Your search keyword '"Witt H"' showing total 37 results

1. Genetic Analysis of the ATG16L1 c.898A>G (p.T300A) Variant in Acute and Chronic Pancreatitis.

Author

Neubauer C, Ewers M, Schulz HU, Weiß FU, Lämmerhirt F, Lerch MM, Bugert P, Landt O, Algül H, Rosendahl J, and Witt H

Subjects

Animals, Humans, Acute Disease, Autophagy-Related Proteins genetics, Gene Frequency, Genetic Predisposition to Disease, Autophagy genetics, Polymorphism, Single Nucleotide, Pancreatitis genetics, Crohn Disease

Abstract

Objectives: Human and animal studies suggest an important role of autophagy in the pathogenesis of pancreatitis. ATG16L1 (autophagy-related 16 like 1) is part of a protein complex that is involved in the formation of autophagosomes. The c.898A > G (p.T300A) variant of ATG16L1 is associated with Crohn disease. In this study, we analyzed ATG16L1 c.898A > G (p.T300A) for an association with pancreatitis., Methods: We genotyped 777 patients and 551 control subjects of German origin by melting curve analysis using fluorescence resonance energy transfer probes. The patient group included 429 patients with nonalcoholic chronic pancreatitis (CP), 141 patients with alcoholic CP, and 207 patients with acute pancreatitis (AP). We classified AP by severity according to the Atlanta symposium 1992., Results: Allele and genotype frequencies of ATG16L1 c.898A > G (p.T300A) did not differ significantly between patients and controls (G allele frequencies: nonalcoholic CP, 49.9%; alcoholic CP, 48.2%; AP, 49.5%; controls, 52.7%). We found no significant association with the severity of AP either., Conclusions: Our data do not support a role of ATG16L1 c.898A > G (p.T300A) in the pathogenesis of AP or CP or an influence on the severity of AP., Competing Interests: The authors declare no conflict of interest., (Copyright © 2023 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2022

2. Analysis of GPRC6A variants in different pancreatitis etiologies.

Author

Kaune T, Ruffert C, Hesselbarth N, Damm M, Krug S, Cardinal von Widdern J, Masson E, Chen JM, Rebours V, Buscail L, Férec C, Grützmann R, Te Morsche RHM, Drenth JP, Cavestro GM, Zuppardo RA, Saftoiu A, Malecka-Panas E, Głuszek S, Bugert P, Lerch MM, Sendler M, Weiss FU, Zou WB, Deng SJ, Liao Z, Scholz M, Kirsten H, Hegyi P, Witt H, Michl P, Griesmann H, and Rosendahl J

Subjects

Adult, Aged, Asian People, DNA genetics, Europe, Female, Genetic Predisposition to Disease, Genetic Variation, Genome-Wide Association Study, Humans, Male, Middle Aged, Pancreatitis, Alcoholic genetics, Polymorphism, Single Nucleotide, Receptors, Calcium-Sensing genetics, Risk Factors, Signal Transduction genetics, White People, Pancreatitis genetics, Receptors, G-Protein-Coupled genetics

Abstract

Background: The G-protein-coupled receptor Class C Group 6 Member A (GPRC6A) is activated by multiple ligands and is important for the regulation of calcium homeostasis. Extracellular calcium is capable to increase NLRP3 inflammasome activity of the innate immune system and deletion of this proinflammatory pathway mitigated pancreatitis severity in vivo. As such this pathway and the GPRC6A receptor is a reasonable candidate gene for pancreatitis. Here we investigated the prevalence of sequence variants in the GPRC6A locus in different pancreatitis aetiologies., Methods: We selected 6 tagging SNPs with the SNPinfo LD TAG SNP Selection tool and the functional relevant SNP rs6907580 for genotyping. Cohorts from Germany, further European countries and China with up to 1,124 patients and 1,999 controls were screened for single SNPs with melting curve analysis., Results: We identified an association of rs1606365(G) with alcoholic chronic pancreatitis in a German (odds ratio (OR) 0.76, 95% confidence interval (CI) 0.65-0.89, p = 8 × 10 -5 ) and a Chinese cohort (OR 0.78, 95% CI 0.64-0.96, p = 0.02). However, this association was not replicated in a combined cohort of European patients (OR 1.18, 95% CI 0.99-1.41, p = 0.07). Finally, no association was found with acute and non-alcoholic chronic pancreatitis., Conclusions: Our results support a potential role of calcium sensing receptors and inflammasome activation in alcoholic chronic pancreatitis development. As the functional consequence of the associated variant is unclear, further investigations might elucidate the relevant mechanisms., Competing Interests: Declaration of competing interest The authors report no conflicts of interest., (Copyright © 2020 IAP and EPC. Published by Elsevier B.V. All rights reserved.)

Published

2020

3. EPC/HPSG evidence-based guidelines for the management of pediatric pancreatitis.

Author

Párniczky A, Abu-El-Haija M, Husain S, Lowe M, Oracz G, Sahin-Tóth M, Szabó FK, Uc A, Wilschanski M, Witt H, Czakó L, Grammatikopoulos T, Rasmussen IC, Sutton R, and Hegyi P

Subjects

Child, Europe, Humans, Risk Factors, Societies, Medical, Pancreatitis therapy, Practice Guidelines as Topic

Abstract

Background: Pediatric pancreatitis is an underdiagnosed disease with variable etiology. In the past 10-15 years the incidence of pediatric pancreatitis has increased, it is now 3.6-13.3 cases per 100,000 children. Up-to-date evidence based management guidelines are lacking for the pediatric pancreatitis. The European Pancreatic Club, in collaboration with the Hungarian Pancreatic Study Group organized a consensus guideline meeting on the diagnosis and management of pancreatitis in the pediatric population., Methods: Pediatric Pancreatitis was divided into three main clinical categories: acute pancreatitis, acute recurrent pancreatitis and chronic pancreatitis. Fifteen relevant topics (acute pancreatitis: diagnosis; etiology; prognosis; imaging; complications; therapy; biliary tract management; acute recurrent pancreatitis: diagnosis; chronic pancreatitis: diagnosis, etiology, treatment, imaging, intervention, pain, complications; enzyme replacement) were defined. Ten experts from the USA and Europe reviewed and summarized the available literature. Evidence was classified according to the GRADE classification system., Results: Within fifteen topics, forty-seven relevant clinical questions were defined. The draft of the updated guideline was presented and discussed at the consensus meeting held during the 49th Meeting of European Pancreatic Club, in Budapest, on July 1, 2017., Conclusions: These evidence-based guidelines provides the current state of the art of the diagnosis and management of pediatric pancreatitis., (Copyright © 2018 IAP and EPC. Published by Elsevier B.V. All rights reserved.)

Published

2018

4. BCL3 Reduces the Sterile Inflammatory Response in Pancreatic and Biliary Tissues.

Author

Song L, Wörmann S, Ai J, Neuhöfer P, Lesina M, Diakopoulos KN, Ruess D, Treiber M, Witt H, Bassermann F, Halangk W, Steiner JM, Esposito I, Rosendahl J, Schmid RM, Riemann M, and Algül H

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, ATP Binding Cassette Transporter, Subfamily B metabolism, Acute Disease, Animals, B-Cell Lymphoma 3 Protein, Bile Ducts pathology, Bone Marrow Transplantation, Ceruletide, Cholangitis, Sclerosing genetics, Cholangitis, Sclerosing metabolism, Cholangitis, Sclerosing pathology, Humans, I-kappa B Proteins metabolism, Mice, Inbred C57BL, Mice, Knockout, NF-KappaB Inhibitor alpha, NF-kappa B p50 Subunit metabolism, Pancreas pathology, Pancreatitis chemically induced, Pancreatitis genetics, Pancreatitis metabolism, Pancreatitis pathology, Phosphorylation, Proteasome Endopeptidase Complex metabolism, Protein Multimerization, Proteolysis, Proto-Oncogene Proteins deficiency, Proto-Oncogene Proteins genetics, Signal Transduction, Taurocholic Acid, Time Factors, Transcription Factor RelA metabolism, Transcription Factors deficiency, Transcription Factors genetics, Ubiquitination, ATP-Binding Cassette Sub-Family B Member 4, Bile Ducts metabolism, Cholangitis, Sclerosing prevention & control, Pancreas metabolism, Pancreatitis prevention & control, Proto-Oncogene Proteins metabolism, Transcription Factors metabolism

Abstract

Background & Aims: Under conditions of inflammation in the absence of micro-organisms (sterile inflammation), necrotic cells release damage-associated molecular patterns that bind to Toll-like receptors on immune cells to activate a signaling pathway that involves activation of IκB kinase and nuclear factor κB (NF-κB). Little is known about the mechanisms that control NF-κB activity during sterile inflammation. We analyzed the contribution of B-cell CLL/lymphoma 3 (BCL3), a transcription factor that associates with NF-κB, in control of sterile inflammation in the pancreas and biliary system of mice., Methods: Acute pancreatitis (AP) was induced in C57BL/6 (control) and Bcl3(-/-) mice by intraperitoneal injection of cerulein or pancreatic infusion of sodium taurocholate. We also studied Mdr2(-/-) mice, which develop spontaneous biliary inflammation, as well as Bcl3(-/-)Mdr2(-/-) mice. We performed immunohistochemical analyses of inflamed and noninflamed regions of pancreatic tissue from patients with AP or primary sclerosing cholangitis (PSC), as well as from mice. Immune cells were characterized by fluorescence-activated cell sorting analysis. Control or Bcl3(-/-) mice were irradiated, injected with bone marrow from Bcl3(-/-) or control mice, and AP was induced., Results: Pancreatic or biliary tissues from patients with AP or PSC had higher levels of BCL3 and phosphorylated RelA and IκBα in inflamed vs noninflamed regions. Levels of BCL3 were higher in pancreata from control mice given cerulein than from mice without AP, and were higher in biliary tissues from Mdr2(-/-) mice than from control mice. Bcl3(-/-) mice developed more severe AP after administration of cerulein or sodium taurocholate than control mice; pancreata from the Bcl3(-/-) mice with AP had greater numbers of macrophages, myeloid-derived suppressor cells, dendritic cells, and granulocytes than control mice with AP. Activation of NF-κB was significantly prolonged in Bcl3(-/-) mice with AP, compared with control mice with AP. Bcl3(-/-)Mdr2(-/-) mice developed more severe cholestasis and had increased markers of liver injury and increased proliferation of biliary epithelial cells and hepatocytes than Mdr2(-/-) mice. In experiments with bone marrow chimeras, expression of BCL3 by acinar cells, but not myeloid cells, was required for reduction of inflammation during development of AP. BCL3 inhibited ubiquitination and proteasome-mediated degradation of p50 homodimers, which prolonged binding of NF-κB heterodimers to DNA., Conclusions: BCL3 is up-regulated in inflamed pancreatic or biliary tissues from mice and patients with AP or cholangitis. Its production appears to reduce the inflammatory response in these tissues via blocking ubiquitination and proteasome-mediated degradation of p50 homodimers., (Copyright © 2016 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2016

5. English language version of the S3-consensus guidelines on chronic pancreatitis: Definition, aetiology, diagnostic examinations, medical, endoscopic and surgical management of chronic pancreatitis.

Author

Hoffmeister A, Mayerle J, Beglinger C, Büchler MW, Bufler P, Dathe K, Fölsch UR, Friess H, Izbicki J, Kahl S, Klar E, Keller J, Knoefel WT, Layer P, Loehr M, Meier R, Riemann JF, Rünzi M, Schmid RM, Schreyer A, Tribl B, Werner J, Witt H, Mössner J, and Lerch MM

Subjects

Chronic Disease, Germany, Humans, United States, Endoscopy, Gastrointestinal standards, Pancreatectomy standards, Pancreatic Function Tests standards, Pancreatitis diagnosis, Pancreatitis therapy, Practice Guidelines as Topic

Abstract

Chronic pancreatitis is a disease of the pancreas in which recurrent inflammatory episodes result in replacement of pancreatic parenchyma by fibrous connective tissue. This fibrotic reorganization of the pancreas leads to a progressive exocrine and endocrine pancreatic insufficiency. In addition, characteristic complications arise, such as pseudocysts, pancreatic duct obstructions, duodenal obstruction, vascular complications, obstruction of the bile ducts, malnutrition and pain syndrome. Pain presents as the main symptom of patients with chronic pancreatitis. Chronic pancreatitis is a risk factor for pancreatic carcinoma. Chronic pancreatitis significantly reduces the quality of life and the life expectancy of affected patients. These guidelines were researched and compiled by 74 representatives from 11 learned societies and their intention is to serve evidence-based professional training as well as continuing education. On this basis they shall improve the medical care of affected patients in both the inpatient and outpatient sector. Chronic pancreatitis requires an adequate diagnostic workup and systematic management, given its severity, frequency, chronicity, and negative impact on the quality of life and life expectancy., (© Georg Thieme Verlag KG Stuttgart · New York.)

Published

2015

6. Rapid progression of a splenic aneurysm due to segmental arterial mediolysis: a rare cause of acute pancreatitis.

Author

Löhr JM, Dinter D, Diehl SJ, Haas SL, Veeser M, Pfützer R, Retter J, Schönberg SO, Düber C, Keim V, Schadendorf D, and Witt H

Subjects

Abdominal Pain etiology, Aneurysm diagnostic imaging, Aneurysm, Ruptured complications, Blood Pressure, Humans, Male, Radiography, Radiology, Interventional, Sexual Dysfunctions, Psychological complications, Aneurysm complications, Pancreatitis etiology, Splenic Artery

Abstract

Background: The etiology of acute pancreatitis can be manifold, beside the usual causes. We are reporting an unusual cause that triggered acute pancreatitis., Patient & Results: A 50 year-old male experienced attacks of acute pancreatitis (abdominal pain and elevated amylase and lipase) during sexual arousal. Serial imaging showed a rapidly-progressing, partly-thrombosed splenic artery aneurysm, with local compression of the pancreas. After angiographic coiling, the attacks subsided. Further angiography revealed additional aneurysms consistent with segmental arterial mediolysis at other sites of the body. Molecular analysis regarding Ehlers-Danlos-syndrome and genetic factors for pancreatitis, autoantibodies and Syphilis serology was negative., Conclusions: Acute pancreatitis was triggered by a transient rise in blood pressure during sexual stimulation, which caused rapid progression of a splenic artery aneurysm as part of systemic segmental arterial mediolysis., (Copyright © 2013 IAP and EPC. Published by Elsevier B.V. All rights reserved.)

Published

2013

7. Deletion of IκBα activates RelA to reduce acute pancreatitis in mice through up-regulation of Spi2A.

Author

Neuhöfer P, Liang S, Einwächter H, Schwerdtfeger C, Wartmann T, Treiber M, Zhang H, Schulz HU, Dlubatz K, Lesina M, Diakopoulos KN, Wörmann S, Halangk W, Witt H, Schmid RM, and Algül H

Subjects

Acinar Cells, Animals, Arginine, Ceruletide, Cytosol metabolism, Disease Models, Animal, Gene Expression Profiling, Genetic Vectors, Genotype, I-kappa B Proteins metabolism, Lentivirus, Mice, Mice, Inbred C57BL, Microarray Analysis, NF-KappaB Inhibitor alpha, Nuclear Proteins metabolism, Pancreas enzymology, Pancreatitis chemically induced, Pancreatitis pathology, Phosphorylation, Serpins metabolism, Signal Transduction, Transcription Factor RelA metabolism, Trypsin metabolism, Up-Regulation, I-kappa B Proteins genetics, NF-kappa B metabolism, Pancreatitis genetics, Pancreatitis metabolism, Serpins genetics, Transcription Factor RelA genetics, alpha 1-Antichymotrypsin genetics

Abstract

Background & Aims: The transcription factor nuclear factor-κB (NF-κB) (a heterodimer of NF-κB1p50 and RelA) is activated rapidly in acute pancreatitis (AP). However, it is not clear whether NF-κB promotes or protects against AP. We used the NF-κB inhibitor protein, inhibitor of κB (IκB)α, to study the roles of NF-κB in the development of AP in mice., Methods: IκBα or the combination of IκBα and RelA selectively were deleted from pancreas of mice using the Cre/locus of cross-over P strategy; cerulein or L-arginine were used to induce AP. We performed microarray analyses of the IκBα- and RelA-deficient pancreata. DNA from healthy individuals and patients with acute or chronic pancreatitis were analyzed for variants in coding regions of alpha-1-antichymotrypsin., Results: Mice with pancreas-specific deletion of IκBα had constitutive activation of RelA and a gene expression profile consistent with NF-κB activation; development of AP in these mice was attenuated and trypsin activation was impaired. However, AP was fully induced in mice with pancreas-specific deletion of IκBα and RelA. By using genome-wide expression analysis, we identified a cluster of NF-κB-regulated genes that might protect against the development of AP. The serine protease inhibitor 2A (Spi2a) was highly up-regulated in IκBα-deficient mice. Lentiviral-mediated expression of Spi2A reduced the development of AP in C57BL/6 and RelA-deficient mice. However, we did not correlate any variants of alpha-1-antichymotrypsin, the human homologue of Spi2a, with acute or chronic pancreatitis., Conclusions: Pancreas-specific deletion of IκBα results in nuclear translocation of RelA and reduces AP induction and trypsin activation in mice after administration of cerulein or L-arginine. Constitutive activation of RelA up-regulates Spi2A, which protects mice against the development of AP., (Copyright © 2013 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2013

8. Opie's hypothesis revisited: acute pancreatitis due to bile reflux into the pancreas.

Author

Löhr JM, Schneider A, Diehl SJ, and Witt H

Subjects

Adult, Humans, Male, Pancreatitis surgery, Sphincterotomy, Transduodenal methods, Bile Reflux complications, Cholangiography methods, Cholangiopancreatography, Endoscopic Retrograde methods, Pancreatitis etiology

Published

2012

9. Genetic analyses of heme oxygenase 1 (HMOX1) in different forms of pancreatitis.

Author

Weis S, Jesinghaus M, Kovacs P, Schleinitz D, Schober R, Ruffert C, Herms M, Wittenburg H, Stumvoll M, Blüher M, Grützmann R, Schulz HU, Keim V, Mössner J, Bugert P, Witt H, Drenth JP, Krohn K, and Rosendahl J

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Case-Control Studies, Child, Female, Humans, Liver Cirrhosis, Alcoholic enzymology, Liver Cirrhosis, Alcoholic genetics, Male, Middle Aged, Polymorphism, Single Nucleotide genetics, Promoter Regions, Genetic genetics, Repetitive Sequences, Nucleic Acid genetics, Sequence Analysis, DNA, Young Adult, Heme Oxygenase-1 genetics, Pancreatitis enzymology, Pancreatitis genetics

Abstract

Background: Heme oxygenase 1 (HMOX1) is the rate limiting enzyme in heme degradation and a key regulator of inflammatory processes. In animal models the course of pancreatitis was ameliorated by up-regulation of HMOX1 expression. Additionally, carbon monoxide released during heme breakdown inhibited proliferation of pancreatic stellate cells and might thereby prevent the development of chronic pancreatitis (CP). Transcription of HMOX1 in humans is influenced by a GT-repeat located in the promoter. As such, HMOX1 variants might be of importance in the pathogenesis of pancreatitis., Methods: The GT-repeat and SNP rs2071746 were investigated with fluorescence labelled primers and by melting curve analysis in 285 patients with acute pancreatitis, 208 patients with alcoholic CP, 207 patients with idiopathic/hereditary CP, 147 patients with alcoholic liver cirrhosis, and in 289 controls, respectively. GT-repeat analysis was extended to a total of 446 alcoholic CP patients. In addition, we performed DNA sequencing in 145 patients with alcoholic CP, 138 patients with idiopathic/hereditary CP, 147 patients with alcoholic liver cirrhosis, and 151 controls. Exon 3 screening was extended to additional patients and controls., Results: S- and L-alleles of the GT-repeat, genotypes and alleles of SNP rs2071746 and non-synonymous variants detected by sequencing were found with similar frequencies in all groups., Conclusions: Although functional data implicate a potential influence of HMOX1 variants on the pathogenesis of pancreatitis, we did not find any association. As rare non-synonymous HMOX1 variants were found in patients and controls, it is rather unlikely that they will have functional consequences essential for pancreatitis development.

Published

2012

10. Genetics of pancreatitis: a guide for clinicians.

Author

Witt H

Subjects

Alcoholism complications, Humans, Pancreatitis complications, Pancreatitis genetics, Practice Guidelines as Topic

Abstract

It is now generally believed that pancreatitis results from pancreatic autodigestion. An inappropriate conversion of pancreatic zymogens to active enzymes within the pancreatic parenchyma is thought to initiate the inflammatory process. A key role has been attributed to the activation of trypsinogen to trypsin, converting all proteolytic proenzymes to their active form. Several gain-of-function mutations in the cationic trypsinogen gene (PRSS1) have been identified in patients with chronic pancreatitis (CP). These mutations lead to enhanced intrapancreatic trypsinogen activation. In contrast, a variant in the anionic trypsinogen (PRSS2) gene, p.G191R, has been described that mitigates intrapancreatic trypsin activity and thereby plays a protective role. Beside trypsinogen mutations, loss-of-function variants in SPINK1, encoding a pancreatic trypsin inhibitor, are strongly associated with idiopathic CP. Approximately 15-40% of patients with so-called idiopathic CP carry p.N34S on one allele or on both alleles. Chymotrypsin C (CTRC) degrades all human trypsin isoforms with high specificity. Two CTRC alterations, p.R254W and p.K247_R254del, are significantly associated with idiopathic as well as alcohol-related CP. Functional analysis of the variants revealed impaired activity and/or reduced secretion. Thus, loss-of-function mutations in CTRC predispose to pancreatitis by diminishing its protective trypsin-degrading activity. Albeit the association between CFTR, the gene mutated in cystic fibrosis, and idiopathic CP is now well established, the pathogenic mechanisms are poorly understood. Nearly 25-30% of patients carry at least one CFTR mutation, but few patients only were compound-heterozygous. Several patients, however, are trans-heterozygous for a CFTR alteration and a PRSS1, SPINK1, or CTRC variant, respectively., (Copyright © 2011 S. Karger AG, Basel.)

Published

2010

11. Angiotensin-converting enzyme insertion/deletion polymorphism in patients with acute and chronic pancreatitis.

Author

Hucl T, Kylanpää ML, Künzli B, Witt H, Lempinen M, Schneider A, Kemppainen E, Löhr M, Haas SL, Friess H, Ockenga J, Rosendahl J, Schulz HU, Gress T, Singer MV, and Pfützer RH

Subjects

Acute Disease, Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Disease Susceptibility, Female, Finland, Genotype, Germany, Humans, Male, Middle Aged, Pancreatitis metabolism, Pancreatitis, Chronic metabolism, Peptidyl-Dipeptidase A metabolism, Young Adult, Gene Deletion, Mutagenesis, Insertional genetics, Pancreatitis genetics, Pancreatitis, Chronic genetics, Peptidyl-Dipeptidase A genetics, Polymorphism, Genetic

Abstract

Background: Reduction in angiotensin-converting enzyme (ACE) activity has been shown to attenuate pancreatic stellate cell activation and pancreatic fibrosis and suggested as a potential treatment for chronic pancreatitis. The ACE gene insertion/deletion (I/D) polymorphism in intron 16 accounts for nearly half the variation in serum ACE levels. This study determined the frequency of the I/D polymorphism in patients with acute and chronic pancreatitis., Methods: In total, 887 patients (346 with alcoholic, 443 with nonalcoholic, and 98 with acute pancreatitis) were enrolled, and were compared with 1294 healthy controls. Genotyping of the I/D polymorphism was performed by PCR or melting curve analyses., Results: No significant differences were found in the prevalence of the ACE-deletion genotype frequencies when patients with alcoholic (27.5%), nonalcoholic (26.4%), and acute pancreatitis (32.7%) were compared with controls (26.9%). Likewise, allele frequencies of the ACE deletion polymorphism were not significantly different in patients with alcoholic (53.8%), nonalcoholic (50.6%), and acute pancreatitis (54.1%) and controls (52.7%)., Conclusion: The I/D polymorphism of the ACE gene was not found to be associated with acute and chronic pancreatitis.

Published

2009

12. The SPINK1 N34S variant is associated with acute pancreatitis.

Author

O'Reilly DA, Witt H, Rahman SH, Schulz HU, Sargen K, Kage A, Cartmell MT, Landt O, Larvin M, Demaine AG, McMahon MJ, Becker M, and Kingsnorth AN

Subjects

Acute Disease, Adolescent, Adult, Age of Onset, Aged, Aged, 80 and over, Female, Gene Frequency, Genetic Predisposition to Disease, Humans, Male, Middle Aged, Phenotype, Polymerase Chain Reaction methods, Polymorphism, Single-Stranded Conformational, Trypsin Inhibitor, Kazal Pancreatic, Carrier Proteins genetics, Pancreatitis genetics

Abstract

Objective: Acute pancreatitis (AP) is a disease whose pathogenesis remains largely obscure. Genetic research has focussed attention upon the role of the pancreatic protease/protease inhibitor system. The aim of this study was to investigate the prevalence of genetic variants of the trypsin inhibitor, SPINK1, in acute pancreatitis., Methods: We genotyped 468 patients with AP and 1117 healthy controls for SPINK1 alterations by single-strand conformation polymorphism analysis and by melting curve analysis using fluorescence resonance energy transfer probes., Results: The c.101A>G (p.N34S) variant was detected in 24/936 alleles of patients and in 18/2234 alleles of healthy controls (odds ratio=3.240; 95% confidence interval: 1.766-5.945; P<0.001). In the UK patients, the mean age of patients with N34S was 11.9 years younger compared with N34S negative patients (P=0.023), but this was not apparent in the German patients. Allele frequencies for the c.163C>T (p.P55S) variant did not differ between patients and controls., Conclusion: The SPINK1 N34S variant is associated with acute pancreatitis. This supports the importance of premature protease activation in the pathogenesis of AP and suggests that mutated SPINK1 may predispose certain individuals to develop this disease.

Published

2008

13. Signal peptide variants that impair secretion of pancreatic secretory trypsin inhibitor (SPINK1) cause autosomal dominant hereditary pancreatitis.

Author

Király O, Boulling A, Witt H, Le Maréchal C, Chen JM, Rosendahl J, Battaggia C, Wartmann T, Sahin-Tóth M, and Férec C

Subjects

Adolescent, Amino Acid Sequence, Animals, Base Sequence, Blotting, Western, CHO Cells, Carrier Proteins chemistry, Child, Cricetinae, Cricetulus, DNA Primers, Female, Humans, Male, Molecular Sequence Data, Pedigree, Reverse Transcriptase Polymerase Chain Reaction, Trypsin Inhibitor, Kazal Pancreatic, Carrier Proteins metabolism, Genes, Dominant, Pancreatitis genetics, Protein Sorting Signals genetics

Abstract

Variants of the SPINK1 gene encoding pancreatic secretory trypsin inhibitor have been described in association with chronic pancreatitis (CP). These alterations are believed to cause a loss of function by either impairing the trypsin inhibitory activity or reducing expression. Here we report two novel SPINK1 variants in exon 1 that affect the secretory signal peptide. The disease-associated c.41T>G (p.L14R) alteration was found in two European families with autosomal dominant hereditary pancreatitis, whereas the c.36G>C (p.L12F) variant was identified as a frequent alteration in subjects of African descent. The functional effects of both alterations and the previously reported c.41T>C (p.L14P) variant were characterized by activity assays and Western blots of wild-type and mutant SPINK1 expressed in human embryonic kidney 293T and Chinese hamster ovary cells. Alterations p.L14R and p.L14P destined the inhibitor for rapid intracellular degradation and thereby abolished SPINK1 secretion, whereas the p.L12F variant showed no detrimental effect. The results provide the first clear experimental demonstration that alterations that markedly reduce SPINK1 expression are associated with classic hereditary pancreatitis. Therefore, these variants should be classified as severe and regarded as disease-causing rather than disease-modifiers., (2007 Wiley-Liss, Inc.)

Published

2007

14. Keratin 8 sequence variants in patients with pancreatitis and pancreatic cancer.

Author

Treiber M, Schulz HU, Landt O, Drenth JP, Castellani C, Real FX, Akar N, Ammann RW, Bargetzi M, Bhatia E, Demaine AG, Battagia C, Kingsnorth A, O'Reilly D, Truninger K, Koudova M, Spicak J, Cerny M, Menzel HJ, Moral P, Pignatti PF, Romanelli MG, Rickards O, De Stefano GF, Zarnescu NO, Choudhuri G, Sikora SS, Jansen JB, Weiss FU, Pietschmann M, Teich N, Gress TM, Ockenga J, Schmidt H, Kage A, Halangk J, Rosendahl J, Groneberg DA, Nickel R, and Witt H

Subjects

Acute Disease, Adenocarcinoma genetics, Adenocarcinoma pathology, Adult, Aged, Alleles, Asian People genetics, Black People genetics, Carcinoma, Pancreatic Ductal genetics, Carcinoma, Pancreatic Ductal pathology, Case-Control Studies, Chronic Disease, Cohort Studies, Female, Gene Frequency, Geography, Heterozygote, Humans, Male, Middle Aged, Pancreatic Neoplasms pathology, Pancreatitis pathology, Pancreatitis, Alcoholic pathology, Polymorphism, Genetic, Retrospective Studies, White People genetics, Genetic Variation, Keratin-8 genetics, Pancreatic Neoplasms genetics, Pancreatitis genetics, Pancreatitis, Alcoholic genetics

Abstract

Keratin 8 (KRT8) is one of the major intermediate filament proteins expressed in single-layered epithelia of the gastrointestinal tract. Transgenic mice over-expressing human KRT8 display pancreatic mononuclear infiltration, interstitial fibrosis and dysplasia of acinar cells resulting in exocrine pancreatic insufficiency. These experimental data are in accordance with a recent report describing an association between KRT8 variations and chronic pancreatitis. This prompted us to investigate KRT8 polymorphisms in patients with pancreatic disorders. The KRT8 Y54H and G62C polymorphisms were assessed in a cohort of patients with acute and chronic pancreatitis of various aetiologies or pancreatic cancer originating from Austria (n=16), the Czech Republic (n=90), Germany (n=1698), Great Britain (n=36), India (n=60), Italy (n=143), the Netherlands (n=128), Romania (n=3), Spain (n=133), and Switzerland (n=129). We also studied 4,234 control subjects from these countries and 1,492 control subjects originating from Benin, Cameroon, Ethiopia, Ecuador, and Turkey. Polymorphisms were analysed by melting curve analysis with fluorescence resonance energy transfer probes. The frequency of G62C did not differ between patients with acute or chronic pancreatitis, pancreatic adenocarcinoma and control individuals. The frequency of G62C varied in European populations from 0.4 to 3.8%, showing a northwest to southeast decline. The Y54H alteration was not detected in any of the 2,436 patients. Only 3/4,580 (0.07%) European, Turkish and Indian control subjects were heterozygous for Y54H in contrast to 34/951 (3.6%) control subjects of African descent. Our data suggest that the KRT8 alterations, Y54H and G62C, do not predispose patients to the development of pancreatitis or pancreatic cancer.

Published

2006

15. Analysis of tumour necrosis factor alpha and interleukin 10 promotor variants in patients with chronic pancreatitis.

Author

Beranek H, Teich N, Witt H, Schulz HU, Mössner J, and Keim V

Subjects

Case-Control Studies, Chronic Disease, Gene Frequency, Genetic Markers, Humans, Pancreatitis genetics, Pancreatitis, Alcoholic etiology, Pancreatitis, Alcoholic genetics, Interleukin-10 genetics, Pancreatitis etiology, Polymorphism, Genetic, Promoter Regions, Genetic, Tumor Necrosis Factor-alpha genetics

Abstract

Objective: Cationic trypsinogen gene mutations are strong risk factors of hereditary pancreatitis. However, 20% of subjects with a trypsinogen mutation never get pancreatitis and the cause of this incomplete penetrance is unknown. We investigated the influence of interleukin 10 (IL10) and tumour necrosis factor alpha (TNFalpha) promotor variants on the manifestation of chronic pancreatitis of different underlying causes and in pancreatic cancer., Methods: A total of 335 German patients with chronic pancreatitis were investigated. In 157 patients the disease was related to alcohol abuse; the other cases were of non-alcoholic origin. In the latter group, the serine protease inhibitor, Kazal type 1 (SPINK1) mutation N34S was found in 72 patients and the trypsinogen mutations N29I or R122H were present in 60 patients; in the remaining 46 patients no mutation was found. In addition, we studied 208 patients with pancreatic cancer. As controls, 116 healthy blood donors and 25 healthy carriers of the trypsinogen mutations N29I or R122H were investigated. After DNA extraction from blood leucocytes, genotyping for the cytokine polymorphisms was performed by induced heteroduplex generators and/or direct DNA sequencing of the IL10 and TNFalpha promotor regions., Results: The frequencies of the promotor polymorphisms of IL10-627A, IL10-1117A, TNF-238A and TNF-308A in patients with alcoholic chronic pancreatitis, idiopathic pancreatitis, SPINK1-N34S-associated chronic pancreatitis and pancreatic cancer did not differ significantly from the control group. The variant TNF-238A was two to four times more frequent in index patients with trypsinogen mutations than in all other groups. The analysis of the allelic frequencies of whole families with trypsinogen mutations revealed that all subjects with the TNF-238A variant suffered from chronic pancreatitis, whereas all intrafamilial controls with wild-type TNF were unaffected., Conclusions: TNFalpha and IL10 promotor variants are not associated with a manifestation of chronic pancreatitis or pancreatic cancer. The variant TNF-238A, however, might be a relevant risk factor for disease manifestation in families with hereditary pancreatitis.

Published

2003

16. The course of genetically determined chronic pancreatitis.

Author

Keim V, Witt H, Bauer N, Bodeker H, Rosendahl J, Teich N, and Mossner J

Subjects

Case-Control Studies, Child, Chronic Disease, Disease Progression, Follow-Up Studies, Genetic Predisposition to Disease, Humans, Mutation, Pancreatitis diagnosis, Pancreatitis genetics, Trypsin, Trypsin Inhibitor, Kazal Pancreatic genetics, Trypsinogen genetics

Abstract

Context: The clinical course of chronic pancreatitis in patients with mutations of cationic trypsinogen and the trypsin inhibitor SPINK1 has not yet been characterized., Setting: Cationic trypsinogen (PRSS1) and the serine protease inhibitor, Kazal type 1 (SPINK1), were analyzed in patients with pancreatitis of unclear origin., Patients: Eighty subjects with trypsinogen mutations (21x N29I, 59x R122H) and 59 patients with the SPINK1 N34S variant (11 homozygous, 48 heterozygous) were included in the study., Main Outcome Measures: In patients with mutations of PRSS1 (N29I, R122H) and SPINK1 (N34S) the parameters such as calcification, dilatation of the main pancreatic duct, diabetes mellitus, hospital treatments, and surgery were recorded., Design: Case control studies were performed to compare both mutational groups, and the follow-up time served as a matching criterion. The Kaplan-Meier analysis was used to estimate the time course of the symptoms., Results: Ten years after the onset of the disease, the probability (+/-SE) of symptoms in patients with PRSS1 mutations was as follows: 1st hospital stay: 86+/-4%; calcification: 21+/-4%; duct dilatation: 26+/-9%; surgery: 19+/-5%; diabetes: 6+/-5%. After 25 years, we found the following data: 1st hospital stay: 96+/-3%; calcification: 38+/-8%; duct dilatation: 38+/-8%; surgery: 37+/-10%; diabetes: 28+/-8%. A case-control-study of 38 pairs of patients with either PRSS1 or SPINK1 mutations showed that the probability of duct dilatation, diabetes and calcification was slightly higher in patients having a SPINK1 mutation. There was no difference between those subjects with a homozygous or heterozygous SPINK1 mutation. In comparison to alcoholic chronic pancreatitis patients, the PRSS1 associated disease revealed a lower frequency of calcification and diabetes., Conclusions: The progression of chronic pancreatitis was slightly more rapid in patients with SPINK1 mutations than in patients with cationic trypsinogen mutations, but was much less than in those having alcoholic chronic pancreatitis.

Published

2003

17. Chronic pancreatitis and cystic fibrosis.

Author

Witt H

Subjects

Chronic Disease, Genetic Predisposition to Disease, Humans, Male, Models, Genetic, Mutation, Pancreatitis, Alcoholic genetics, Vas Deferens abnormalities, Cystic Fibrosis genetics, Pancreatitis genetics

Abstract

Recent discoveries of trypsinogen and trypsin inhibitor mutations in patients with chronic pancreatitis (CP) support the hypothesis that an inappropriate activation of pancreatic zymogens to active enzymes within the pancreatic parenchyma starts the inflammatory process. Current data suggest that CP may be inherited dominant, recessive, or complex as a result of mutations in the above mentioned or yet unidentified genes. Evaluation of patients with CP should include genetic testing. Cystic fibrosis (CF) is an autosomal recessive inherited disorder caused by mutations in the CF transmembrane conductance regulator (CFTR) gene and is characterised by pancreatic insufficiency and chronic bronchopulmonary infection. The progression and severity of pulmonary disease differs considerably between people with identical CFTR mutations and does not seem to correlate with the type or class of the CFTR mutation. The identification of further disease modifying genetic factors will increase the pathophysiological understanding and may help to identify new therapeutic targets.

Published

2003

18. SPINK1 mutations and phenotypic expression in patients with pancreatitis associated with trypsinogen mutations.

Author

Weiss FU, Simon P, Witt H, Mayerle J, Hlouschek V, Zimmer KP, Schnekenburger J, Domschke W, Neoptolemos JP, and Lerch MM

Subjects

DNA chemistry, DNA genetics, DNA Mutational Analysis, Family Health, Female, Humans, Male, Mutation, Mutation, Missense, Pancreatitis metabolism, Pancreatitis pathology, Pedigree, Phenotype, Polymorphism, Genetic, Severity of Illness Index, Trypsin Inhibitor, Kazal Pancreatic metabolism, Pancreatitis genetics, Trypsin Inhibitor, Kazal Pancreatic genetics, Trypsinogen metabolism

Published

2003

19. Tropical calcific pancreatitis: strong association with SPINK1 trypsin inhibitor mutations.

Author

Bhatia E, Choudhuri G, Sikora SS, Landt O, Kage A, Becker M, and Witt H

Subjects

Adult, Chronic Disease, Diabetes Mellitus genetics, Family Health, Female, Heterozygote, Homozygote, Humans, India, Male, Pedigree, Trypsinogen genetics, Pancreatitis genetics, Point Mutation, Trypsin, Trypsin Inhibitor, Kazal Pancreatic genetics

Abstract

Background & Aims: Tropical calcific pancreatitis (TCP) is a chronic pancreatitis unique to developing countries in tropical regions. The cause of TCP is obscure. Whereas environmental factors, such as protein energy malnutrition and ingestion of cassava, have been implicated, a genetic predisposition to the disease also may be important. In the present study we report on mutations in the serine protease inhibitor, Kazal type 1 (SPINK1) gene in north Indian patients with TCP., Methods: We studied 66 unrelated TCP patients (44 men, 49 with diabetes, and 6 with family history of TCP), 25 relatives, and 92 healthy control subjects. Samples were analyzed for SPINK1 variants (-53C>T, L14P, N34S, P55S, and 272T>C) and cationic trypsinogen (PRSS1) variants (A16V, K23R, N29I, and R122H) by melting curve analysis., Results: Twenty-nine patients (44%) carried the N34S missense mutation, of whom 9 (14%) were homozygotes. In contrast, only 2 (2.2%) control subjects were N34S heterozygotes (prevalence ratio 20.2; 95% confidence interval 5.0-81.8; P < 0.0001 vs. TCP). The severity of pancreatitis did not differ between TCP patients with or without N34S, or among those heterozygous or homozygous for N34S. Among TCP patients with or without diabetes, the frequency of N34S carriers (43% vs. 47%) and N34S homozygotes (14% vs. 12%) was similar., Conclusions: TCP is highly associated with the SPINK1 N34S mutation. The high prevalence of N34S in TCP patients with and without diabetes suggests that these 2 subtypes have a similar genetic predisposition. The genetic predisposition to TCP resembles, at least in part, the idiopathic chronic pancreatitis found in industrialized countries.

Published

2002

20. Mutations of the serine protease inhibitor, Kazal type 1 gene, in patients with idiopathic chronic pancreatitis.

Author

Truninger K, Witt H, Köck J, Kage A, Seifert B, Ammann RW, Blum HE, and Becker M

Subjects

Adult, Age of Onset, Chronic Disease, Cohort Studies, DNA analysis, Female, Gene Frequency, Heterozygote, Homozygote, Humans, Male, Pancreatitis epidemiology, Pancreatitis physiopathology, Reference Values, Pancreatitis genetics, Point Mutation, Trypsin Inhibitor, Kazal Pancreatic genetics

Abstract

Objective: The pathogenesis of chronic pancreatitis (CP) is poorly understood. Genetic studies revealed mutations in the cationic trypsinogen gene and an increased frequency of cystic fibrosis gene mutations in patients with CP. Recently, a point mutation (N34S) in the gene encoding the serine protease inhibitor, Kazal type 1 (SPINK1), was found in approximately 20% of patients with CP. The aim of our study was to determine the frequency of the N34S SPINKI gene mutation in a well-defined patient cohort with idiopathic CP (ICP) and to compare the incidence with healthy controls. In addition, we investigated the impact of this mutation on the long-term course of CP., Methods: Fourteen patients with early-onset and four patients with late-onset CP of our well-defined pancreatitis cohort were enrolled in the present study, and 397 healthy individuals served as a control population. Coding exonic and the flanking intronic sequences of SPINK1 were investigated by direct DNA sequencing. The mutations found were confirmed by melting curve analysis. In addition, the N34S mutation was detected by analyzing the DNA fragments generated by digestion with restriction enzyme TspR I. Clinical data of patients with the N34S mutation were compared with those without mutations., Results: The N34S mutation was detected in six of 14 (43%) patients with early-onset ICP. One patient was homozygous, and five patients were heterozygous for this mutation. The N34S mutation in a heterozygous state was found in four of 397 healthy controls (1.0%). The different allele frequency observed (seven of 28 vs four of 794) was significant (odds ratio = 66, 95% CI = 18-242, p < 0.0001). The clinical course was similar in patients with a mutation compared with those without a mutation. No other SPINKI mutations were detected. The N34S mutation was not found in patients with late-onset ICP., Conclusions: Our results indicate that the N34S mutation in the SPINKI gene is strongly associated with ICP, especially with the early-onset type. The natural course is similar in patients with mutations compared with SPINK1 mutation-negative patients. The N34S mutation may easily be screened for by restriction digestion with TspR I.

Published

2002

21. The SPINK in chronic pancreatitis: similar finds, different minds.

Author

Witt H

Subjects

Chronic Disease, DNA Mutational Analysis, Genetic Predisposition to Disease, Humans, Mutation, Pancreatitis genetics, Trypsin Inhibitor, Kazal Pancreatic genetics

Published

2002

22. Alpha1-antitrypsin genotypes in patients with chronic pancreatitis.

Author

Witt H, Kage A, Luck W, and Becker M

Subjects

Adolescent, Adult, Base Sequence, Case-Control Studies, Chi-Square Distribution, Child, Child, Preschool, Chronic Disease, Female, Genotype, Humans, Male, Molecular Sequence Data, Pancreatitis diagnosis, Polymerase Chain Reaction, Probability, Prognosis, Prospective Studies, Reference Values, Sensitivity and Specificity, alpha 1-Antitrypsin analysis, alpha 1-Antitrypsin Deficiency diagnosis, Mutation, Pancreatitis genetics, alpha 1-Antitrypsin genetics, alpha 1-Antitrypsin Deficiency genetics

Abstract

Background: An association between alpha1-antitrypsin deficiency and chronic pancreatitis (CP) has been reported in several case reports and two systematic studies. However, conflicting results have been shown in other studies of patients with CP. All previous studies were performed by phenotyping or by measurement of serum concentrations of alpha1-antitrypsin. The aim of this study was to investigate the relationship between alpha1-antitrypsin deficiency and CP by genetic analysis., Methods: Ninety-six unrelated children and adolescents with idiopathic or hereditary CP and 185 healthy controls were enrolled. DNA was extracted from peripheral blood leukocytes and the exons 5 and 7 of the alpha1-antitrypsin gene were amplified by polymerase chain reaction using mutagenic forward primers introducing a Taq I restriction site. Genotyping of the S allele and the Z allele was performed by restriction fragment length polymorphism analysis using Taq I., Results: Seven out of 96 patients (7.3%) with CP were heterozygous for an alpha1-antitrypsin deficiency allele (4 for the S allele and 3 for the Z allele). No patient was homozygous or compound heterozygous for these alleles. Twenty out of 185 control individuals (10.8%) were heterozygous for the S or Z allele (PiS: 12 controls; PiZ: 8 controls). No significant differences were found between the allele frequency in patients and the control individuals (P > 0.1)., Conclusions: Alpha1-antitrypsin deficiency is not related to the pathogenesis of idiopathic or hereditary CP.

Published

2002

23. Genetics of chronic pancreatitis.

Author

Witt H and Becker M

Subjects

Child, Chromosomes, Human, Pair 12, Chromosomes, Human, Pair 14, Chromosomes, Human, Pair 5, Chromosomes, Human, Pair 7, Chronic Disease, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Humans, Mutation genetics, Pancreatitis epidemiology, Pancreatitis etiology, Prevalence, Trypsin Inhibitor, Kazal Pancreatic genetics, Trypsinogen genetics, alpha 1-Antitrypsin genetics, Pancreatitis genetics, Trypsin

Published

2002

24. Genetic aspects of chronic pancreatitis: insights into aetiopathogenesis and clinical implications.

Author

Truninger K, Ammann RW, Blum HE, and Witt H

Subjects

Chronic Disease, Cystic Fibrosis genetics, Genetic Predisposition to Disease genetics, Genetic Testing, Genotype, Humans, Mutation, Pancreatitis genetics, Pancreatitis therapy, Polymorphism, Genetic, Trypsin Inhibitor, Kazal Pancreatic genetics, Trypsinogen genetics, Pancreatitis etiology, Trypsin

Abstract

The recent genetic discoveries in CP support the hypothesis that inappropriate intrapancreatic activation of zymogens by trypsin results in autodigestion and pancreatitis. Two different protective mechanisms prevent activation of the pancreatic digestive enzyme cascade. First, SPINK1 inhibits up to 20% of potential trypsin activity and, second, trypsin itself activates trypsin-like enzymes readily degrading trypsinogen and other zymogens. Pancreatitis may therefore be the result of an imbalance between proteases and their inhibitors within the pancreatic parenchyma. The discovery of PRSS1 mutations in families with CP was the first breakthrough in the understanding of the underlying genetic mechanisms. Enhanced trypsinogen activation may be the common initiating step in pancreatitis caused by these mutations. The discovery of SPINK1 mutations underlines the importance of the protease inhibitor system in the pathogenesis of CP. Thus, gain-of-function in the cationic trypsinogen resulting in an enhanced autoactivation, or loss-of-function mutations in SPINK1 leading to decreased inhibitory capacity, may similarly disturb the delicate intrapancreatic balance of proteases and their inhibitors. The recent findings of SPINK1, CFTR, and PRSS1 mutations in CP patients without a family history have challenged the concept of idiopathic CP as a non-genetic disorder and the differentiation between HP and ICP. There is a clear mode of autosomal dominant inheritance for some mutations (R122H, N291, possibly MIT), whereas the inheritance pattern (autosomal recessive, complex, or modifying) of other mutations (A16V, N34S) is controverted or unknown. The lack of mutations in the above-mentioned genes in many patients suggests that CP may also be caused by genetic alterations in yet unidentified genes. Evaluation of CP patients without an obvious predisposing factor, e.g. alcohol abuse, should include genetic testing even in the absence of a family history of pancreatitis. Finally, identification of further disease-causing genes will create a better understanding of pathogenesis and may help to develop specific preventive and therapeutic strategies.

Published

2001

25. [Genetic aspects of chronic pancreatitis].

Author

Witt H, Simon P, and Lerch MM

Subjects

Chronic Disease, Humans, Pancreatitis physiopathology, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Mutation, Pancreatitis genetics, Trypsin Inhibitor, Kazal Pancreatic genetics, Trypsinogen genetics

Published

2001

26. Mutation in the SPINK1 trypsin inhibitor gene, alcohol use, and chronic pancreatitis.

Author

Witt H, Luck W, Becker M, Böhmig M, Kage A, Truninger K, Ammann RW, O'Reilly D, Kingsnorth A, Schulz HU, Halangk W, Kielstein V, Knoefel WT, Teich N, and Keim V

Subjects

Chronic Disease, Humans, Mutation, Pancreatitis etiology, Alcoholism complications, Pancreatitis genetics, Trypsin Inhibitor, Kazal Pancreatic genetics

Published

2001

27. SPINK1 mutations in chronic pancreatitis.

Author

Witt H, Hennies HC, and Becker M

Subjects

Chronic Disease, Humans, Mutation, Pancreatitis genetics, Trypsin Inhibitor, Kazal Pancreatic genetics

Published

2001

28. Gene mutations in children with chronic pancreatitis.

Author

Witt H

Subjects

Child, Chronic Disease, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Humans, Serine Proteinase Inhibitors genetics, Trypsinogen genetics, alpha 1-Antitrypsin genetics, Mutation genetics, Pancreatitis genetics, Trypsin

Abstract

In the last few years, several genes have been identified as being associated with hereditary and idiopathic chronic pancreatitis (CP), i.e. PRSS1, CFTR and SPINK1. In this study, we investigated 164 unrelated children and adolescents with CP for mutations in disease-associated genes by direct DNA sequencing, SSCP, RFLP and melting curve analysis. In 15 patients, we detected a PRSS1 mutation (8 with A16V, 5 with R122H, 2 with N29I), and in 34 patients, a SPINK1 mutation (30 with N34S, 4 with others). SPINK1 mutations were predominantly found in patients without a family history (29/121). Ten patients were homozygous for N34S, SPINK1 mutations were most common in 'idiopathic' CP, whereas patients with 'hereditary' CP predominantly showed a PRSS1 mutation (R122H, N29I). In patients without a family history, the most common PRSS1 mutation was A16V (7/121). In conclusion, our data suggest that CP may be inherited in a dominant, recessive or multigenetic manner as a result of mutations in the above-mentioned or as yet unidentified genes. This challenges the concept of idiopathic CP as a nongenetic disorder and the differentiation between hereditary and idiopathic CP. Therefore, we propose to classify CP as either 'primary CP' (with or without a family history) or 'secondary CP' caused by toxic, metabolic or other factors.

Published

2001

29. Mutations in the gene encoding the serine protease inhibitor, Kazal type 1 are associated with chronic pancreatitis.

Author

Witt H, Luck W, Hennies HC, Classen M, Kage A, Lass U, Landt O, and Becker M

Subjects

Adolescent, Child, Chromosomes, Human, Pair 5 genetics, Chronic Disease, DNA Mutational Analysis, Exons genetics, Female, Genotype, Haplotypes genetics, Humans, Introns genetics, Linkage Disequilibrium genetics, Lod Score, Male, Models, Biological, Mutation, Missense genetics, Polymorphism, Genetic genetics, Mutation genetics, Pancreatitis genetics, Trypsin Inhibitor, Kazal Pancreatic genetics

Abstract

Chronic pancreatitis (CP) is a continuing or relapsing inflammatory disease of the pancreas. In approximately one-third of all cases, no aetiological factor can be found, and these patients are classified as having idiopathic disease. Pathophysiologically, autodigestion and inflammation may be caused by either increased proteolytic activity or decreased protease inhibition. Several studies have demonstrated mutations in the cationic trypsinogen gene (PRSS1) in patients with hereditary or idiopathic CP. It is thought that these mutations result in increased trypsin activity within the pancreatic parenchyma. Most patients with idiopathic or hereditary CP, however, do not have mutations in PRSS1 (ref. 4). Here we analysed 96 unrelated children and adolescents with CP for mutations in the gene encoding the serine protease inhibitor, Kazal type 1 (SPINK1), a pancreatic trypsin inhibitor. We found mutations in 23% of the patients. In 18 patients, 6 of whom were homozygous, we detected a missense mutation of codon 34 (N34S). We also found four other sequence variants. Our results indicate that mutations in SPINK1 are associated with chronic pancreatitis.

Published

2000

30. A signal peptide cleavage site mutation in the cationic trypsinogen gene is strongly associated with chronic pancreatitis.

Author

Witt H, Luck W, and Becker M

Subjects

Adolescent, Amino Acid Sequence genetics, Cations, Child, Child, Preschool, Chronic Disease, Female, Humans, Infant, Male, Molecular Sequence Data, Polymerase Chain Reaction, Polymorphism, Single-Stranded Conformational, Mutation physiology, Pancreatitis genetics, Protein Sorting Signals genetics, Trypsinogen genetics

Abstract

Background & Aims: In pancreatitis, a key role has been attributed to the inappropriate conversion of trypsinogen to trypsin. Recently, two mutations of the cationic trypsinogen gene were found in families with hereditary pancreatitis. This study was conducted to determine the spectrum and frequency of cationic trypsinogen mutations in unrelated patients with idiopathic or hereditary chronic pancreatitis (CP)., Methods: DNA samples from 44 unrelated children and adolescents with CP (30 patients with idiopathic CP and 14 with hereditary CP) and from 56 family members were investigated. The cationic trypsinogen gene was screened for mutations by single-strand conformation polymorphism analysis and DNA sequencing., Results: A mutation in the cationic trypsinogen gene was detected in 5 patients: in 2 patients with a family history of CP and in 3 patients with idiopathic CP. In 1 patient the formerly described R122H mutation was detected. In 4 patients a hitherto unknown mutation was found at the signal peptide cleavage site leading to an alanine to valine exchange in codon 16. The mutations were inherited in all cases. In 95 unrelated control individuals the A16V mutation was not found., Conclusions: Heterozygosity for the A16V mutation is strongly associated with CP. These results indicate that a significant percentage of patients with idiopathic CP may have a genetic basis for their disorder; therefore, genetic testing should be included in the diagnostic evaluation of these patients.

Published

1999

31. Pathogenese der chronischen Pankreatitis

Author

Witt, H.

Published

2014

32. United European Gastroenterology evidence-based guidelines for the diagnosis and therapy of chronic pancreatitis (HaPanEU)

Author

Lohr, J. M., Dominguez-Munoz, E., Rosendahl, J., Besselink, M., Mayerle, J., Lerch, M. M., Haas, S., Akisik, F., Kartalis, N., Iglesias-Garcia, J., Keller, J., Boermeester, M., Werner, J., Dumonceau, J. -M., Fockens, P., Drewes, A., Ceyhan, G., Lindkvist, B., Drenth, J., Ewald, N., Hardt, P., Madaria, E., Witt, H., Schneider, A., Manfredi, Riccardo, Brondum, F. J., Rudolf, S., Bollen, T., Bruno, M., Dimcevski, G., Giovannini, M., Pukitis, A., Petrone, M., Oppong, K., Ammori, B., Izbiki, J. R., Ganeh, P., Salvia, R., Sauvanet, A., Barbu, S., Lyadov, V., Gubergrits, N., Okhlobystiy, A. V., Arvanitakis, M., Costamagna, Guido, Pap, A., Andersson, R., Hauge, T., Mckay, C., Regner, S., Dite, P., Olesen, S., Duggan, S., Hopper, A., Phillips, M., Shvets, O., Vujasinovic, M., Czako, L., Piemonti, L., Kocher, H., Rebours, V., Stimac, D., Hegyi, P., Gheorghe, C., Lindgren, F., Boraschi, P., Friess, H., Deprez, P., and Gastroenterology & Hepatology

Subjects

endoscopic therapy, Chronic pancreatitis, Development and Evaluation, Grading of Recommendations Assessment, diabetes mellitus, evidence-based, guidelines, pancreatic exocrine insufficiency, medicine.medical_specialty, Evidence-based practice, macromolecular substances, Review, Review Article, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Diabetes mellitus, Journal Article, Medicine, Settore MED/36 - DIAGNOSTICA PER IMMAGINI E RADIOTERAPIA, business.industry, Pancreatic exocrine insufficiency, medicine.disease, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], Oncology, 030220 oncology & carcinogenesis, Pancreatitis, 030211 gastroenterology & hepatology, Develompent and Evaluation, business

Abstract

Contains fulltext : 169869.pdf (Publisher’s version ) (Open Access) BACKGROUND: There have been substantial improvements in the management of chronic pancreatitis, leading to the publication of several national guidelines during recent years. In collaboration with United European Gastroenterology, the working group on 'Harmonizing diagnosis and treatment of chronic pancreatitis across Europe' (HaPanEU) developed these European guidelines using an evidence-based approach. METHODS: Twelve multidisciplinary review groups performed systematic literature reviews to answer 101 predefined clinical questions. Recommendations were graded using the Grading of Recommendations Assessment, Development and Evaluation system and the answers were assessed by the entire group in a Delphi process online. The review groups presented their recommendations during the 2015 annual meeting of United European Gastroenterology. At this one-day, interactive conference, relevant remarks were voiced and overall agreement on each recommendation was quantified using plenary voting (Test and Evaluation Directorate). After a final round of adjustments based on these comments, a draft version was sent out to external reviewers. RESULTS: The 101 recommendations covered 12 topics related to the clinical management of chronic pancreatitis: aetiology (working party (WP)1), diagnosis of chronic pancreatitis with imaging (WP2 and WP3), diagnosis of pancreatic exocrine insufficiency (WP4), surgery in chronic pancreatitis (WP5), medical therapy (WP6), endoscopic therapy (WP7), treatment of pancreatic pseudocysts (WP8), pancreatic pain (WP9), nutrition and malnutrition (WP10), diabetes mellitus (WP11) and the natural course of the disease and quality of life (WP12). Using the Grading of Recommendations Assessment, Development and Evaluation system, 70 of the 101 (70%) recommendations were rated as 'strong' and plenary voting revealed 'strong agreement' for 99 (98%) recommendations. CONCLUSIONS: The 2016 HaPanEU/United European Gastroenterology guidelines provide evidence-based recommendations concerning key aspects of the medical and surgical management of chronic pancreatitis based on current available evidence. These recommendations should serve as a reference standard for existing management of the disease and as a guide for future clinical research.

Published

2017

33. α1-Antitrypsin Genotypes in Patients with Chronic Pancreatitis.

Author

Witt, H., Kage, A., Luck, W., and Becker, M.

Subjects

ALPHA 1-antitrypsin, PANCREATITIS

Abstract

Background: An association between α1-antitrypsin deficiency and chronic pancreatitis (CP) has been reported in several case reports and two systematic studies. However, conflicting results have been shown in other studies of patients with CP. All previous studies were performed by phenotyping or by measurement of serum concentrations of α1-antitrypsin. The aim of this study was to investigate the relationship between α1-antitrypsin deficiency and CP by genetic analysis. Methods: Ninety-six unrelated children and adolescents with idiopathic or hereditary CP and 185 healthy controls were enrolled. DNA was extracted from peripheral blood leukocytes and the exons 5 and 7 of the α1-antitrypsin gene were amplified by polymerase chain reaction using mutagenic forward primers introducing a Taq I restriction site. Genotyping of the S allele and the Z allele was performed by restriction fragment length polymorphism analysis using Taq I. Results: Seven out of 96 patients (7.3%) with CP were heterozygous for an α1-antitrypsin deficiency allele (4 for the S allele and 3 for the Z allele). No patient was homozygous or compound heterozygous for these alleles. Twenty out of 185 control individuals (10.8%) were heterozygous for the S or Z allele (PiS: 12 controls; PiZ: 8 controls). No significant differences were found between the allele frequency in patients and the control individuals (P > 0.1). Conclusions: α1- antitrypsin deficiency is not related to the pathogenesis of idiopathic or hereditary CP. [ABSTRACT FROM AUTHOR]

Published

2002

34. SPINK 1/PSTI mutations are associated with acute and chronic pancreatitis.

Author

O'Reilly, A.D., Witt, H., Sargen, K., Kage, A., Cartmell, M.T., Becker, M., and Kingsnorth, A.N.

Subjects

*GENETIC mutation, *PANCREATITIS, *PROTEASE inhibitors, *TRYPSIN inhibitors, *PATHOLOGY

Abstract

Aims: Recent genetic research has focussed attention upon the role of the protease/protease inhibitor system in the pathogenesis of pancreatitis. This study investigates the prevalence of the recently described N34S mutation, within the trypsin inhibitor gene, SPINK 1/PSTI, in acute and chronic pancreatitis. Methods: One hundred and thirty-five patients with acute pancreatitis, 66 with chronic pancreatitis, 214 ethnically matched controls (including 71 alcoholic controls) were genotyped for the presence of the N34S mutation, by polymerase chain reaction and melting curve analysis. Results: The presence of the SPINK 1/PSTI mutation was detected in 5/135 patients with acute pancreatitis (P = 0.008); 3/77 patients with acute gallstone pancreatitis and 2/34 patients with acute idiopathic pancreatitis (P = 0.017 and P = 0.017, respectively), with respect to controls. It was also detected in 4/66 patients with chronic pancreatitis (P = 0.002); 3/47 with alcoholic CP (P = 0.005) and 1/16 with idiopathic chronic pancreatitis but was not detected among any of the 214 ethnically matched controls. Conclusions: This study describes the association of the N34S mutation of the SPINK 1/PSTI gene with acute and chronic pancreatitis. These findings support the importance of premature protease activation in the pathogenesis of pancreatitis and suggest that a genetic alteration to the trypsin inhibitor, SPINK 1/PSTI, may predispose certain individuals to develop this condition. [ABSTRACT FROM AUTHOR]

Published

2001

35. Analysis of GPRC6A variants in different pancreatitis etiologies

Author

Markus M. Lerch, Emmanuelle Masson, Joost P.H. Drenth, Peter Bugert, Jian-Min Chen, Wen Bin Zou, Marko Damm, Matthias Sendler, Jonas Rosendahl, Heidi Griesmann, Holger Kirsten, Claudia Ruffert, Ewa Małecka-Panas, Markus Scholz, Nico Hesselbarth, Tom Kaune, Rene H. M. te Morsche, Péter Hegyi, Stanisław Głuszek, Zhuan Liao, Julian Cardinal von Widdern, Heiko Witt, Raffaella Alessia Zuppardo, Robert Grützmann, Louis Buscail, Sebastian Krug, Shun Jiang Deng, Frank Ulrich Weiss, Vinciane Rebours, Giulia Martina Cavestro, Claude Férec, Adrian Saftoiu, Patrick Michl, Kaune, T., Ruffert, C., Hesselbarth, N., Damm, M., Krug, S., Cardinal von Widdern, J., Masson, E., Chen, J. -M., Rebours, V., Buscail, L., Ferec, C., Grutzmann, R., te Morsche, R. H. M., Drenth, J. P., Cavestro, G. M., Zuppardo, R. A., Saftoiu, A., Malecka-Panas, E., Gluszek, S., Bugert, P., Lerch, M. M., Sendler, M., Weiss, F. U., Zou, W. -B., Deng, S. -J., Liao, Z., Scholz, M., Kirsten, H., Hegyi, P., Witt, H., Michl, P., Griesmann, H., and Rosendahl, J.

Subjects

Adult, Male, Candidate gene, Pancreatitis, Alcoholic, Endocrinology, Diabetes and Metabolism, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, White People, Receptors, G-Protein-Coupled, 03 medical and health sciences, 0302 clinical medicine, Asian People, Risk Factors, Genetics, Humans, Medicine, SNP, Genetic Predisposition to Disease, Aged, Inflammation, Hepatology, G-Protein coupled receptor, business.industry, Gastroenterology, Genetic Variation, Inflammasome, DNA, Odds ratio, Middle Aged, Tag SNP, medicine.disease, Europe, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], Pancreatitis, 030220 oncology & carcinogenesis, Cohort, Immunology, Female, Calcium, 030211 gastroenterology & hepatology, business, Receptors, Calcium-Sensing, Genome-Wide Association Study, Signal Transduction, medicine.drug

Abstract

Contains fulltext : 229360.pdf (Publisher’s version ) (Closed access) BACKGROUND: The G-protein-coupled receptor Class C Group 6 Member A (GPRC6A) is activated by multiple ligands and is important for the regulation of calcium homeostasis. Extracellular calcium is capable to increase NLRP3 inflammasome activity of the innate immune system and deletion of this proinflammatory pathway mitigated pancreatitis severity in vivo. As such this pathway and the GPRC6A receptor is a reasonable candidate gene for pancreatitis. Here we investigated the prevalence of sequence variants in the GPRC6A locus in different pancreatitis aetiologies. METHODS: We selected 6 tagging SNPs with the SNPinfo LD TAG SNP Selection tool and the functional relevant SNP rs6907580 for genotyping. Cohorts from Germany, further European countries and China with up to 1,124 patients and 1,999 controls were screened for single SNPs with melting curve analysis. RESULTS: We identified an association of rs1606365(G) with alcoholic chronic pancreatitis in a German (odds ratio (OR) 0.76, 95% confidence interval (CI) 0.65-0.89, p = 8 × 10(-5)) and a Chinese cohort (OR 0.78, 95% CI 0.64-0.96, p = 0.02). However, this association was not replicated in a combined cohort of European patients (OR 1.18, 95% CI 0.99-1.41, p = 0.07). Finally, no association was found with acute and non-alcoholic chronic pancreatitis. CONCLUSIONS: Our results support a potential role of calcium sensing receptors and inflammasome activation in alcoholic chronic pancreatitis development. As the functional consequence of the associated variant is unclear, further investigations might elucidate the relevant mechanisms.

Published

2020

36. Polymorphisms at PRSS1-PRSS2 and CLDN2-MORC4 loci associate with alcoholic and non-alcoholic chronic pancreatitis in a European replication study

Author

Emmanuelle MASSON, Julia Mayerle, Michael Stumvoll, Sevastita Iordache, Matthias Löhr, Frank Ulrich Weiss, Jochen Hampe, Josefina Mora Brugués, Peter Kovacs, Jian-Min Chen, Anita Gasiorowska, Milena Di Leo, Giulia Martina Cavestro, DAVIDE MARTORANA, Stephen Pereira, Halina Cichoż-Lach, Markus M. Lerch, Ewa Malecka-Wojciesko, Hana Algül, Francisco X Real, Adrian Saftoiu, Derikx, M H, Kovacs, P, Scholz, M, Masson, E, Chen, J M, Ruffert, C, Lichtner, P, Te Morsche, Rhm, Cavestro, G, PanEuropean Working group on Alcoholic ChronicPancreatitis members and, Collaborator, Ferec, C, Drenth, Jph, Witt, H, and Rosendahl, J

Subjects

Genetics, ddc:610, Hereditary pancreatitis, education.field_of_study, medicine.medical_specialty, Trypsinogen, business.industry, Population, Alcohol dependence, 610 Medizin, Gastroenterology, Single-nucleotide polymorphism, Locus (genetics), medicine.disease, ddc, chemistry.chemical_compound, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], chemistry, Internal medicine, Cohort, medicine, Pancreatitis, education, business

Abstract

Objective Several genetic risk factors have been identified for non-alcoholic chronic pancreatitis (NACP). A genome-wide association study reported an association of chronic pancreatitis (CP) with variants in PRSS1 – PRSS2 ( rs10273639 ; near the gene encoding cationic trypsinogen) and CLDN2 – MORC4 loci ( rs7057398 in RIPPLY1 and rs12688220 in MORC4 ). We aimed to refine these findings in a large European cohort. Design We studied 3062 patients with alcohol-related CP (ACP) or NACP and 5107 controls. Also, 1559 German patients with alcohol-associated cirrhosis or alcohol dependence were included for comparison. We performed several meta-analyses to examine genotype–phenotype relationships. Results Association with ACP was found for rs10273639 (OR, 0.63; 95% CI 0.55 to 0.72). ACP was also associated with variants rs7057398 and rs12688220 in men (OR, 2.26; 95% CI 1.94 to 2.63 and OR, 2.66; 95% CI 2.21 to 3.21, respectively) and in women (OR, 1.57; 95% CI 1.14 to 2.18 and OR 1.71; 95% CI 1.41 to 2.07, respectively). Similar results were obtained when German patients with ACP were compared with those with alcohol-associated cirrhosis or alcohol dependence. In the overall population of patients with NACP, association with rs10273639 was absent (OR, 0.93; 95% CI 0.79 to 1.01), whereas rs7057398 of the X chromosomal single nucleotide polymorphisms was associated with NACP in women only (OR, 1.32; 95% CI 1.15 to 1.51). Conclusions The single-nucleotide polymorphisms rs10273639 at the PRSS1–PRSS2 locus and rs7057398 and rs12688220 at the CLDN2 – MORC4 locus are associated with CP and strongly associate with ACP, but only rs7057398 with NACP in female patients.

Published

2015

37. A degradation-sensitive anionic trypsinogen (PRSS2) variant protects against chronic pancreatitis

Author

Heiko, Witt, Miklos Sahin Toth, Olfert, Landt, Jian Min Chen, Thilo, Kahne, Drenth, Joost P. H., Zoltan, Kukor, Edit, Szepessy, Walter, Halangk, Stefan, Dahm, Klaus, Rohde, Hans Ulrich Schulz, Cedric Le Marechal, Nejat, Akar, Ammann, Rudolf W., Kaspar, Truninger, Mario, Bargetzi, Eesh, Bhatia, Carlo, Castellani, Giulia Martina Cavestro, Milos, Cerny, DESTRO-BISOL, Giovanni, Spedini, Gabriella, Hans, Eiberg, Jansen, Jan B. M. J., Monika, Koudova, Eva, Rausova, Milan, Macek, Macek Jr, M., Nuria, Malats, Real, Francisco X., Hans Jurgen Menzel, Pedro, Moral, Roberta, Galavotti, Pier Franco Pignatti, Olga, Rickards, Julius, Spicak, Narcis Octavian Zarnescu, Wolfgang, Bock, Gress, Thomas M., Helmut, Friess, Johann, Ockenga, Hartmut, Schmidt, Roland, Pfutzer, Matthias, Lohr, Peter, Simon, Frank Ulrich Weiss, Lerch, Markus M., Niels, Teich, Volker, Keim, Thomas, Berg, Bertram, Wiedenmann, Werner, Luck, David Alexander Groneberg, Michael, Becker, Thomas, Keil, Andreas, Kage, Jana, Bernardova, Markus, Braun, Claudia, Guldner, Juliane, Halangk, Jonas, Rosendahl, Ulrike, Witt, Matthias, Treiber, Renate, Nickel, Claude, Ferec, Witt, H, SAHIN TOTH, M, Landt, O, Chen, Jm, Kahne, T, Drenth, Jp, Kukor, Z, Szepessy, E, Halangk, W, Dahm, S, Rohde, K, Schulz, Hu, LE MARECHAL, C, Akar, N, Ammann, Rw, Truninger, K, Bargetzi, M, Bhatia, E, Castellani, C, Cavestro, GIULIA MARTINA, Cerny, M, DESTRO BISOL, G, Spedini, G, Eiberg, H, Jansen, Jb, Koudova, M, Rausova, E, MACEK M., Jr, Malats, N, Real, Fx, Menzel, Hj, Moral, P, Galavotti, R, Pignatti, Pf, Rickards, O, Spicak, J, Zarnescu, No, Bock, W, Gress, Tm, Friess, H, Ockenga, J, Schmidt, H, Pfutzer, R, Lohr, M, Simon, P, Weiss, Fu, Lerch, Mm, Teich, N, Keim, V, Berg, T, Wiedenmann, B, Luck, W, Groneberg, Da, Becker, M, Keil, T, Kage, A, Bernardova, J, Braun, M, Guldner, C, Halangk, J, Rosendahl, J, Witt, U, Treiber, M, Nickel, R, and Ferec, C.

Subjects

trypsin inhibitor, Models, Molecular, Enteropeptidase, Pancreatic disease, Membrane transport and intracellular motility [NCMLS 5], arginine, genetic risk, chemistry.chemical_compound, Models, proteinosis, Trypsin, Pancreatic Secretory Trypsin Inhibitor, PRSS1 gene, enteropeptidase, medicine.diagnostic_test, adult, Hydrolysis, cationic trypsinogen, protection, unclassified drug, enzyme activity, female, priority journal, risk factor, CHRONIC PANCREATITIS, protein degradation, Trypsinogen, medicine.drug, medicine.medical_specialty, anionic trypsinogen, Proteolysis, Biology, Article, male, Internal medicine, Genetics, medicine, Matrix-Assisted Laser Desorption-Ionization, Humans, PRSS2, controlled study, human, Molecular gastro-enterology and hepatology [IGMD 2], gene, DNA Primers, Genetic polymorphism, catalysis, Base Sequence, Spectrometry, disease predisposition, Molecular, cationic trypsinogen prss1, glycine, pancreatic secretory trypsin inhibitor spink1, trypsin, trypsinogen, article, chronic pancreatitis, codon, genetic susceptibility, major clinical study, nucleotide sequence, Chronic Disease, Haplotypes, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Mass, medicine.disease, Tripsinogen, Tripsina, Settore BIO/18 - Genetica, Endocrinology, Genetic defects of metabolism [UMCN 5.1], Pancreatitis, chemistry, Genètica

Abstract

Chronic pancreatitis is a common inflammatory disease of the pancreas. Mutations in the genes encoding cationic trypsinogen (PRSS1) and the pancreatic secretory trypsin inhibitor (SPINK1) are associated with chronic pancreatitis. Because increased proteolytic activity owing to mutated PRSS1 enhances the risk for chronic pancreatitis, mutations in the gene encoding anionic trypsinogen (PRSS2) may also predispose to disease. Here we analyzed PRSS2 in individuals with chronic pancreatitis and controls and found, to our surprise, that a variant of codon 191 (G191R) is overrepresented in control subjects: G191R was present in 220/6,459 (3.4%) controls but in only 32/2,466 (1.3%) affected individuals (odds ratio 0.37; P = 1.1 x 10(-8)). Upon activation by enterokinase or trypsin, purified recombinant G191R protein showed a complete loss of trypsin activity owing to the introduction of a new tryptic cleavage site that renders the enzyme hypersensitive to autocatalytic proteolysis. In conclusion, the G191R variant of PRSS2 mitigates intrapancreatic trypsin activity and thereby protects against chronic pancreatitis. The initial experiments were supported by the DFG (Wi 2036/1-1). This work was supported by the Sonnenfeld-Stiftung, Berlin, Germany (to H.W.), the US National Institutes of Health (NIH) (grant DK058088 to M.S.-T.), INSERM (Institut National de la Santé et de la Recherche Médicale) and the Programme Hospitalier de Recherche Clinique (grant PHRC R 08-04 to C.F.)

Published

2006