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Bradykinin B2 receptors mediate contraction in the normal and inflamed human gallbladder in vitro.

作者信息

Trevisani Marcello, Amadesi Silvia, Schmidlin Fabien, Poblete Maria T, Bardella Elisabetta, Maggiore Barbara, Harrison Selena, Figueroa Carlos D, Tognetto Michele, Navarra Giuseppe, Turini Alessandro, Bunnett Nigel W, Geppetti Pierangelo, De Giorgio Roberto

机构信息

Department of Experimental Medicine and Clinical Medicine, Pharmacology Unit, University of Ferrara, Italy.

出版信息

Gastroenterology. 2003 Jul;125(1):126-35. doi: 10.1016/s0016-5085(03)00694-2.

Abstract

BACKGROUND & AIMS: The components of the kinin system, including kinongens, kininogenases, and B(2) and B(1) receptors, are expressed and activated during inflammation. Here, we investigated the expression of the kinin B(2) receptor messenger RNA, kininogen and kallikrein immunoreactivity, and the ability of kinins to contract control and inflamed gallbladders in vitro.

METHODS

Human gallbladders, obtained from patients undergoing cholecystectomy either for acute cholecystitis secondary to gallstone disease or during elective gastro-entero-pancreatic surgery (controls), were processed for reverse-transcription polymerase chain reaction analysis, kallikrein and kininogen immunohistochemistry, binding studies, and in vitro contractility studies.

RESULTS

Tissue expression of B(2) receptor messenger RNA and specific binding of [(3)H]-bradykinin increased significantly in acute cholecystitis compared to controls. Kallikrein immunoreactivity was detected in the epithelium and infiltrating leukocytes, whereas kininogen immunoreactivity in the lumen of blood vessels and interstitial space. Bradykinin contracted isolated strips of control and acute cholecystitis gallbladders. In acute cholecystitis tissue, efficacy of bradykinin was higher than that of control gallbladders and similar to that of cholecystokinin. The contraction induced by bradykinin was significantly attenuated by B(2) receptor antagonism but not by cyclooxygenase inhibition and B(1), muscarinic, or tachykinin receptor antagonism.

CONCLUSIONS

All the components of the kinin system are expressed in the human gallbladder. Bradykinin is a powerful spasmogen via B(2) receptor activation in the normal and, especially, in the inflamed human gallbladder.

摘要

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