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酯酶抑制剂可防止实验性胰腺炎的两种非侵入性模型中的溶酶体酶重新分布。

Esterase inhibitors prevent lysosomal enzyme redistribution in two noninvasive models of experimental pancreatitis.

作者信息

Ohshio G, Saluja A K, Leli U, Sengupta A, Steer M L

机构信息

Department of Surgery, Harvard Digestive Diseases Center, Beth Israel Hospital, Boston, Massachusetts.

出版信息

Gastroenterology. 1989 Mar;96(3):853-9.

PMID:2464526
Abstract

Earlier studies have indicated that lysosomal enzymes such as cathepsin B become redistributed within pancreatic acinar cells during the early stages of both diet- and secretagogue-induced acute pancreatitis. As a result, cathepsin B and digestive zymogens became colocalized within large cytoplasmic vacuoles. As cathepsin B can activate trypsinogen, this colocalization could result in intracellular digestive enzyme activation. The present study investigates the protective effects of gabexate mesilate (FOY) and camostate (FOY 305) on both of these noninvasive models of experimental pancreatitis. These esterase inhibitors prevented the hyperamylasemia, pancreatic edema, and acinar cell vacuolization that characterize secretagogue-induced pancreatitis and the hyperamylasemia and mortality that characterize diet-induced pancreatitis. In addition, FOY and FOY 305 were found to significantly decrease the subcellular redistribution of cathepsin B that occurs in both models. These findings indicate that enzyme activity sensitive to inhibition by FOY and FOY 305 may be critical to the redistribution phenomenon that characterizes both of these models of pancreatitis.

摘要

早期研究表明,在饮食和促分泌素诱导的急性胰腺炎早期阶段,诸如组织蛋白酶B等溶酶体酶会在胰腺腺泡细胞内重新分布。结果,组织蛋白酶B和消化酶原在大的细胞质空泡内共定位。由于组织蛋白酶B可激活胰蛋白酶原,这种共定位可能导致细胞内消化酶的激活。本研究调查了甲磺酸加贝酯(FOY)和抑肽酶(FOY 305)对这两种非侵入性实验性胰腺炎模型的保护作用。这些酯酶抑制剂可预防促分泌素诱导的胰腺炎所特有的高淀粉酶血症、胰腺水肿和腺泡细胞空泡化,以及饮食诱导的胰腺炎所特有的高淀粉酶血症和死亡率。此外,发现FOY和FOY 305可显著减少在两种模型中均出现的组织蛋白酶B的亚细胞重新分布。这些发现表明,对FOY和FOY 305抑制敏感的酶活性可能对这两种胰腺炎模型所特有的重新分布现象至关重要。

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