Department of Molecular and Cell Biology, Henry M. Goldman School of Dental Medicine, Boston University, Boston, Massachusetts.
Am J Physiol Gastrointest Liver Physiol. 2014 Mar;306(6):G466-73. doi: 10.1152/ajpgi.00419.2013. Epub 2014 Jan 23.
Variations in the serine protease 1 (PRSS1) gene encoding human cationic trypsinogen have been conclusively associated with autosomal dominant hereditary pancreatitis and sporadic nonalcoholic chronic pancreatitis. Most high-penetrance PRSS1 variants increase intrapancreatic trypsin activity by stimulating trypsinogen autoactivation and/or by inhibiting chymotrypsin C-dependent trypsinogen degradation. Alternatively, some PRSS1 variants can cause trypsinogen misfolding, which results in intracellular retention and degradation with consequent endoplasmic reticulum stress. However, not all PRSS1 variants are pathogenic, and clinical relevance of rare variants is often difficult to ascertain. Here we review the PRSS1 variants published since 1996 and discuss their functional properties and role in chronic pancreatitis.
丝氨酸蛋白酶 1(PRSS1)基因编码的人类阳离子胰蛋白酶原的变异与常染色体显性遗传性胰腺炎和散发性非酒精性慢性胰腺炎有明确的关联。大多数高外显率的 PRSS1 变体通过刺激胰蛋白酶原自动激活和/或抑制糜蛋白酶 C 依赖性胰蛋白酶原降解来增加胰内胰蛋白酶活性。或者,一些 PRSS1 变体可导致胰蛋白酶原错误折叠,导致细胞内滞留和降解,从而导致内质网应激。然而,并非所有 PRSS1 变体都是致病性的,稀有变体的临床相关性通常难以确定。在这里,我们回顾了自 1996 年以来发表的 PRSS1 变体,并讨论了它们的功能特性及其在慢性胰腺炎中的作用。
