Park Ae Kyung, Lee Jeong Hye, Chi Young Min, Park Hyun
Division of Biotechnology, College of Life Sciences, Korea University, Seoul 136-713, South Korea; Division of Polar Life Sciences, Korea Polar Research Institute, Yeonsu-gu, Incheon 406-840, South Korea.
Division of Biotechnology, College of Life Sciences, Korea University, Seoul 136-713, South Korea.
Biochem Biophys Res Commun. 2016 Apr 29;473(2):625-9. doi: 10.1016/j.bbrc.2016.03.144. Epub 2016 Mar 30.
Spr1814 of Streptococcus pneumoniae is a response regulator (RR) that belongs to the NarL/FixJ subfamily and has a four-helix helix-turn-helix DNA-binding domain. Here, the X-ray crystal structure of the full-length spr1814 in complex with a phosphate analogue beryllium fluoride (BeF3(-)) was determined at 2.0 Å. This allows for a structural comparison with the previously reported full-length unphosphorylated spr1814. The phosphorylation of conserved aspartic acid residue of N-terminal receiver domain triggers a structural perturbation at the α4-β5-α5 interface, leading to the domain reorganization of spr1814, and this is achieved by a rotational change in the C-terminal DNA-binding domain.
肺炎链球菌的Spr1814是一种应答调节因子(RR),属于NarL/FixJ亚家族,具有一个四螺旋的螺旋-转角-螺旋DNA结合结构域。在此,全长spr1814与磷酸类似物氟化铍(BeF3(-))复合物的X射线晶体结构在2.0埃分辨率下得以确定。这使得能够与先前报道的全长未磷酸化spr1814进行结构比较。N端接收结构域保守天冬氨酸残基的磷酸化在α4-β5-α5界面引发结构扰动,导致spr1814的结构域重组,这是通过C端DNA结合结构域的旋转变化实现的。
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