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首页> 美国卫生研究院文献>Biochemical Journal >Multiple binding sites involved in the effect of choline esters on decarbamoylation of monomethylcarbamoyl- or dimethylcarbamoly-acetylcholinesterase.
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Multiple binding sites involved in the effect of choline esters on decarbamoylation of monomethylcarbamoyl- or dimethylcarbamoly-acetylcholinesterase.

机译:涉及胆碱酯对单甲基氨基甲酰基-或二甲基氨基甲酰基-乙酰胆碱酯酶的脱氨基甲酰基化作用的多个结合位点。

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Multiple binding sites for inhibitory choline esters in spontaneous decarbamoylation of dimethylcarbamoyl-acetylcholinesterase (AChE) were suggested from a wide range of IC50 values, in contrast with a limited range of AC50 values (concentration giving 50% of maximal activation) at a peripheral activatory site. Association of choline esters containing a long acyl chain (C7-C12) with the hydrophobic zone in the active site could be deduced from a linear relationship between the size of the acyl group and the inhibitory potency in either spontaneous decarbamoylation or acetylthiocholine hydrolysis. Direct support for laurylcholine binding to the active site might come from the competitive inhibition (Ki 33 microM) of choline-catalysed decarbamoylation by laurylcholine. Moreover, its inhibitory action was greater for monomethylcarbamoyl-AChE than for dimethylcarbamoyl-AChE, where there is a greater steric hindrance at the active centre. In further support, the inhibition of pentanoylthiocholine-induced decarbamoylation by laurylcholine was suggested to be due to laurylcholine binding to a central site rather than a peripheral site, similar to the inhibition of spontaneous decarbamoylation by laurylcholine. Supportive data for acetylcholine binding to the active site are provided by the results that acetylcholine is a competitive inhibitor (Ki 7.6 mM) of choline-catalysed decarbamoylation, and its inhibitory action was greater for monomethylcarbamoyl-AChE than for dimethylcarbamoyl-AChE. Meanwhile, choline esters with an acyl group of an intermediate size (C4-C6), more subject to steric exclusion at the active centre, and less associable with the hydrophobic zone, appear to bind preferentially to a peripheral activity site. Thus the multiple effects of choline esters may be governed by hydrophobicity and/or a steric effect exerted by the acyl moiety at the binding sites.
机译:从宽范围的IC50值中提出了抑制性胆碱酯在二甲基氨基甲酰基-乙酰胆碱酯酶(AChE)自发脱氨基甲酰基化中的多个结合位点,而在外围激活位点的AC50值范围有限(最大激活浓度为50%),则有很多结合位点。可以从酰基大小与自发脱氨基甲酰基化或乙酰基硫代胆碱水解中的抑制能力之间的线性关系推断出含有长酰基链(C7-C12)的胆碱酯与活性位点的疏水性缔合。十二烷基胆碱与活性位点结合的直接支持可能来自十二烷基胆碱对胆碱催化的脱氨甲酰化的竞争性抑制(Ki 33 microM)。此外,其对单甲基氨基甲酰基-AChE的抑制作用要大于对二甲基氨基甲酰基-AChE的抑制作用,后者在活性中心具有更大的空间位阻。在进一步的支持中,有人提出抑制月桂酰胆碱对戊酰硫胆碱诱导的去氨甲酰基化的作用是由于月桂酰胆碱结合于中心位点而不是外围位点,类似于对月桂酰胆碱的自发去氨甲酰化的抑制。乙酰胆碱是胆碱催化的脱氨甲酰基反应的竞争性抑制剂(Ki 7.6 mM),其结果为乙酰胆碱结合到活性位点提供了支持性数据,其对单甲基氨基甲酰基-AChE的抑制作用大于对二甲基氨基甲酰基-AChE的抑制作用。同时,具有中等大小(C 4 -C 6)的酰基的胆碱酯似乎优先结合到外周活性位,所述中等大小的酰基(C 4 -C 6)在活性中心更易发生空间排阻,而与疏水区的缔合较少。因此,胆碱酯的多重作用可以由在结合位点处的酰基部分所施加的疏水性和/或位阻作用决定。

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