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梭菌焦磷酸酶调节区 CBS 和 DRTGG 结构域与抑制剂 AMP 和激活剂四聚腺苷二磷酸复合物的晶体结构

Crystal structures of the CBS and DRTGG domains of the regulatory region of Clostridiumperfringens pyrophosphatase complexed with the inhibitor, AMP, and activator, diadenosine tetraphosphate.

机构信息

Department of Biochemistry and Food Chemistry, University of Turku, Vatselankatu 2, FI-20014 Turku, Finland.

出版信息

J Mol Biol. 2010 May 7;398(3):400-13. doi: 10.1016/j.jmb.2010.03.019. Epub 2010 Mar 19.

Abstract

Nucleotide-binding cystathionine beta-synthase (CBS) domains serve as regulatory units in numerous proteins distributed in all kingdoms of life. However, the underlying regulatory mechanisms remain to be established. Recently, we described a subfamily of CBS domain-containing pyrophosphatases (PPases) within family II PPases. Here, we express a novel CBS-PPase from Clostridium perfringens (CPE2055) and show that the enzyme is inhibited by AMP and activated by a novel effector, diadenosine 5',5-P1,P4-tetraphosphate (AP(4)A). The structures of the AMP and AP(4)A complexes of the regulatory region of C. perfringens PPase (cpCBS), comprising a pair of CBS domains interlinked by a DRTGG domain, were determined at 2.3 A resolution using X-ray crystallography. The structures obtained are the first structures of a DRTGG domain as part of a larger protein structure. The AMP complex contains two AMP molecules per cpCBS dimer, each bound to a single monomer, whereas in the activator-bound complex, one AP(4)A molecule bridges two monomers. In the nucleotide-bound structures, activator binding induces significant opening of the CBS domain interface, compared with the inhibitor complex. These results provide structural insight into the mechanism of CBS-PPase regulation by nucleotides.

摘要

核苷酸结合半胱氨酸β-合成酶 (CBS) 结构域作为调节单位存在于分布在所有生命领域的众多蛋白质中。然而,其潜在的调节机制仍有待确定。最近,我们在 II 型磷酸酶家族内描述了一个包含 CBS 结构域的焦磷酸酶 (PPase) 亚家族。在这里,我们表达了来自产气荚膜梭菌 (CPE2055) 的一种新型 CBS-PPase,并表明该酶被 AMP 抑制,被一种新型效应物二腺苷 5',5'-P1,P4-四磷酸 (AP(4)A) 激活。使用 X 射线晶体学,以 2.3 A 的分辨率测定了包含一对 CBS 结构域和 DRTGG 结构域的产气荚膜梭菌 PPase (cpCBS) 调节区域的 AMP 和 AP(4)A 复合物的结构。获得的结构是 DRTGG 结构域作为更大蛋白质结构的一部分的第一个结构。AMP 复合物每个 cpCBS 二聚体包含两个 AMP 分子,每个分子都与单个单体结合,而在激活剂结合的复合物中,一个 AP(4)A 分子桥接两个单体。在核苷酸结合结构中,与抑制剂复合物相比,激活剂结合诱导 CBS 结构域界面的显著打开。这些结果为核苷酸对 CBS-PPase 调节的机制提供了结构上的见解。

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