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胆囊收缩素受体拮抗剂

CCK receptor antagonists.

作者信息

Dunlop J

机构信息

CNS Disorders, Wyeth-Ayerst Research, Princeton, NJ 08543, USA.

出版信息

Gen Pharmacol. 1998 Oct;31(4):519-24. doi: 10.1016/s0306-3623(98)00078-0.

Abstract
  1. The peptide hormone and neurotransmitter, cholecystokinin, is widely distributed throughout the gastrointestinal tract and central nervous system and mediates a diverse number of biological functions. 2. Two receptor subtypes, CCK-A and CCK-B, have been identified by both pharmacological characterization and molecular cloning. The CCK-A receptor is the predominant peripheral CCK receptor subtype and the CCK-B receptor is the predominant central CCK receptor. In addition, there are discrete populations of CCK-A receptors in the brain and CCK-B receptors are present in gastric mucosa. 3. Subtype selective antagonists have been developed which discriminate between the two receptor subtypes. One of the major chemical classes has exploited a benzodiazepine template present in asperlicin which was initially discovered in a natural product screen for CCK receptor antagonists. 4. The structurally related benzodiazepines L-365,260, L-740,093, and YM022 are selective antagonists of the CCK-B receptor subtype. Their in vitro pharmacological profiles have been characterized using the human CCK-B receptor expressed in CHO cells. 5. L-365,260 behaves in a manner consistent with that of a competitive antagonist and both L-740,093 and YM022 behave as insurmountable CCK-B receptor antagonists in vitro.
摘要
  1. 肽类激素和神经递质胆囊收缩素广泛分布于胃肠道和中枢神经系统,并介导多种生物学功能。2. 通过药理学特性鉴定和分子克隆已确定了两种受体亚型,即CCK - A和CCK - B。CCK - A受体是主要的外周CCK受体亚型,CCK - B受体是主要的中枢CCK受体。此外,大脑中存在离散的CCK - A受体群体,胃黏膜中存在CCK - B受体。3. 已开发出区分这两种受体亚型的亚型选择性拮抗剂。主要的化学类别之一利用了阿斯匹林中存在的苯二氮䓬模板,阿斯匹林最初是在CCK受体拮抗剂的天然产物筛选中发现的。4. 结构相关的苯二氮䓬类药物L - 365,260、L - 740,093和YM022是CCK - B受体亚型的选择性拮抗剂。它们的体外药理学特性已通过在CHO细胞中表达的人CCK - B受体进行了表征。5. L - 365,260的行为与竞争性拮抗剂一致,而L - 740,093和YM022在体外表现为不可克服的CCK - B受体拮抗剂。

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