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东莨菪碱和甲基东莨菪碱对映体在神经元(M1)、心脏(M2)和胰腺(M3)毒蕈碱受体上的结合动力学。

Binding kinetics of quinuclidinyl benzilate and methyl-quinuclidinyl benzilate enantiomers at neuronal (M1), cardiac (M2), and pancreatic (M3) muscarinic receptors.

作者信息

Waelbroeck M, Tastenoy M, Camus J, Christophe J

机构信息

Department of Biochemistry and Nutrition, Medical School, Université Libre de Bruxelles, Belgium.

出版信息

Mol Pharmacol. 1991 Sep;40(3):413-20.

PMID:1896027
Abstract

We analyzed the competition kinetics of quinuclidinyl benzilate (QNB) and QNB methiodide enantiomers on human NB-OK1 neuroblastoma (M1), rat cardiac (M2), and rat pancreas (M3) muscarinic binding sites. The association rate constants of the four drugs depended on the receptor subtype studied and were lower with pancreas (M3) (1-9 x 10(5) M-1 sec-1) than with cardiac (M2) (1-5 x 10(6) M-1 sec-1) and NB-OK1 (M1) (1-5 x 10(6) M-1 sec-1) binding sites. At each receptor subtype, we observed no significant difference between the association rate constants of the R- and S-enantiomers of either QNB or QNB methiodide. Receptor stereoselectivity, when present, was associated with differences in unlabeled drug dissociation rate constants. The dissociation rate constant varied much more than the association rate constant, when either (R)-QNB dissociation from the three subtypes (half-life, 77 min to greater than 340 min; best fit, 40 days) or dissociation of the four drugs from each receptor subtype (half-lives varying from 1.4 min to 4 hr at M1 receptors, 1.1 to 77 min at M2 receptors, and 3.5 min to greater than 340 min at M3 receptors were obtained by competition kinetics analysis) was compared.

摘要

我们分析了东莨菪碱(QNB)和东莨菪碱甲基碘对映体在人NB - OK1神经母细胞瘤(M1)、大鼠心脏(M2)和大鼠胰腺(M3)毒蕈碱结合位点上的竞争动力学。这四种药物的结合速率常数取决于所研究的受体亚型,胰腺(M3)的结合速率常数(1 - 9×10⁵ M⁻¹ sec⁻¹)低于心脏(M2)(1 - 5×10⁶ M⁻¹ sec⁻¹)和NB - OK1(M1)(1 - 5×10⁶ M⁻¹ sec⁻¹)结合位点。在每种受体亚型上,我们观察到QNB或QNB甲基碘的R - 和S - 对映体的结合速率常数之间没有显著差异。当存在受体立体选择性时,与未标记药物解离速率常数的差异有关。无论是(R)-QNB从三种亚型上的解离(半衰期,77分钟至大于340分钟;最佳拟合,40天),还是通过竞争动力学分析得到的四种药物从每种受体亚型上的解离(在M1受体处半衰期从1.4分钟到4小时不等,在M2受体处为1.1至77分钟,在M3受体处为3.5分钟至大于340分钟),解离速率常数的变化都远大于结合速率常数。

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