BACKGROUND: acute recurrent pancreatitis is a complex multigenic disease, the diagnosis is even more difficult when this disease develops in a child. CASE PRESENTATION: a 6-years old boy, hospitalized with epigastric pain radiating to the back showed high serum levels of serum amylase, lipase, CRP and erythrosedimentation rate. Several similar milder episodes of pain, followed by quick recovery and complete disappearance of symptoms were reported during the previous 13 months. The child was medically treated and after 7 days with normal clinic and laboratory tests was discharged with a hypolipidic diet. All the known aetiologic hypotheses were excluded by anamnestic investigation, clinical observation and biochemical evaluation, whereas, anatomic abnormality were excluded by a secretin stimulated magnetic resonance (MRI). At the last follow-up visit, (11 months later), the child showed a normal body weight and anthropometric profile, without further abdominal pain. Mutation screening for coding regions of PRSS1, SPINK1, CFTR and the new hereditary pancreatitis-associated chymotrypsin C (CTRC) genes showed a novel variation, c.541A > G (p.S181G), in the exon 4 of PRSS1 gene and the classical CF p.F508del mutation in the CFTR. Both mutations were present in his clinically normal mother and absent in the patient's father. CONCLUSIONS: this report extend the spectrum of PRSS1 mutations, however, the absence of family history of pancreatitis leaves the present case without the hallmark of the hereditary origin of pancreatitis. At the present knowledge it can be only stated that the combined genotype CFTR (F508del)/PRSS1 (S181G) is associated to a mild phenotype of acute recurrent pancreatitis in this child without any further conclusion on its pathogenetic role or prediction on the course of the disease.
BACKGROUND: acute recurrent pancreatitis is a complex multigenic disease, the diagnosis is even more difficult when this disease develops in a child. CASE PRESENTATION: a 6-years old boy, hospitalized with epigastric pain radiating to the back showed high serum levels of serum amylase, lipase, CRP and erythrosedimentation rate. Several similar milder episodes of pain, followed by quick recovery and complete disappearance of symptoms were reported during the previous 13 months. The child was medically treated and after 7 days with normal clinic and laboratory tests was discharged with a hypolipidic diet. All the known aetiologic hypotheses were excluded by anamnestic investigation, clinical observation and biochemical evaluation, whereas, anatomic abnormality were excluded by a secretin stimulated magnetic resonance (MRI). At the last follow-up visit, (11 months later), the child showed a normal body weight and anthropometric profile, without further abdominal pain. Mutation screening for coding regions of PRSS1, SPINK1, CFTR and the new hereditary pancreatitis-associated chymotrypsin C (CTRC) genes showed a novel variation, c.541A > G (p.S181G), in the exon 4 of PRSS1 gene and the classical CF p.F508del mutation in the CFTR. Both mutations were present in his clinically normal mother and absent in the patient's father. CONCLUSIONS: this report extend the spectrum of PRSS1 mutations, however, the absence of family history of pancreatitis leaves the present case without the hallmark of the hereditary origin of pancreatitis. At the present knowledge it can be only stated that the combined genotype CFTR (F508del)/PRSS1 (S181G) is associated to a mild phenotype of acute recurrent pancreatitis in this child without any further conclusion on its pathogenetic role or prediction on the course of the disease.
Authors: D C Whitcomb; M C Gorry; R A Preston; W Furey; M J Sossenheimer; C D Ulrich; S P Martin; L K Gates; S T Amann; P P Toskes; R Liddle; K McGrath; G Uomo; J C Post; G D Ehrlich Journal: Nat Genet Date: 1996-10 Impact factor: 38.330
Authors: D C Whitcomb; R A Preston; C E Aston; M J Sossenheimer; P S Barua; Y Zhang; A Wong-Chong; G J White; P G Wood; L K Gates; C Ulrich; S P Martin; J C Post; G D Ehrlich Journal: Gastroenterology Date: 1996-06 Impact factor: 22.682
Authors: Heiko Witt; Miklós Sahin-Tóth; Olfert Landt; Jian-Min Chen; Thilo Kähne; Joost Ph Drenth; Zoltán Kukor; Edit Szepessy; Walter Halangk; Stefan Dahm; Klaus Rohde; Hans-Ulrich Schulz; Cédric Le Maréchal; Nejat Akar; Rudolf W Ammann; Kaspar Truninger; Mario Bargetzi; Eesh Bhatia; Carlo Castellani; Giulia Martina Cavestro; Milos Cerny; Giovanni Destro-Bisol; Gabriella Spedini; Hans Eiberg; Jan B M J Jansen; Monika Koudova; Eva Rausova; Milan Macek; Núria Malats; Francisco X Real; Hans-Jürgen Menzel; Pedro Moral; Roberta Galavotti; Pier Franco Pignatti; Olga Rickards; Julius Spicak; Narcis Octavian Zarnescu; Wolfgang Böck; Thomas M Gress; Helmut Friess; Johann Ockenga; Hartmut Schmidt; Roland Pfützer; Matthias Löhr; Peter Simon; Frank Ulrich Weiss; Markus M Lerch; Niels Teich; Volker Keim; Thomas Berg; Bertram Wiedenmann; Werner Luck; David Alexander Groneberg; Michael Becker; Thomas Keil; Andreas Kage; Jana Bernardova; Markus Braun; Claudia Güldner; Juliane Halangk; Jonas Rosendahl; Ulrike Witt; Matthias Treiber; Renate Nickel; Claude Férec Journal: Nat Genet Date: 2006-05-14 Impact factor: 38.330
Authors: Maria Rosaria D'Apice; Stefano Gambardella; Mario Bengala; Silvia Russo; Anna Maria Nardone; Vincenzina Lucidi; Federica Sangiuolo; Giuseppe Novelli Journal: BMC Med Genet Date: 2004-04-14 Impact factor: 2.103