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介导人胆囊和升结肠收缩的胆囊收缩素受体的药理学特性

Pharmacological characterization of cholecystokinin receptors mediating contraction of human gallbladder and ascending colon.

作者信息

Morton M F, Welsh N J, Tavares I A, Shankley N P

机构信息

Academic Department of Surgery, Rayne Institute, GKT Schools of Medicine and Dentistry, London SE5 9NU, UK.

出版信息

Regul Pept. 2002 Apr 15;105(1):59-64. doi: 10.1016/s0167-0115(01)00383-4.

DOI:10.1016/s0167-0115(01)00383-4
PMID:11853872
Abstract

Cholecystokinin (CCK) produces contractions of gallbladder and colon in a number of different species. Although the effects of CCK on the human gallbladder are relatively well documented, the CCK receptors in the human colon have not been clearly characterised. Therefore, in this study, the CCK receptors in the human gallbladder and colon were compared using pharmacological techniques. Contraction of specimens of the human tissue was measured using in vitro organ bath bioassay. The effect of selective concentrations of CCK(1) and CCK(2) receptor antagonists (L-364,718 and JB93182, respectively) was determined on agonist concentration-effect (E/[A]) curves obtained by cumulative dosing with sulphated CCK. The CCK(1) antagonist L-364,718 produced a rightward shift of the CCK-8S [E/[A] curve in the human gallbladder (pA(2)=9.15 +/- 0.26) and ascending colon (pA(2)=9.20 +/- .33). In both tissues, the CCK(2) receptor antagonist, JB93182, had no effect on the CCK E/[A] curves. In addition, in the colon, pentagastrin responses were inhibited by L-364,718 but unaffected by JB93182. These data indicate that the CCK-induced contraction of the human colon and gallbladder smooth muscle is mediated solely through the CCK(1) receptor subtype, and the antagonist affinity estimates are consistent with those previously obtained in experiments on animal tissue.

摘要

胆囊收缩素(CCK)可使多种不同物种的胆囊和结肠产生收缩。尽管CCK对人体胆囊的作用已有相对充分的文献记载,但人体结肠中的CCK受体尚未得到明确表征。因此,在本研究中,运用药理学技术对人体胆囊和结肠中的CCK受体进行了比较。采用体外器官浴生物测定法测量人体组织标本的收缩情况。通过用硫酸化CCK累积给药获得激动剂浓度 - 效应(E/[A])曲线,测定了选择性浓度的CCK(1)和CCK(2)受体拮抗剂(分别为L - 364,718和JB93182)的作用。CCK(1)拮抗剂L - 364,718使人体胆囊(pA(2)=9.15±0.26)和升结肠(pA(2)=9.20±0.33)中的CCK - 8S [E/[A]曲线向右移动。在两种组织中,CCK(2)受体拮抗剂JB93182对CCK E/[A]曲线均无影响。此外,在结肠中,五肽胃泌素反应受到L - 364,718的抑制,但不受JB93182的影响。这些数据表明,CCK诱导的人体结肠和胆囊平滑肌收缩仅通过CCK(1)受体亚型介导,且拮抗剂亲和力估计值与先前在动物组织实验中获得的结果一致。

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