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人类急性胰腺炎。病理生理学与治疗的临床及生化研究。

Acute pancreatitis in man. A clinical and biochemical study of pathophysiology and treatment.

作者信息

Lasson A

出版信息

Scand J Gastroenterol Suppl. 1984;99:1-57.

PMID:6205440
Abstract

The correlation between clinical course, protease inhibitors, complement and kinin activation was studied in vivo in 27 attacks of acute pancreatitis and also in vitro. The value of peritoneal lavage was retrospectively analyzed in 73 pancreatitis attacks. The effect of aprotinin was studied in vitro. Complement and kinin activation occurred in vitro when alpha-macroglobulin (alpha 2-M) concentration was below 35%, in spite of 90% free and reactive alpha 1-protease inhibitor. These low alpha 2-M levels were found in the general circulation in severe attacks. Functional alpha 2-M levels were lower than electroimmunoassay values during the acute disease. Complement and kinin activation was present both in blood and in peritoneal fluid. The extent of activation was closely correlated to the severity of the pancreatitis attack. Classical as well as alternative complement activation occurred. Kinin activation was caused by plasma kallikrein as well as by other kininogenases. Functional kallikrein inhibition was lower than electroimmunoassay values for the C1 inactivator. High levels of activated trypsin was found in complex with alpha 1-protease inhibitor in severe attacks. These findings together with the low functional alpha 2-M and a possible functional deficiency also of the C1 inactivator make trypsin-induced activation of the complement as well as the kinin system possible in acute pancreatitis. Changes in proteases and protease inhibitors were most pronounced in the peritoneal fluid, functional alpha 2-M and C1 inactivator being zero, indicating that the primary event occurs locally in and around the pancreas. Peritoneal lavage thus ought to be beneficial. The good results achieved with peritoneal lavage in the retrospective analysis of the 73 clinically severe attacks seem to verify this conclusion. The biochemical changes seen in vivo indicate alpha 2-M and C1 inactivator to be most important against proteolytic activation of the complement and kinin systems. Treatment with purified protease inhibitors might be beneficial. This also seems to be true of aprotinin, according to the in vitro results, provided very high doses are used. All antiprotease therapy seems to be most important intraperitoneally.

摘要

在27例急性胰腺炎发作病例中,对临床病程、蛋白酶抑制剂、补体和激肽激活之间的相关性进行了体内研究,同时也进行了体外研究。对73例胰腺炎发作病例的腹腔灌洗价值进行了回顾性分析。在体外研究了抑肽酶的作用。尽管有90%的游离和活性α1-蛋白酶抑制剂,但当α2-巨球蛋白(α2-M)浓度低于35%时,体外会发生补体和激肽激活。在严重发作的全身循环中发现了这些低α2-M水平。在急性疾病期间,功能性α2-M水平低于免疫电泳测定值。补体和激肽激活在血液和腹腔液中均存在。激活程度与胰腺炎发作的严重程度密切相关。经典和替代补体激活均发生。激肽激活由血浆激肽释放酶以及其他激肽原酶引起。功能性激肽释放酶抑制低于C1灭活剂的免疫电泳测定值。在严重发作中,发现高水平的活化胰蛋白酶与α1-蛋白酶抑制剂形成复合物。这些发现连同低功能性α2-M以及C1灭活剂可能的功能缺陷,使得胰蛋白酶诱导的补体以及激肽系统激活在急性胰腺炎中成为可能。蛋白酶和蛋白酶抑制剂的变化在腹腔液中最为明显,功能性α2-M和C1灭活剂为零,表明主要事件发生在胰腺内及其周围局部。因此,腹腔灌洗应该是有益的。在对73例临床严重发作病例的回顾性分析中,腹腔灌洗取得的良好结果似乎证实了这一结论。体内观察到的生化变化表明α2-M和C1灭活剂对补体和激肽系统的蛋白水解激活最为重要。用纯化的蛋白酶抑制剂治疗可能有益。根据体外结果,只要使用非常高的剂量,抑肽酶似乎也是如此。所有抗蛋白酶治疗似乎在腹腔内最为重要。

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