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首页> 外文期刊>Current Protein and Peptide Science >Achieving Functionality Through Modular Build-up: Structure and Size Selection of Serine Oligopeptidases
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Achieving Functionality Through Modular Build-up: Structure and Size Selection of Serine Oligopeptidases

机译:通过模块化构建实现功能:丝氨酸寡肽酶的结构和尺寸选择

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Enzymes of the prolyl oligopeptidase family (S9 family) recognize their substrates not only by the specificity motif to be cleaved but also by size - they hydrolyze oligopeptides smaller than 30 amino acids. They belong to the serine-protease family, but differ from classical serine-proteases in size (80 kDa), structure (two domains) and regulation system (size selection of substrates). This group of enzymes is an important target for drug design as they are linked to amnesia, schizophrenia, type 2 diabetes, trypanosomiasis, periodontitis and cell growth. By comparing the structure of various members of the family we show that the most important features contributing to selectivity and efficiency are: (i) whether the interactions weaving the two domains together play a role in stabilizing the catalytic triad and thus their absence may provide for its deactivation: these oligopeptidases can screen their substrates by opening up, and (ii) whether the interaction-prone beta-edge of the hydrolase domain is accessible and thus can guide a multimerization process that creates shielded entrance or intricate inner channels for the size-based selection of substrates. These cornerstones can be used to estimate the multimeric state and selection strategy of yet undetermined structures.
机译:脯氨酰寡肽酶的酶(S9家族)不仅通过裂解的特异性基序来识别它们的基材,而且通过尺寸 - 它们水解小于30个氨基酸的寡肽。它们属于丝氨酸蛋白酶家族,但与大小(80kDa),结构(两个域)和调节系统(衬底的尺寸选择)不同的丝氨酸蛋白酶不同。该组酶是药物设计的重要目标,因为它们与胃杉,精神分裂症,2型糖尿病,锥虫病,牙周炎和细胞生长相关。通过比较家庭各种成员的结构,表明有助于选择性和效率的最重要特征是:(i)将两个结构域的相互作用在一起起作用在稳定催化三合会的作用,因此它们的缺席可以提供它的失活:这些寡肽酶可以通过打开筛选它们的基材,并且(ii)可以使用水解酶域的相互作用β-边缘,从而可以引导多聚化过程,该过程为尺寸创造屏蔽入口或复杂的内部通道。基于基材的选择。这些基石可用于估计尚未确定的结构的多端状态和选择策略。

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