胰腺炎中的胰蛋白酶:罪魁祸首、介质还是表象?

IF 4.3 3区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY World Journal of Gastroenterology Pub Date : 2024-11-07 DOI:10.3748/wjg.v30.i41.4417
Anna S Gukovskaya, Markus M Lerch, Julia Mayerle, Matthias Sendler, Baoan Ji, Ashok K Saluja, Fred S Gorelick, Ilya Gukovsky
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引用次数: 0

摘要

胰腺炎是一种常见的、危及生命的胰腺外分泌炎症性疾病。其发病机理尚不明确,也没有特异或有效的治疗方法。胆结石和过量饮酒是胰腺炎的主要病因;一小部分患者的疾病是遗传性的。胰腺炎被认为是由受损的胰腺尖突细胞(主要的胰腺外分泌细胞类型)引发,导致实质坏死以及局部和全身炎症。这些细胞的主要功能是产生、储存和分泌各种酶,以分解各类营养物质。大多数消化酶,包括所有蛋白酶,都是以非活性原形(酶原)的形式由渐冻人细胞分泌的,在生理条件下,只有到达肠道时才会被激活。肠道中的非活性胰蛋白酶原生成胰蛋白酶对其他酶原的生理活化起着至关重要的作用。有人提出,胰腺炎是由腺体的蛋白自消化引起的,而腺体的蛋白自消化是由过早/不适当的胰蛋白酶原在胰腺细胞内活化介导的。在急性和慢性胰腺炎的实验模型以及人类疾病中,都能观察到胰腺细胞内胰蛋白酶原的活化。基于这些观察结果,胰蛋白酶原活化被认为是胰腺炎的核心致病机制--这一概念已有百年历史。本综述总结了实验性和遗传性啮齿类动物胰腺炎模型中胰蛋白酶原激活的数据,特别是最近模拟遗传性胰腺炎相关突变的基因工程小鼠模型;分析了介导胰蛋白酶原激活和保护胰腺免受其破坏性影响的机制;讨论了我们知识中的空白、潜在的治疗方法和未来研究的方向。我们的结论是,胰蛋白酶不是疾病发病机制的罪魁祸首,充其量只是某些胰腺炎反应的介质。因此,寻找有效疗法的重点应放在预防胰腺内其他病理过程或使其正常化的方法上,如导致实质细胞死亡和炎症持续不退的自噬缺陷。
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Trypsin in pancreatitis: The culprit, a mediator, or epiphenomenon?

Pancreatitis is a common, life-threatening inflammatory disease of the exocrine pancreas. Its pathogenesis remains obscure, and no specific or effective treatment is available. Gallstones and alcohol excess are major etiologies of pancreatitis; in a small portion of patients the disease is hereditary. Pancreatitis is believed to be initiated by injured acinar cells (the main exocrine pancreas cell type), leading to parenchymal necrosis and local and systemic inflammation. The primary function of these cells is to produce, store, and secrete a variety of enzymes that break down all categories of nutrients. Most digestive enzymes, including all proteases, are secreted by acinar cells as inactive proforms (zymogens) and in physiological conditions are only activated when reaching the intestine. The generation of trypsin from inactive trypsinogen in the intestine plays a critical role in physiological activation of other zymogens. It was proposed that pancreatitis results from proteolytic autodigestion of the gland, mediated by premature/inappropriate trypsinogen activation within acinar cells. The intra-acinar trypsinogen activation is observed in experimental models of acute and chronic pancreatitis, and in human disease. On the basis of these observations, it has been considered the central pathogenic mechanism of pancreatitis - a concept with a century-old history. This review summarizes the data on trypsinogen activation in experimental and genetic rodent models of pancreatitis, particularly the more recent genetically engineered mouse models that mimic mutations associated with hereditary pancreatitis; analyzes the mechanisms mediating trypsinogen activation and protecting the pancreas against its' damaging effects; discusses the gaps in our knowledge, potential therapeutic approaches, and directions for future research. We conclude that trypsin is not the culprit in the disease pathogenesis but, at most, a mediator of some pancreatitis responses. Therefore, the search for effective therapies should focus on approaches to prevent or normalize other intra-acinar pathologic processes, such as defective autophagy leading to parenchymal cell death and unrelenting inflammation.

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来源期刊
World Journal of Gastroenterology
World Journal of Gastroenterology 医学-胃肠肝病学
CiteScore
7.80
自引率
4.70%
发文量
464
审稿时长
2.4 months
期刊介绍: The primary aims of the WJG are to improve diagnostic, therapeutic and preventive modalities and the skills of clinicians and to guide clinical practice in gastroenterology and hepatology.
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