domain; small-angle X-ray scattering; unwinding activity
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Year: 2017 PMID: 29107486 DOI: 10.1016/j.str.2017.09.013
Source DB: PubMed Journal: Structure ISSN: 0969-2126 Impact factor: 5.006