Heterozygous Spink1 Deficiency Promotes Trypsin-dependent Chronic Pancreatitis in Mice

IF 7.1 1区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Cellular and Molecular Gastroenterology and Hepatology Pub Date : 2024-01-01 DOI:10.1016/j.jcmgh.2024.05.009

Alexandra Demcsák, Miklós Sahin-Tóth

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引用次数: 0

Abstract

Background & Aims

Heterozygous SPINK1 mutations are strong risk factors for chronic pancreatitis in humans, yet heterozygous disruption of mouse Spink1 yielded no pancreatic phenotype. To resolve this contradiction, we used CRISPR/Cas9-mediated genome editing to generate heterozygous Spink1-deleted mice (Spink1-KO^het) in the C57BL/6N strain and studied the effect of this allele in trypsin-independent and trypsin-dependent pancreatitis models.

Methods

We investigated severity of acute pancreatitis and progression to chronic pancreatitis in Spink1-KO^het mice after transient (10 injections) and prolonged (2 × 8 injections) cerulein hyperstimulation. We crossed Spink1-KO^het mice with T7D23A and T7D22N,K24R mice that carry strongly autoactivating trypsinogen mutants and exhibit spontaneous chronic pancreatitis.

Results

Prolonged but not transient cerulein stimulation resulted in increased intrapancreatic trypsin activity and more severe acute pancreatitis in Spink1-KO^het mice relative to the C57BL/6N control strain. After the acute episode, Spink1-KO^het mice developed progressive disease with chronic pancreatitis-like features, whereas C57BL/6N mice recovered rapidly. Trypsinogen mutant mice carrying the Spink1-KO^het allele exhibited strikingly more severe chronic pancreatitis than the respective parent strains.

Conclusions

Heterozygous Spink1 deficiency caused more severe acute pancreatitis after prolonged cerulein stimulation and promoted chronic pancreatitis after the cerulein-induced acute episode, and in two strains of trypsinogen mutant mice with spontaneous disease. In contrast, acute pancreatitis induced with limited cerulein hyperstimulation was unaffected by heterozygous Spink1 deletion, in agreement with recent observations that trypsin activity does not mediate pathologic responses in this model. Taken together, the findings strongly support the notion that loss-of-function SPINK1 mutations in humans increase chronic pancreatitis risk in a trypsin-dependent manner.

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杂合子 Spink1 缺乏症会促进小鼠胰蛋白酶依赖性慢性胰腺炎的发生。

背景和目的：SPINK1杂合子突变是人类慢性胰腺炎的高危因素，但小鼠Spink1的杂合子干扰却不会产生胰腺表型。为了解决这一矛盾，我们利用 CRISPR/Cas9 介导的基因组编辑技术，在 C57BL/6N 品系中产生了杂合子 Spink1 缺失小鼠（Spink1-KOhet），并研究了该等位基因在胰蛋白酶依赖型和胰蛋白酶依赖型胰腺炎模型中的影响：方法：我们研究了Spink1-KOhet小鼠在瞬时（10次注射）和长期（2×8次注射）胰激素过度刺激后急性胰腺炎的严重程度以及慢性胰腺炎的进展。我们将 Spink1-KOhet 小鼠与 T7D23A 和 T7D22N,K24R 小鼠杂交，这些小鼠携带强自激活胰蛋白酶原突变体，表现出自发性慢性胰腺炎。与 C57BL/6N 对照品系相比，Spink1-KOhet 小鼠在长期而非短暂的胰凝乳蛋白刺激下，胰腺内胰蛋白酶活性增加，急性胰腺炎更加严重。急性发作后，Spink1-KOhet 小鼠的疾病呈进行性发展，具有类似慢性胰腺炎的特征，而 C57BL/6N 小鼠则迅速恢复。携带 Spink1-KOhet 等位基因的胰蛋白酶原突变小鼠表现出的慢性胰腺炎比各自的亲本品系要严重得多：结论：杂合子Spink1缺乏症会在长时间胰凝乳蛋白刺激后引起更严重的急性胰腺炎，并在胰凝乳蛋白诱导的急性发作后促进慢性胰腺炎的发生。与此相反，杂合子 Spink1 基因缺失不会影响有限的胰岛素过度刺激诱发的急性胰腺炎，这与最近的观察结果一致，即胰蛋白酶活性并不介导该模型中的病理反应。综上所述，这些发现有力地支持了这样一种观点，即人类功能缺失的 SPINK1 基因突变会以胰蛋白酶依赖性的方式增加慢性胰腺炎的风险。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cellular and Molecular Gastroenterology and Hepatology Medicine-Gastroenterology

CiteScore

13.00

自引率

2.80%

发文量

246

审稿时长

42 days

期刊介绍： "Cell and Molecular Gastroenterology and Hepatology (CMGH)" is a journal dedicated to advancing the understanding of digestive biology through impactful research that spans the spectrum of normal gastrointestinal, hepatic, and pancreatic functions, as well as their pathologies. The journal's mission is to publish high-quality, hypothesis-driven studies that offer mechanistic novelty and are methodologically robust, covering a wide range of themes in gastroenterology, hepatology, and pancreatology. CMGH reports on the latest scientific advances in cell biology, immunology, physiology, microbiology, genetics, and neurobiology related to gastrointestinal, hepatobiliary, and pancreatic health and disease. The research published in CMGH is designed to address significant questions in the field, utilizing a variety of experimental approaches, including in vitro models, patient-derived tissues or cells, and animal models. This multifaceted approach enables the journal to contribute to both fundamental discoveries and their translation into clinical applications, ultimately aiming to improve patient care and treatment outcomes in digestive health.