Genetics of Pancreatitis: The 2014 Update

Masamune, Atsushi

doi:10.1620/tjem.232.69

Cited by 49 publications

(33 citation statements)

References 51 publications

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“…Although our cohort is small, those observations are consistent with the results of a pooled case-control analysis showing that 6.2% of pdac patients have a history of pancreatitis 29 . Younger patients (<65 years of age) with a history of pancreatitis could be at increased risk for a genetic predisposition to pdac, including hereditary pancreatitis 30 . Several studies have shown that an increased body mass index (bmi) is associated with pdac risk 31 .…”

Section: Discussionmentioning

confidence: 99%

Establishing a Clinic-Based Pancreatic Cancer and Periampullary Tumour Research Registry in Quebec

Bascuñana

Hall

et al. 2015

Current Oncology

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Participation rates were 88.4% for all referrals and 89.2% for pdac referrals. Family history, epidemiologic and clinical data, and biospecimens were ascertained from 91.9%, 54.6%, and 97.5% respectively of patients with pdac. Although demographics and trends in risk factors in our patients were consistent with published statistics for patients with pdac, the qpcs is enriched for families with French-Canadian ancestry (37.4%), a population with recurrent germline mutations in hereditary diseases. ConclusionsUsing rapid ascertainment, a pdac and pat research registry with high participation rates can be established. The qpcs is a valuable research resource and its enrichment with patients of French-Canadian ancestry provides a unique opportunity for studies of heredity in these diseases.

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Section: Discussionmentioning

confidence: 99%

Establishing a Clinic-Based Pancreatic Cancer and Periampullary Tumour Research Registry in Quebec

Bascuñana

Hall

et al. 2015

Current Oncology

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“…Even though p.N34S was presumed to cause a loss of function, the exact mechanism of action has never been identified, as no functional defect was demonstrated for p.N34S or any of the four intronic variants associated with this haplotype (5,7,19,20,24,26). In contrast, an unambiguous loss-of-function phenotype was evident for variant c.194ϩ2TϾC (28,35,39, and references therein), the second most frequent SPINK1 mutation that affects a splice site in intron-3 and causes exon skipping with markedly reduced SPINK1 mRNA expression (19,23). This intronic mutation is in complete linkage disequilibrium (i.e., found together) with the promoter variant c.-215GϾA.…”

mentioning

confidence: 99%

Functional significance of SPINK1 promoter variants in chronic pancreatitis

Derikx

Geisz

Kereszturi

et al. 2015

American Journal of Physiology-Gastrointestinal and Liver Physi

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Chronic pancreatitis is a progressive inflammatory disorder of the pancreas, which often develops as a result of genetic predisposition. Some of the most frequently identified risk factors affect the serine protease inhibitor Kazal type 1 ( SPINK1) gene, which encodes a trypsin inhibitor responsible for protecting the pancreas from premature trypsinogen activation. Recent genetic and functional studies indicated that promoter variants in the SPINK1 gene might contribute to disease risk in carriers. Here, we investigated the functional effects of 17 SPINK1 promoter variants using luciferase reporter gene expression assay in four different cell lines, including three pancreatic acinar cell lines (rat AR42J with or without dexamethasone-induced differentiation and mouse 266-6) and human embryonic kidney 293T cells. We found that most variants caused relatively small changes in promoter activity. Surprisingly, however, we observed significant variations in the effects of the promoter variants in the different cell lines. Only four variants exhibited consistently reduced promoter activity in all acinar cell lines, confirming previous reports that variants c.-108G>T, c.-142T>C, and c.-147A>G are risk factors for chronic pancreatitis and identifying c.-52G>T as a novel risk variant. In contrast, variant c.-215G>A, which is linked with the disease-associated splice-site mutation c.194+2T>C, caused increased promoter activity, which may mitigate the overall effect of the pathogenic haplotype. Our study lends further support to the notion that sequence evaluation of the SPINK1 promoter region in patients with chronic pancreatitis is justified as part of the etiological investigation.

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“…The exocrine pancreas with its huge rate of protein synthesis is particularly vulnerable when subjected to congestion in the busy proteintrafficking lanesan inevitable consequence of pancreastasis episodes, despite the acinar cell's best efforts to compensate by endocrine rerouting of newly synthesised enzymes; removal of zymogen granules via the three-pronged strategy of centripetal dissolution, crinophagy and basolateral redirection; and down-regulation of enzyme synthesis (19,30,34,52). The close integration between oxidative, electrophilic, ER, and inflammation stress is now regarded as the basis for many chronic diseases (177) and, increasingly, for chronic pancreatitis (97,112,123).…”

Section: Endoplasmic Reticulum Stressmentioning

confidence: 99%

“…The 1998 version (24) views the acinar cell as the site of mounting electrophilic stress that steadily erodes methyl (CH 3 ) and thiol (SH) -principally glutathione (GSH ) -moieties, as a result of CYP induction, concurrent exposure to a toxicant that yields RXS, and insufficiency of refurbishing micronutrients (Figure 1). A fourth factor must now be built into the equation, namely, gene mutations that might favour the cytoplasmic presence of trypsin (97): the enzyme, as also chymotrysin, is readily inhibited by GSH via SH-SS exchange (24) should it break loose of constraint by SPINK1 (serine protease inhibitor Kazal type 1) (118), but less GSH is then available for control of electrophilic / oxidative stress and other vital roles (24,30,162). The qualifying clauses help to explain why patients on CYP-inducing anticonvulsant drugs rarely develop chronic pancreatitis, or why profound electrophilic / oxidative stress but with low CYP activity in children with kwashiorkor results in painless loss of acini, not chronic pancreatitis (64).…”

Section: Electrophilic Stress Template Component Clausesmentioning

confidence: 99%

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Micronutrient ('Antioxidant') Therapy for Chronic Pancreatitis: Basis and Clinical Experience

Braganza

The Pancreapedia: Exocrine Pancreas Knowledge Base

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Genetics of Pancreatitis: The 2014 Update

Cited by 49 publications

References 51 publications

Establishing a Clinic-Based Pancreatic Cancer and Periampullary Tumour Research Registry in Quebec

Establishing a Clinic-Based Pancreatic Cancer and Periampullary Tumour Research Registry in Quebec

Functional significance of SPINK1 promoter variants in chronic pancreatitis

Micronutrient ('Antioxidant') Therapy for Chronic Pancreatitis: Basis and Clinical Experience

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