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Crystal Structure of the Peptidase Domain of Streptococcus ComA, a Bifunctional ATP-binding Cassette Transporter Involved in the Quorum-sensing Pathway*

机译:链球菌ComA的肽酶结构域的晶体结构,一种双功能ATP结合盒式转运蛋白,参与群体感应途径*

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摘要

ComA of Streptococcus is a member of the bacteriocin-associated ATP-binding cassette transporter family and is postulated to be responsible for both the processing of the propeptide ComC and secretion of the mature quorum-sensing signal. The 150-amino acid peptidase domain (PEP) of ComA specifically recognizes an extended region of ComC that is 15 amino acids in length. It has been proposed that an amphipathic α-helix formed by the N-terminal leader region of ComC, as well as the Gly-Gly motif at the cleavage site, is critical for the PEP-ComC interaction. To elucidate the substrate recognition mechanism, we determined the three-dimensional crystal structure of Streptococcus mutans PEP and then constructed models for the PEP·ComC complexes. PEP had an overall structure similar to the papain-like cysteine proteases as has long been predicted. The active site was located at the bottom of a narrow cleft, which is suitable for binding the Gly-Gly motif. Together with the results from mutational experiments, a shallow hydrophobic concave surface of PEP was proposed as a site that accommodates the N-terminal helix of ComC. This dual mode of substrate recognition would provide the small PEP domain with an extremely high substrate specificity.
机译:链球菌的ComA是与细菌素相关的ATP结合盒转运蛋白家族的成员,并被认为既负责前肽ComC的处理又负责成熟群体感应信号的分泌。 ComA的150个氨基酸的肽酶结构域(PEP)特异性识别ComC的扩展区域,该区域的长度为15个氨基酸。已经提出,由ComC的N末端前导区形成的两亲性α-螺旋以及在切割位点的Gly-Gly基序对于PEP-ComC相互作用是至关重要的。为了阐明底物识别机制,我们确定了变形链球菌PEP的三维晶体结构,然后构建了PEP·ComC复合物的模型。如长期以来所预测的,PEP具有类似于木瓜蛋白酶样半胱氨酸蛋白酶的总体结构。活性位点位于狭窄裂口的底部,适合结合Gly-Gly基序。与突变实验的结果一起,提出了PEP的浅疏水凹面作为容纳ComC N末端螺旋的位点。底物识别的这种双重模式将为小PEP域提供极高的底物特异性。

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