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The Relationship of Anatomic Variation of Pancreatic Ductal System and Pancreaticobiliary Diseases

The aims of this study were to identify the morphological diversities and anatomical variations of pancreatic ductal system and to define the relationships between pancreatic ductal systems, pancreaticobiliary diseases, and procedure-related complications, including post-ERCP pancreatitis. This stud...

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Autores principales: Bang, Seungmin, Suh, Jung Hoon, Park, Byung Kyu, Park, Seung Woo, Song, Si Young, Chung, Jae Bock
Formato: Texto
Lenguaje:English
Publicado: Yonsei University College of Medicine 2006
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2687635/
https://www.ncbi.nlm.nih.gov/pubmed/16642555
http://dx.doi.org/10.3349/ymj.2006.47.2.243
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author Bang, Seungmin
Suh, Jung Hoon
Park, Byung Kyu
Park, Seung Woo
Song, Si Young
Chung, Jae Bock
author_facet Bang, Seungmin
Suh, Jung Hoon
Park, Byung Kyu
Park, Seung Woo
Song, Si Young
Chung, Jae Bock
author_sort Bang, Seungmin
collection PubMed
description The aims of this study were to identify the morphological diversities and anatomical variations of pancreatic ductal system and to define the relationships between pancreatic ductal systems, pancreaticobiliary diseases, and procedure-related complications, including post-ERCP pancreatitis. This study included 582 patients in whom both pancreatic duct (PD) and common bile duct were clearly visible by ERCP. PD systems were categorized into four types according to the relationship between common bile duct and PD. In types A and B, Wirsung duct formed the main PD. In type C, Wirsung duct did not form the main PD. If PD system did not fall into any of these three types, it was categorized as type D. The distribution of types among pancreatic ducts examined was as follows: type A: 491 cases (84.4%), type B: 56 cases (9.6%), type C: 20 cases (3.4%), and type D: 15 cases (2.6%). The anomalous anatomic variations of PD systems were divided into migration, fusion, and duplication anomalies. PD anomalies were noted in 51 patients, of which 19 (3.3%) were fusion anomalies (12 complete pancreas divisum, 7 incomplete pancreas divisum), and 32 (5.5%) were duplication anomalies (5 number variations, 27 form variations). No significant relationships between various PD morphologies and pancreaticobiliary diseases were found. However, post-ERCP hyperamylasemia was more frequently found in types C (41.7%), D (50%) and A (19.8%) than in type B (9.4%). In summary, whether Wirsung duct forms the main PD and the presence or absence of the opening of the Santorini duct are both important factors in determining the development of pancreatitis and hyperamylasemia after ERCP.
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spelling pubmed-26876352009-06-04 The Relationship of Anatomic Variation of Pancreatic Ductal System and Pancreaticobiliary Diseases Bang, Seungmin Suh, Jung Hoon Park, Byung Kyu Park, Seung Woo Song, Si Young Chung, Jae Bock Yonsei Med J Original Article The aims of this study were to identify the morphological diversities and anatomical variations of pancreatic ductal system and to define the relationships between pancreatic ductal systems, pancreaticobiliary diseases, and procedure-related complications, including post-ERCP pancreatitis. This study included 582 patients in whom both pancreatic duct (PD) and common bile duct were clearly visible by ERCP. PD systems were categorized into four types according to the relationship between common bile duct and PD. In types A and B, Wirsung duct formed the main PD. In type C, Wirsung duct did not form the main PD. If PD system did not fall into any of these three types, it was categorized as type D. The distribution of types among pancreatic ducts examined was as follows: type A: 491 cases (84.4%), type B: 56 cases (9.6%), type C: 20 cases (3.4%), and type D: 15 cases (2.6%). The anomalous anatomic variations of PD systems were divided into migration, fusion, and duplication anomalies. PD anomalies were noted in 51 patients, of which 19 (3.3%) were fusion anomalies (12 complete pancreas divisum, 7 incomplete pancreas divisum), and 32 (5.5%) were duplication anomalies (5 number variations, 27 form variations). No significant relationships between various PD morphologies and pancreaticobiliary diseases were found. However, post-ERCP hyperamylasemia was more frequently found in types C (41.7%), D (50%) and A (19.8%) than in type B (9.4%). In summary, whether Wirsung duct forms the main PD and the presence or absence of the opening of the Santorini duct are both important factors in determining the development of pancreatitis and hyperamylasemia after ERCP. Yonsei University College of Medicine 2006-04-30 2006-04-30 /pmc/articles/PMC2687635/ /pubmed/16642555 http://dx.doi.org/10.3349/ymj.2006.47.2.243 Text en Copyright © 2006 The Yonsei University College of Medicine http://creativecommons.org/licenses/by-nc/3.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0) which permits unrestricted noncommercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Article
Bang, Seungmin
Suh, Jung Hoon
Park, Byung Kyu
Park, Seung Woo
Song, Si Young
Chung, Jae Bock
The Relationship of Anatomic Variation of Pancreatic Ductal System and Pancreaticobiliary Diseases
title The Relationship of Anatomic Variation of Pancreatic Ductal System and Pancreaticobiliary Diseases
title_full The Relationship of Anatomic Variation of Pancreatic Ductal System and Pancreaticobiliary Diseases
title_fullStr The Relationship of Anatomic Variation of Pancreatic Ductal System and Pancreaticobiliary Diseases
title_full_unstemmed The Relationship of Anatomic Variation of Pancreatic Ductal System and Pancreaticobiliary Diseases
title_short The Relationship of Anatomic Variation of Pancreatic Ductal System and Pancreaticobiliary Diseases
title_sort relationship of anatomic variation of pancreatic ductal system and pancreaticobiliary diseases
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2687635/
https://www.ncbi.nlm.nih.gov/pubmed/16642555
http://dx.doi.org/10.3349/ymj.2006.47.2.243
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