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CEL-DUP2 的特征:羧基酯脂肪酶基因的完全重复不太可能影响慢性胰腺炎的风险。

Characterization of CEL-DUP2: Complete duplication of the carboxyl ester lipase gene is unlikely to influence risk of chronic pancreatitis.

机构信息

The Gade Laboratory for Pathology, Department of Clinical Medicine, University of Bergen, Bergen, Norway; Department of Medical Genetics, Haukeland University Hospital, Bergen, Norway; Center for Diabetes Research, Department of Clinical Science, University of Bergen, Bergen, Norway.

Univ Brest, Inserm, EFS, UMR 1078, GGB, F-29200, Brest, France; CHRU Brest, Service de Génétique, Brest, France.

出版信息

Pancreatology. 2020 Apr;20(3):377-384. doi: 10.1016/j.pan.2020.01.011. Epub 2020 Jan 20.

Abstract

BACKGROUND/OBJECTIVES: Carboxyl ester lipase is a pancreatic enzyme encoded by CEL, an extremely polymorphic human gene. Pathogenic variants of CEL either increases the risk for chronic pancreatitis (CP) or cause MODY8, a syndrome of pancreatic exocrine and endocrine dysfunction. Here, we aimed to characterize a novel duplication allele of CEL (CEL-DUP2) and to investigate whether it associates with CP or pancreatic cancer.

METHODS

The structure of CEL-DUP2 was determined by a combination of Sanger sequencing, DNA fragment analysis, multiplex ligation-dependent probe amplification and whole-genome sequencing. We developed assays for screening of CEL-DUP2 and analyzed cohorts of idiopathic CP, alcoholic CP and pancreatic cancer. CEL protein expression was analyzed by immunohistochemistry.

RESULTS

CEL-DUP2 consists of an extra copy of the complete CEL gene. The allele has probably arisen from non-allelic, homologous recombination involving the adjacent pseudogene of CEL. We found no association between CEL-DUP2 carrier frequency and CP in cohorts from France (cases/controls: 2.5%/2.4%; P = 1.0), China (10.3%/8.1%; P = 0.08) or Germany (1.6%/2.3%; P = 0.62). Similarly, no association with disease was observed in alcohol-induced pancreatitis (Germany: 3.2%/2.3%; P = 0.51) or pancreatic cancer (Norway; 2.5%/3.2%; P = 0.77). Notably, the carrier frequency of CEL-DUP2 was more than three-fold higher in Chinese compared with Europeans. CEL protein expression was similar in tissues from CEL-DUP2 carriers and controls.

CONCLUSIONS

Our results support the contention that the number of CEL alleles does not influence the risk of pancreatic exocrine disease. Rather, the pathogenic CEL variants identified so far involve exon 11 sequence changes that substantially alter the protein's tail region.

摘要

背景/目的:羧基酯脂肪酶是一种由 CEL 编码的胰腺酶,CEL 是一个高度多态性的人类基因。CEL 的致病变体要么增加慢性胰腺炎(CP)的风险,要么导致 MODY8,即胰腺外分泌和内分泌功能障碍的综合征。在这里,我们旨在描述 CEL 的一种新型重复等位基因(CEL-DUP2),并研究其是否与 CP 或胰腺癌有关。

方法

通过 Sanger 测序、DNA 片段分析、多重连接依赖性探针扩增和全基因组测序相结合的方法确定 CEL-DUP2 的结构。我们开发了用于筛选 CEL-DUP2 的检测方法,并分析了特发性 CP、酒精性 CP 和胰腺癌队列。通过免疫组织化学分析 CEL 蛋白的表达。

结果

CEL-DUP2 由完整 CEL 基因的额外拷贝组成。该等位基因可能是由涉及 CEL 相邻假基因的非等位同源重组产生的。我们在法国(病例/对照:2.5%/2.4%;P=1.0)、中国(10.3%/8.1%;P=0.08)或德国(1.6%/2.3%;P=0.62)的队列中未发现 CEL-DUP2 携带频率与 CP 之间存在关联。同样,在酒精性胰腺炎(德国:3.2%/2.3%;P=0.51)或胰腺癌(挪威;2.5%/3.2%;P=0.77)中也未观察到与疾病的关联。值得注意的是,与欧洲人相比,中国人 CEL-DUP2 的携带频率高出三倍以上。CEL-DUP2 携带者和对照组织中的 CEL 蛋白表达相似。

结论

我们的结果支持这样的观点,即 CEL 等位基因的数量不会影响胰腺外分泌疾病的风险。相反,迄今为止发现的致病 CEL 变体涉及外显子 11 序列变化,这些变化极大地改变了蛋白质的尾部区域。

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