首页> 美国卫生研究院文献>AMB Express >Substrate stereoselectivity of poly(Asp) hydrolase-1 capable of cleaving β-amide bonds as revealed by investigation of enzymatic hydrolysis of stereoisomeric β-tri(Asp)s
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Substrate stereoselectivity of poly(Asp) hydrolase-1 capable of cleaving β-amide bonds as revealed by investigation of enzymatic hydrolysis of stereoisomeric β-tri(Asp)s

机译:研究立体异构体β-tri(Asp)s的酶促水解揭示了能够裂解β-酰胺键的poly(Asp)水解酶-1的底物立体选择性

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摘要

We previously reported that poly(Asp) hydrolase-1 (PahZ1KP-2) from Pedobacter sp. KP-2 selectively, but not completely, cleaved the amide bonds between β-Asp units in thermally synthesized poly(Asp) (tPAA). In the present study, the enzymatic hydrolysis of stereoisomeric β-tri(Asp)s by PahZ1KP-2 was investigated to clarify the substrate stereoselectivity of PahZ1KP-2 in the hydrolysis of tPAA. The results suggest the following structural features of PahZ1KP-2 at its substrate binding site: (1) the active site contains four subsites (2, 1, −1, and −2), three of which need to be occupied by Asp units for cleavage to occur; (2) for the hydrolysis to proceed, subsite 1 should be occupied by an l-Asp unit, whereas the other three subsites may accept both l- and d-Asp units; (3) for the two central subsites between which cleavage occurs, the (l-Asp)-(d-Asp) sequence is the most favorable for cleavage.
机译:我们先前曾报道过Pedobacter sp。的poly(Asp)水解酶1(PahZ1KP-2)。 KP-2选择性但不完全裂解热合成聚(Asp)(tPAA)中β-Asp单元之间的酰胺键。在本研究中,研究了PahZ1KP-2对立体异构体β-tri(Asp)s的酶促水解,以阐明PahZ1KP-2在tPAA水解中的底物立体选择性。结果表明PahZ1KP-2在其底物结合位点具有以下结构特征:(1)活性位点包含四个亚位点(2、1,-1和-2),其中三个需要被Asp单元占据分裂发生; (2)为了进行水解,子位点1应被一个l-Asp单元占据,而其他三个子位点可以同时接受l-和d-Asp单元; (3)对于在其间发生切割的两个中心亚位点,(1-Asp)-(d-Asp)序列最有利于切割。

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