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Name of Journal: World Journal of Gastrointestinal OncologyManuscript NO: 43026Manuscript?Type: ORIGINAL ARTICLE Observational StudyRisk of cholangiocarcinoma in patients undergoing therapeutic endoscopic retrograde cholangiopancreatography or cholecystectomy: A population based studyWang CC et al. Risk of cholangiocarcinoma in patients undergoing therapeutic bile duct managementChi-Chih Wang, Ming-Chang Tsai, Wen-Wei Sung, Tzu-Wei Yang, Hsuan-Yi Chen, Yao-Tung Wang, Chang-Cheng Su, Ming-Hseng Tseng, Chun-Che LinChi-Chih Wang, Ming-Chang Tsai, Wen-Wei Sung, Yao-Tung Wang, Chun-Che Lin, Institute of Medicine, Chung Shan Medical University, Taichung 40201, TaiwanChi-Chih Wang, Ming-Chang Tsai, Wen-Wei Sung, Tzu-Wei Yang, Hsuan-Yi Chen, Yao-Tung Wang, Chun-Che Lin, School of Medicine, Chung Shan Medical University, Taichung 40201, TaiwanChi-Chih Wang, Ming-Chang Tsai, Tzu-Wei Yang, Hsuan-Yi Chen, Chang-Cheng Su, Chun-Che Lin, Division of Gastroenterology and Hepatology, Department of Internal Medicine, Chung Shan Medical University Hospital, Taichung 40201, TaiwanWen-Wei Sung, Department of Urology, Chung Shan Medical University Hospital, Taichung 40201, TaiwanTzu-Wei Yang, Institute and Department of Biological Science and Technology, National Chiao Tung University, Hsinchu 30010, TaiwanYao-Tung Wang, Division of Pulmonary Medicine, Department of Internal Medicine, Chung Shan Medical University Hospital, Taichung 40201, TaiwanMing-Hseng Tseng, Department of Medical Informatics, Chung Shan Medical University, Taichung 40201, TaiwanMing-Hseng Tseng, Information Technology Office, Chung Shan Medical University Hospital, Taichung 40201, TaiwanORCID?number: Chi-Chih Wang (0000-0002-8222-0503); Ming-Chang Tsai (0000-0002-7687-2329); Wen-Wei Sung (0000-0002-2375-0029); Tzu-Wei Yang (0000-0002-1522-8177); Hsuan-Yi Chen (0000-0003-1001-7968); Yao-Tung Wang (0000-0002-0300-0896); Chang-Cheng Su (0000-0002-7211-4192); Ming-Hseng Tseng (0000-0001-8868-1610); Chun-Che Lin (0000-0002-2474-6734).Author contributions: Tseng MH and Lin CC contributed equally to this manuscript; Wang CC, Tseng MH and Sung WW contributed to conception and design; Tseng MH contributed to acquisition of data; Tsai MC, Wang CC, Wang YT and Chen HY contributed to analysis and interpretation of data; Wang CC, Yang TW and Chen HY contributed to drafting of the manuscript; Yang TW, Sung WW and Lin CC contributed to critical revision of the manuscript; Tsai MC, Sung WW and Su CC contributed to statistical analysis; Tseng MH and Lin CC contributed to supervision. Supported by Chung Shan Medical University Hospital research program, Taichung, Taiwan, No. CSH- 2013-C-032.Institutional review board statement: This study was approved by the Institutional Review Board of Chung Shan Medical University Hospital, rmed consent statement: The Institutional Review Board waved the need of informed consent in this study as it is a retrospective study based on the National Health Insurance Research Database.Conflict-of-interest statement: None.STROBE statement: The authors have read the STROBE Statement-checklist of items, and the manuscript was prepared and revised according to the STROBE Statement-checklist of items.Open-Access: This article is an open-access article which was selected by an in-house editor and fully peer-reviewed by external reviewers. It is distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited and the use is non-commercial. See: author: Chun-Che Lin, MD, PhD, Attending Doctor, Chief Doctor, Doctor, Professor, Division of Gastroenterology and Hepatology, Department of Internal Medicine, Chung Shan Medical University Hospital, No.110, Sec.1, Jianguo N.Rd., Taichung 40201, Taiwan. cshy333@.twTelephone: +886-424730022-11603Fax: +886-423248130Received: October 25, 2018 Peer-review started: October 25, 2018 First decision: December 10, 2018 Revised: January 16, 2019 Accepted: January 29, 2019 Article in press: Published online: AbstractBACKGROUNDCholangiocarcinoma is a highly lethal disease that had been underestimated in the past two decades. Many risk factors are well documented for in cholangiocarcinoma, but the impacts of advanced biliary interventions, like endoscopic sphincterotomy (ES), endoscopic papillary balloon dilatation (EPBD), and cholecystectomy, are inconsistent in the previous literature. AIMTo clarify the risks of cholangiocarcinoma after ES/EPBD, cholecystectomy or no intervention for cholelithiasis using the National Health Insurance Research Database (NHIRD).METHODSFrom data of NHIRD 2004-2011 in Taiwan, we selected 7938 cholelithiasis cases as well as 23814 control group cases (matched by sex and age in a 1:3 ratio). We compared the previous risk factors of cholangiocarcinoma and cholangiocarcinoma rate in the cholelithiasis and control groups. The incidences of total and subsequent cholangiocarcinoma were calculated in ES/EPBD patients, cholecystectomy patients, cholelithiasis patients without intervention, and groups from the normal population. RESULTSIn total, 537 cases underwent ES/EPBD, 1743 cases underwent cholecystectomy, and 5658 cholelithiasis cases had no intervention. Eleven (2.05%), 37 (0.65%), and 7 (0.40%) subsequent cholangiocarcinoma cases were diagnosed in the ES/EPBD, no intervention, and cholecystectomy groups, respectively, and the odds ratio for subsequent cholangiocarcinoma was 3.13 in the ES/EPBD group and 0.61 in the cholecystectomy group when compared with the no intervention group.CONCLUSIONIn conclusion, symptomatic cholelithiasis patients who undergo cholecystectomy can reduce the incidence of subsequent cholangiocarcinoma, while cholelithiasis patients who undergo ES/EPBD are at a great risk of subsequent cholangiocarcinoma according to our findings.Key words: Cholangiocarcinoma; Endoscopic sphincterotomy; Endoscopic papillary balloon dilatation; Cholecystectomy? The Author(s) 2019. Published by Baishideng Publishing Group Inc. All rights reserved.Core tip: There are many risk factors well demonstrated in cholangiocarcinoma, but the impacts of advanced biliary interventions, like endoscopic sphincterotomy (ES), endoscopic papillary balloon dilatation (EPBD) and cholecystectomy, are inconsistence in previous literature. We tried to evaluate the subsequent cholangiocarcinoma risk in cholelithiasis patients who underwent ES, EPBD and cholecystectomy. Cholecystectomy can reduce the incidence of subsequent cholangiocarcinoma, while cholelithiasis patients underwent ES/EPBD are in a huge risk of subsequent cholangiocarcinoma in our database study.Wang CC, Tsai MC, Sung WW, Yang TW, Chen HY, Wang YT, Su CC, Tseng MH, Lin CC. Risk of cholangiocarcinoma in patients undergoing therapeutic endoscopic retrograde cholangiopancreatography or cholecystectomy: A population based study. World J Gastrointest Oncol 2019; In pressINTRODUCTIONCholangiocarcinoma, which arises from the epithelial cells of the intrahepatic or extrahepatic bile ducts, is a highly lethal disease that has been underestimated in the past two decades. Unlike the decline in mortality due to primary liver cancer, the mortality of intra-hepatic cholangiocarcinoma (ICC) has increased in both sexes in EuropePEVuZE5vdGU+PENpdGU+PEF1dGhvcj5CZXJ0dWNjaW88L0F1dGhvcj48WWVhcj4yMDEzPC9ZZWFy

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ADDIN EN.CITE.DATA [1]. At the same time, previous studies have shown that the incidence of ICC has been rising, while the incidence of extra-hepatic cholangiocarcinoma (ECC) has declined internationallyPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5XZWx6ZWw8L0F1dGhvcj48WWVhcj4yMDA2PC9ZZWFyPjxS

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ADDIN EN.CITE.DATA [2-5] in the past thirty years, except in Denmark ADDIN EN.CITE <EndNote><Cite><Author>Jepsen</Author><Year>2007</Year><RecNum>1049</RecNum><DisplayText><style face="superscript">[6]</style></DisplayText><record><rec-number>1049</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1530416410">1049</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Jepsen, P.</author><author>Vilstrup, H.</author><author>Tarone, R. E.</author><author>Friis, S.</author><author>Sorensen, H. T.</author></authors></contributors><auth-address>Department of Clinical Epidemiology, Aarhus University Hospital, Ole Worms Alle 1150, DK-8000 Aarhus C, Denmark. pj@dce.au.dk</auth-address><titles><title>Incidence rates of intra- and extrahepatic cholangiocarcinomas in Denmark from 1978 through 2002</title><secondary-title>J Natl Cancer Inst</secondary-title></titles><periodical><full-title>J Natl Cancer Inst</full-title></periodical><pages>895-7</pages><volume>99</volume><number>11</number><keywords><keyword>Adult</keyword><keyword>Aged</keyword><keyword>Aged, 80 and over</keyword><keyword>Bile Duct Neoplasms/classification/*epidemiology</keyword><keyword>*Bile Ducts, Extrahepatic</keyword><keyword>*Bile Ducts, Intrahepatic</keyword><keyword>Cholangiocarcinoma/*epidemiology</keyword><keyword>Denmark/epidemiology</keyword><keyword>Female</keyword><keyword>Humans</keyword><keyword>Incidence</keyword><keyword>Male</keyword><keyword>Middle Aged</keyword><keyword>Time Factors</keyword></keywords><dates><year>2007</year><pub-dates><date>Jun 6</date></pub-dates></dates><isbn>1460-2105 (Electronic)&#xD;0027-8874 (Linking)</isbn><accession-num>17551150</accession-num><urls><related-urls><url>;[6]. Unfortunately, the global incidence data may be inaccurate because of ICC registered as part of primary liver cancer and ECC mixed with gallbladder cancers in the databases of many countries.The previous literature has listed many well known risk factors for cholangiocarcinoma, such as primary sclerosing cholangitisPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5CZXJncXVpc3Q8L0F1dGhvcj48WWVhcj4yMDAyPC9ZZWFy

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ADDIN EN.CITE.DATA [10,11], specific parasite infection ADDIN EN.CITE <EndNote><Cite><Author>Watanapa</Author><Year>2002</Year><RecNum>1056</RecNum><DisplayText><style face="superscript">[12]</style></DisplayText><record><rec-number>1056</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1530606604">1056</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Watanapa, P.</author><author>Watanapa, W. B.</author></authors></contributors><auth-address>Departments of Surgery and Physiology, Faculty of Medicine, Siriraj Hospital, Mahidol University, Bangkok 10 700, Thailand.</auth-address><titles><title>Liver fluke-associated cholangiocarcinoma</title><secondary-title>Br J Surg</secondary-title></titles><periodical><full-title>Br J Surg</full-title></periodical><pages>962-70</pages><volume>89</volume><number>8</number><keywords><keyword>Animals</keyword><keyword>Bile Duct Neoplasms/*parasitology/pathology/therapy</keyword><keyword>*Bile Ducts, Intrahepatic</keyword><keyword>Cholangiocarcinoma/*parasitology/pathology/therapy</keyword><keyword>Cricetinae</keyword><keyword>Diterpenes/therapeutic use</keyword><keyword>Epoxy Compounds</keyword><keyword>Humans</keyword><keyword>Liver Diseases, Parasitic/*complications</keyword><keyword>Opisthorchiasis/*complications</keyword><keyword>*Opisthorchis</keyword><keyword>*Phenanthrenes</keyword><keyword>Survival Analysis</keyword><keyword>Treatment Outcome</keyword></keywords><dates><year>2002</year><pub-dates><date>Aug</date></pub-dates></dates><isbn>0007-1323 (Print)&#xD;0007-1323 (Linking)</isbn><accession-num>12153620</accession-num><urls><related-urls><url>;[12], cholelithiasisPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5XZWx6ZWw8L0F1dGhvcj48WWVhcj4yMDA3PC9ZZWFyPjxS

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ADDIN EN.CITE.DATA [19,20]. However, the true etiology of cholangiocarcinoma is still a mystery, although several hypotheses have been proposed, including destruction of the integrity of the bile duct through procedures like therapeutic endoscopic retrograde cholangiopancreatography (ERCP) or cholecystectomy. The major indications for ERCP are choledocholithiasis, rather than biliary or pancreatic neoplasms, or the need to manage postoperative biliary complicationsPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5Db21taXR0ZWU8L0F1dGhvcj48WWVhcj4yMDEwPC9ZZWFy

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ADDIN EN.CITE.DATA [21-23]. Therapeutic ERCP, including endoscopic sphincterotomy (ES) and endoscopic papillary balloon dilatation (EPBD), has been considered to have increased future cholangiocarcinoma incidence for over a decadePEVuZE5vdGU+PENpdGU+PEF1dGhvcj5TaGV0aDwvQXV0aG9yPjxZZWFyPjIwMDI8L1llYXI+PFJl

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ADDIN EN.CITE.DATA [24-26]. Because cholelithiasis itself is one of the risk factors of cholangiocarcinoma, the impact of the incidence of a subsequent cholangiocarcinoma for advanced bile duct management is hard to evaluate.ES had been shown to increase biliary epithelial atypiaPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5LYWxhaXR6aXM8L0F1dGhvcj48WWVhcj4yMDEyPC9ZZWFy

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ADDIN EN.CITE.DATA [27], and previous data have indicated that therapeutic ERCP can increase the subsequent cholangiocarcinoma rate ADDIN EN.CITE <EndNote><Cite><Author>Oliveira-Cunha</Author><Year>2016</Year><RecNum>1066</RecNum><DisplayText><style face="superscript">[28]</style></DisplayText><record><rec-number>1066</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1530608620">1066</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Oliveira-Cunha, M.</author><author>Dennison, A. R.</author><author>Garcea, G.</author></authors></contributors><auth-address>Department of Hepatobiliary and Pancreatic Surgery, University Hospitals of Leicester, NHS Trust, Leicester, UK.</auth-address><titles><title>Late Complications After Endoscopic Sphincterotomy</title><secondary-title>Surg Laparosc Endosc Percutan Tech</secondary-title></titles><periodical><full-title>Surg Laparosc Endosc Percutan Tech</full-title></periodical><pages>1-5</pages><volume>26</volume><number>1</number><keywords><keyword>Bile Duct Neoplasms/etiology</keyword><keyword>Cholangiocarcinoma/etiology</keyword><keyword>Cholangiopancreatography, Endoscopic Retrograde/adverse effects</keyword><keyword>Cholangitis/etiology</keyword><keyword>Choledocholithiasis/*surgery</keyword><keyword>Gallstones/etiology</keyword><keyword>Humans</keyword><keyword>Postoperative Complications/etiology</keyword><keyword>Recurrence</keyword><keyword>Sphincterotomy, Endoscopic/*adverse effects</keyword></keywords><dates><year>2016</year><pub-dates><date>Feb</date></pub-dates></dates><isbn>1534-4908 (Electronic)&#xD;1530-4515 (Linking)</isbn><accession-num>26679684</accession-num><urls><related-urls><url>;[28]. At the same time, many recent larger population-based studies have demonstrated that ES does not increase the incidence of cholangiocarcinomaPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5QZW5nPC9BdXRob3I+PFllYXI+MjAxNTwvWWVhcj48UmVj

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ADDIN EN.CITE.DATA [29]. At the same time, cholelithiasis and cholecystectomy had been of concern due to the increase in ICC ADDIN EN.CITE <EndNote><Cite><Author>Guo</Author><Year>2014</Year><RecNum>1074</RecNum><DisplayText><style face="superscript">[32]</style></DisplayText><record><rec-number>1074</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1531015821">1074</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Guo, L.</author><author>Mao, J.</author><author>Li, Y.</author><author>Jiao, Z.</author><author>Guo, J.</author><author>Zhang, J.</author><author>Zhao, J.</author></authors></contributors><auth-address>Department of General Surgery, Key Laboratory of Digestive System Tumors, Lanzhou University Second Hospital, Lanzhou 730000, Gansu Province, China.</auth-address><titles><title>Cholelithiasis, cholecystectomy and risk of hepatocellular carcinoma: a meta-analysis</title><secondary-title>J Cancer Res Ther</secondary-title></titles><periodical><full-title>J Cancer Res Ther</full-title></periodical><pages>834-8</pages><volume>10</volume><number>4</number><keywords><keyword>Carcinoma, Hepatocellular/*etiology/pathology</keyword><keyword>Cholecystectomy/*adverse effects</keyword><keyword>Cholelithiasis/*complications/pathology</keyword><keyword>Humans</keyword><keyword>Liver Neoplasms/*etiology/pathology</keyword></keywords><dates><year>2014</year><pub-dates><date>Oct-Dec</date></pub-dates></dates><isbn>1998-4138 (Electronic)&#xD;1998-4138 (Linking)</isbn><accession-num>25579515</accession-num><urls><related-urls><url>;[32] and ECCPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5UYW88L0F1dGhvcj48WWVhcj4yMDEwPC9ZZWFyPjxSZWNO

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ADDIN EN.CITE.DATA [33], but some studies have shown that cholecystectomy decreases the subsequent cholangiocarcinoma rate in cholelithiasis patients ADDIN EN.CITE <EndNote><Cite><Author>Nordenstedt</Author><Year>2012</Year><RecNum>1075</RecNum><DisplayText><style face="superscript">[34]</style></DisplayText><record><rec-number>1075</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1531015939">1075</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Nordenstedt, H.</author><author>Mattsson, F.</author><author>El-Serag, H.</author><author>Lagergren, J.</author></authors></contributors><auth-address>Upper Gastrointestinal Research, Department of Molecular Medicine and Surgery, Karolinska Institutet, Stockholm, Sweden. helena.nordenstedt@ki.se</auth-address><titles><title>Gallstones and cholecystectomy in relation to risk of intra- and extrahepatic cholangiocarcinoma</title><secondary-title>Br J Cancer</secondary-title></titles><periodical><full-title>Br J Cancer</full-title></periodical><pages>1011-5</pages><volume>106</volume><number>5</number><keywords><keyword>Adult</keyword><keyword>Aged</keyword><keyword>Bile Duct Neoplasms/diagnosis/epidemiology/*etiology</keyword><keyword>*Bile Ducts, Extrahepatic</keyword><keyword>*Bile Ducts, Intrahepatic</keyword><keyword>Cholangiocarcinoma/diagnosis/epidemiology/*etiology</keyword><keyword>*Cholecystectomy</keyword><keyword>Cohort Studies</keyword><keyword>Female</keyword><keyword>Gallstones/*complications/surgery</keyword><keyword>Humans</keyword><keyword>Male</keyword><keyword>Middle Aged</keyword><keyword>Risk Factors</keyword><keyword>Sweden/epidemiology</keyword></keywords><dates><year>2012</year><pub-dates><date>Feb 28</date></pub-dates></dates><isbn>1532-1827 (Electronic)&#xD;0007-0920 (Linking)</isbn><accession-num>22240785</accession-num><urls><related-urls><url>;[34]. The inconsistency of the previous evidence led us to conduct this study using the National Health Insurance Research Database (NHIRD) 2004-2011 in Taiwan. Our goal was to re-confirm the old risk factors in modern society and to clarify the risk of cholangiocarcinoma in the medium time period following therapeutic ERCP or cholecystectomy in cholelithiasis patients.MATERIALS AND METHODSThis study was approved by the Institutional Review Board of Chung Shan Medical University Hospital, Taiwan. The IRB waved the need for informed consent in this study as it is a retrospective study based on the NHIRD. All authors declare no any conflicts of interest.Study designThis study is a population-based retrospective cohort study based on Taiwan’s NHIRD, which covers more than 99% of the Taiwanese population ADDIN EN.CITE <EndNote><Cite><Author>Cheng</Author><Year>2003</Year><RecNum>825</RecNum><DisplayText><style face="superscript">[35]</style></DisplayText><record><rec-number>825</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1486278740">825</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Cheng, T. M.</author></authors></contributors><auth-address>International Forum, Princeton University&apos;s International Center, USA.</auth-address><titles><title>Taiwan&apos;s new national health insurance program: genesis and experience so far</title><secondary-title>Health Aff (Millwood)</secondary-title></titles><periodical><full-title>Health Aff (Millwood)</full-title></periodical><pages>61-76</pages><volume>22</volume><number>3</number><keywords><keyword>Cost Sharing</keyword><keyword>Delivery of Health Care/economics/*organization &amp; administration/standards</keyword><keyword>Drug Costs</keyword><keyword>Health Expenditures/statistics &amp; numerical data</keyword><keyword>Health Services Accessibility</keyword><keyword>Humans</keyword><keyword>Medically Uninsured</keyword><keyword>National Health Programs/economics/*organization &amp; administration</keyword><keyword>Policy Making</keyword><keyword>Program Evaluation</keyword><keyword>Quality Assurance, Health Care</keyword><keyword>Taiwan</keyword><keyword>Universal Coverage</keyword><keyword>Utilization Review</keyword></keywords><dates><year>2003</year><pub-dates><date>May-Jun</date></pub-dates></dates><isbn>0278-2715 (Print)&#xD;0278-2715 (Linking)</isbn><accession-num>12757273</accession-num><urls><related-urls><url>;[35]. The study methods of NHIRD have been described in detail in previous studiesPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5XdTwvQXV0aG9yPjxZZWFyPjIwMDk8L1llYXI+PFJlY051

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ADDIN EN.CITE.DATA [36,37]. Symptomatic cholelithiasis cases with above 18 years of age were included from one million random samples of NHIRD data obtained between January 2005 and December 2007 using Codes of International Statistical Classification of Diseases and Related Health Problems-9th Edition (ICD-9), which were registered once in admission or three times in outpatient clinics to avoid bias from possible classification errors. After study group selection, we built the control group with propensity score matching by sex and age in a 1:3 ratio. The control group cases were defined as individuals who had neither been diagnosed with cholelithiasis nor undergone a related medical procedure, such as cholecystectomy or ERCP, in the previous year. Cholelithiasis patients who had undergone ES, EPBD, or cholecystectomy in the previous year or who were diagnosed after cholangiocarcinoma were excluded from further analysis. We then excluded patients, who diagnosed with cholangiocarcinoma from January to December 2004 in both the control and study groups. The cholangiocarcinoma patients in Taiwan have catastrophic illness cards that waive their medical expenses by ICD-9 registration; therefore, we considered that a one year time period for exclusion was adequate. The variables such as economic status, place of residence, follow-up time, and cholangiocarcinoma rate, as well as the historical common risk factors, such as CHB, CHC, HP, DM, end-stage renal disease (ESRD) on dialysis, congenital cystic disease of liver (CCDL), Clonorchis Opisthorchis (CO), and inflammatory bowel disease (IBD), were compared in cholelithiasis and control group.The cases of cholelithiasis were divided into three groups of patients who underwent ES or EPBD, patients who underwent cholecystectomy, and patients without any therapeutic intervention between January 2005 to December 2011. The patients who underwent both ES/EPBD and cholecystectomy were registered in the ES/EPBD group in our settings. The details of study design are shown in Figure 1. The ICD-9 codes for the listed diseases and procedure codes are listed in Supplementary Table 1. The stratification of age, gender, economic status, place of residence, follow-up time, cholangiocarcinoma rate, and historical common risk factors were compared in each group. Patients who experienced cholangiocarcinoma in the first 6 mo after ES, EPBD, or cholecystectomy were excluded from further analysis, because these cases should be considered as misdiagnoses or concurrent malignancies rather than subsequent cholangiocarcinoma. The time cumulative risk of cholangiocarcinoma in the different groups was calculated. Data processing and statistical analysisThe NHIRD, which includes one a representative population of one million persons residing in Taiwan between 2004 and 2011 was managed using Microsoft SQL Server 2008 R2 (Microsoft Corporation, Redmond, WA, United States) and the SQL programming language for the data query and data processing jobs. Statistical analysis was done using OpenEpi: Open source epidemiologic statistics for public health, version 3.01 ADDIN EN.CITE <EndNote><Cite><Author>Dean AG</Author><Year>updated 2013/04/06, accessed 2018/01/06</Year><RecNum>1081</RecNum><DisplayText><style face="superscript">[38]</style></DisplayText><record><rec-number>1081</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1531909509">1081</key></foreign-keys><ref-type name="Web Page">12</ref-type><contributors><authors><author>Dean AG, Sullivan KM, Soe MM.</author></authors></contributors><titles><title>OpenEpi: Open Source Epidemiologic Statistics for Public Health, Version.</title></titles><dates><year>updated 2013/04/06, accessed 2018/01/06</year></dates><urls><related-urls><url> </url></related-urls></urls></record></Cite></EndNote>[38]. Kaplan-Meier survival analyses were conducted using SPSS version 19. Person time analyses were done using OpenEpi version 3.01.Data obtained from the study were compared with the use of the 2 test for categorical variables, the t-test, or one-way ANOVA (Analysis of Variance) for continuous variables, and the Log Rank (Mantel-Cox) test for survival curves. A two-tailed P-value of 0.05 was considered statistically significant in this study.RESULTSBecause we used age and sex to find three times as many normal population subjects without cholelithiasis to be our control group, we could not evaluate age and sex as risk stratification in our comparisons of the cholelithiasis and control groups.Cholelithiasis cases and their matched controlsIn total, 7938 adult cholelithiasis cases were selected from one million random samples of NHIRD data obtained between January 2005 and December 2007. The control group consisted of 23814 cases without cholelithiasis and matched by age and sex. The mean age of both groups was 59.15 ± 16.53 and the proportion of female patients was 52.15% in both groups. The mean follow up time was 57.96 ± 21.48 mo in cholelithiasis group and 63.12 ± 15.6 mo in the normal population in our analysis. Demographic data revealed that the cholelithiasis patients had a minimum basic salary (49.92%) and residence in a lived in remote villages (1.65%) and the differences were statistically significant when compared to the control group. The proportion of historical risk factors for cholangiocarcinoma, like CHB, CHC, HP, DM, ESRD, CCDL, and IBD, were 9.50% vs 2.80%, 6.83% vs 1.99%, 1.61% vs 0.55%, 29.21% vs 18.17%, 2.34% vs 1.50%, 0.64% vs 0.03% and 1.5% vs 0.77% in the cholelithiasis group versus the normal population, respectively. All the proportions of comorbidity were significantly high (P < 0.001) in the cholelithiasis group, except for CO infection because neither group showed CO infection. In total,147 cholelithiasis cases and 39 normal population cases experienced cholangiocarcinoma during the follow-up period. After exclusion of cases with cholangiocarcinoma in the initial 6 mo in both groups, 55 cholelithiasis cases and 35 normal population cases developed cholangiocarcinoma, with a mean follow up of 36.73 ± 20.57 mo and 35.27 ± 19.94 mo, respectively. The subsequent cholangiocarcinoma rate was higher in the cholelithiasis group than in the control group (0.69% vs 0.15%, P < 0.001). The detailed information is shown in Table 1.Cholelithiasis cases that underwent ES/EPBD, cholecystectomy, and no interventionThere were 537 cases that underwent ES/EPBD, 1743 cases that underwent cholecystectomy, and 5658 cases that received no intervention, and we observed no significant difference in the mean age. However, the mean age after age stratification of patients above 70 years old was higher in the ES/EPBD group (79.11 ± 5.13), followed by the no intervention group (78.78 ± 6.08) and the cholecystectomy group (78.01 ± 5.54). Other demographic data in our analysis showed some differences: Follow-up time, place of residence, proportion of CHB, proportion of CHC, and proportion of CCDL. The details are shown in Table 2.In total, 27 patients (5.03%) were diagnosed with cholangiocarcinoma in the ES/EPBD group, while 105 (1.86%) were diagnosed with cholangiocarcinoma in the no intervention group, and 15 (0.86%) were diagnosed in the cholecystectomy group during the follow-up period. After exclusion of possible misdiagnoses and concurrent cholangiocarcinoma, by excluding cholangiocarcinoma diagnosed within 6 mo after the procedure, 11 (2.05%), 37 (0.65%), and 7 (0.40%) cholangiocarcinoma cases were diagnosed in the ES/EPBD, no intervention, and cholecystectomy groups, respectively. The time to diagnosis for subsequent cholangiocarcinoma was 41.17 ± 22.51 mo in the ES/EPBD group, 35.46 ± 19.08 mo in the no intervention group, and 33.70 ± 23.35 mo in the cholecystectomy group. The odds ratio for subsequent cholangiocarcinoma was 3.13 in the ES/EPBD group and 0.61 in cholecystectomy group when compared with the no intervention group. The results were similar if we excluded the cholangiocarcinoma cases within one year after the procedure or the diagnosis of cholelithiasis. The cumulative cholangiocarcinoma rates in the three groups in the 7-year follow-up period are demonstrated in Figure 2.The incidence of cholangiocarcinomaThe incidence of cholangiocarcinoma after the initial 6 mo was compared using incidence rate/1000 person-years. In the ES/EPBD group, the incidence of cholangiocarcinoma was 4.37 (2.30-7.59) per 1000 person-years, which is more than 15 times of the incidence of the normal population. The incidence of cholangiocarcinoma in ES/EPBD was especially high in females (6.31/1000 person-years) and patients older than 70 years (7.53/1000 person-years). In the cholecystectomy group, the incidence of cholangiocarcinoma was 0.79 (0.34–1.55) per 1000 person-years, which is still higher than the cholangiocarcinoma incidence in the normal population. The highest incidence of cholangiocarcinoma was found in patients older than 70 years (2.15/1000 person-years). The cholelithiasis patients without advanced intervention had an incidence of cholangiocarcinoma of 1.38 (0.99–1.88) per 1000 person-years. The highest incidence of cholangiocarcinoma in this subgroup was observed in men (1.72/1000 person-years) and in elderly patients (2.80/1000 person-years). The incidence comparisons are shown in Table 3. For the recurrent biliary events, the comparisons between cholangiocarcinoma patients and non-cholangiocarcinoma patients in ES/EPBD group were listed in the Supplementary Table 2. DISCUSSIONIn our study, the intervention rate was higher than that reported previously ADDIN EN.CITE <EndNote><Cite><Author>Lirussi</Author><Year>1999</Year><RecNum>1080</RecNum><DisplayText><style face="superscript">[39]</style></DisplayText><record><rec-number>1080</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1531904313">1080</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Lirussi, F.</author><author>Nassuato, G.</author><author>Passera, D.</author><author>Toso, S.</author><author>Zalunardo, B.</author><author>Monica, F.</author><author>Virgilio, C.</author><author>Frasson, F.</author><author>Okolicsanyi, L.</author></authors></contributors><auth-address>Institute of Internal Medicine, University of Padua, Italy.</auth-address><titles><title>Gallstone disease in an elderly population: the Silea study</title><secondary-title>Eur J Gastroenterol Hepatol</secondary-title></titles><periodical><full-title>Eur J Gastroenterol Hepatol</full-title></periodical><pages>485-91</pages><volume>11</volume><number>5</number><keywords><keyword>Age Factors</keyword><keyword>Aged</keyword><keyword>Cholelithiasis/chemistry/diagnostic imaging/*epidemiology/*physiopathology</keyword><keyword>Cross-Sectional Studies</keyword><keyword>Female</keyword><keyword>*Gallbladder Emptying</keyword><keyword>Humans</keyword><keyword>Italy/epidemiology</keyword><keyword>Male</keyword><keyword>Middle Aged</keyword><keyword>Prevalence</keyword><keyword>Radiography</keyword><keyword>Ultrasonography</keyword></keywords><dates><year>1999</year><pub-dates><date>May</date></pub-dates></dates><isbn>0954-691X (Print)&#xD;0954-691X (Linking)</isbn><accession-num>10755250</accession-num><urls><related-urls><url>;[ HYPERLINK \l "_ENREF_39" \o "Lirussi, 1999 #1080" 39], because this was a hospital-based cohort database, which meant that nearly all cholelithiasis cases were regarded as symptomatic patients. 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ADDIN EN.CITE.DATA [40], while the latter can be explained by diets high in cholesterol, saturated fat, and excess carbohydrates ADDIN EN.CITE <EndNote><Cite><Author>Gaby</Author><Year>2009</Year><RecNum>1078</RecNum><DisplayText><style face="superscript">[41]</style></DisplayText><record><rec-number>1078</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1531648847">1078</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Gaby, A. R.</author></authors></contributors><auth-address>American Holistic Medical Association, USA.</auth-address><titles><title>Nutritional approaches to prevention and treatment of gallstones</title><secondary-title>Altern Med Rev</secondary-title></titles><periodical><full-title>Altern Med Rev</full-title></periodical><pages>258-67</pages><volume>14</volume><number>3</number><keywords><keyword>Ascorbic Acid/*therapeutic use</keyword><keyword>Cholesterol/metabolism</keyword><keyword>Dietary Fats/adverse effects</keyword><keyword>Drug Combinations</keyword><keyword>Feeding Behavior</keyword><keyword>Gallstones/diet therapy/*drug therapy/etiology</keyword><keyword>Humans</keyword><keyword>Iron, Dietary/*therapeutic use</keyword><keyword>Lecithins/*therapeutic use</keyword><keyword>Monoterpenes/*therapeutic use</keyword><keyword>Nutrition Disorders/complications</keyword><keyword>Obesity/complications</keyword></keywords><dates><year>2009</year><pub-dates><date>Sep</date></pub-dates></dates><isbn>1089-5159 (Print)&#xD;1089-5159 (Linking)</isbn><accession-num>19803550</accession-num><urls><related-urls><url>;[41]. The same conditions explained the higher portion of cholelithiasis patients among residents of remote villages than in the normal population. Because primary sclerosing cholangitisPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5CZXJncXVpc3Q8L0F1dGhvcj48WWVhcj4yMDAyPC9ZZWFy

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ADDIN EN.CITE.DATA [10,11], CO ADDIN EN.CITE <EndNote><Cite><Author>Watanapa</Author><Year>2002</Year><RecNum>1056</RecNum><DisplayText><style face="superscript">[12]</style></DisplayText><record><rec-number>1056</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1530606604">1056</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Watanapa, P.</author><author>Watanapa, W. B.</author></authors></contributors><auth-address>Departments of Surgery and Physiology, Faculty of Medicine, Siriraj Hospital, Mahidol University, Bangkok 10 700, Thailand.</auth-address><titles><title>Liver fluke-associated cholangiocarcinoma</title><secondary-title>Br J Surg</secondary-title></titles><periodical><full-title>Br J Surg</full-title></periodical><pages>962-70</pages><volume>89</volume><number>8</number><keywords><keyword>Animals</keyword><keyword>Bile Duct Neoplasms/*parasitology/pathology/therapy</keyword><keyword>*Bile Ducts, Intrahepatic</keyword><keyword>Cholangiocarcinoma/*parasitology/pathology/therapy</keyword><keyword>Cricetinae</keyword><keyword>Diterpenes/therapeutic use</keyword><keyword>Epoxy Compounds</keyword><keyword>Humans</keyword><keyword>Liver Diseases, Parasitic/*complications</keyword><keyword>Opisthorchiasis/*complications</keyword><keyword>*Opisthorchis</keyword><keyword>*Phenanthrenes</keyword><keyword>Survival Analysis</keyword><keyword>Treatment Outcome</keyword></keywords><dates><year>2002</year><pub-dates><date>Aug</date></pub-dates></dates><isbn>0007-1323 (Print)&#xD;0007-1323 (Linking)</isbn><accession-num>12153620</accession-num><urls><related-urls><url>;[12], cholelithiasisPEVuZE5vdGU+PENpdGU+PEF1dGhvcj5XZWx6ZWw8L0F1dGhvcj48WWVhcj4yMDA3PC9ZZWFyPjxS

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ADDIN EN.CITE.DATA [19,20] are important risk factors for cholangiocarcinoma, we subjected these factors to further evaluation to compare cholelithiasis patients and a normal population. In our analysis, CHB, CHC, DM, HP infection, ESRD, CCDL, and IBD were more common in cholelithiasis patients and some of these factors logically increased the rate of cholangiocarcinoma by increasing the incidence of cholelithiasis ADDIN EN.CITE <EndNote><Cite><Author>Acalovschi</Author><Year>2009</Year><RecNum>814</RecNum><DisplayText><style face="superscript">[42]</style></DisplayText><record><rec-number>814</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1486266365">814</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Acalovschi, M.</author><author>Buzas, C.</author><author>Radu, C.</author><author>Grigorescu, M.</author></authors></contributors><auth-address>3rd Medical Clinic, University of Medicine and Pharmacy, Cluj-Napoca, Romania. monacal@umfcluj.ro</auth-address><titles><title>Hepatitis C virus infection is a risk factor for gallstone disease: a prospective hospital-based study of patients with chronic viral C hepatitis</title><secondary-title>J Viral Hepat</secondary-title><short-title>HCV vs gallstone</short-title></titles><periodical><full-title>J Viral Hepat</full-title></periodical><pages>860-6</pages><volume>16</volume><number>12</number><keywords><keyword>Adolescent</keyword><keyword>Adult</keyword><keyword>Aged</keyword><keyword>Aged, 80 and over</keyword><keyword>Fatty Liver/complications</keyword><keyword>Female</keyword><keyword>Gallstones/*epidemiology/*etiology</keyword><keyword>Hepatitis C, Chronic/*complications</keyword><keyword>Hospitals</keyword><keyword>Humans</keyword><keyword>Male</keyword><keyword>Middle Aged</keyword><keyword>Obesity/complications</keyword><keyword>Prevalence</keyword><keyword>Prospective Studies</keyword><keyword>Risk Factors</keyword><keyword>Young Adult</keyword></keywords><dates><year>2009</year><pub-dates><date>Dec</date></pub-dates></dates><isbn>1365-2893 (Electronic)&#xD;1352-0504 (Linking)</isbn><accession-num>19486279</accession-num><urls><related-urls><url>;[42]. Because CO infection is extremely rare in modern Taiwanese society, no CO-infected patient was found in our study in either group. The cholangiocarcinoma rate was higher in cholelithiasis patients than in the normal population (0.69% vs 0.15%), thereby confirming the previous concept of cholelithiasis as an important risk factor for cholangiocarcinoma.The rate of total cholangiocarcinoma and subsequent cholangiocarcinoma (diagnosed 6 mo after procedure) are highest in ES/EPBD patients, followed by cholelithiasis patients without intervention, and the lowest cholangiocarcinoma rate was found in cholecystectomy patients. The odds ratio of ES/EPBD patients for cholangiocarcinoma was 3.13 when compared with no intervention, indicating that the subsequent cholangiocarcinoma rate was high after ES/EPBD in cholelithiasis patients. Cholecystectomy decreased the cholangiocarcinoma rate in cholelithiasis patients in our study and this effect was compatible with previous literature reports ADDIN EN.CITE <EndNote><Cite><Author>Nordenstedt</Author><Year>2012</Year><RecNum>1079</RecNum><DisplayText><style face="superscript">[34]</style></DisplayText><record><rec-number>1079</rec-number><foreign-keys><key app="EN" db-id="2xsdas9ees02x4ew5545dve9sedxfx2ew09s" timestamp="1531659158">1079</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Nordenstedt, H.</author><author>Mattsson, F.</author><author>El-Serag, H.</author><author>Lagergren, J.</author></authors></contributors><auth-address>Upper Gastrointestinal Research, Department of Molecular Medicine and Surgery, Karolinska Institutet, Stockholm, Sweden. helena.nordenstedt@ki.se</auth-address><titles><title>Gallstones and cholecystectomy in relation to risk of intra- and extrahepatic cholangiocarcinoma</title><secondary-title>Br J Cancer</secondary-title></titles><periodical><full-title>Br J Cancer</full-title></periodical><pages>1011-5</pages><volume>106</volume><number>5</number><keywords><keyword>Adult</keyword><keyword>Aged</keyword><keyword>Bile Duct Neoplasms/diagnosis/epidemiology/*etiology</keyword><keyword>*Bile Ducts, Extrahepatic</keyword><keyword>*Bile Ducts, Intrahepatic</keyword><keyword>Cholangiocarcinoma/diagnosis/epidemiology/*etiology</keyword><keyword>*Cholecystectomy</keyword><keyword>Cohort Studies</keyword><keyword>Female</keyword><keyword>Gallstones/*complications/surgery</keyword><keyword>Humans</keyword><keyword>Male</keyword><keyword>Middle Aged</keyword><keyword>Risk Factors</keyword><keyword>Sweden/epidemiology</keyword></keywords><dates><year>2012</year><pub-dates><date>Feb 28</date></pub-dates></dates><isbn>1532-1827 (Electronic)&#xD;0007-0920 (Linking)</isbn><accession-num>22240785</accession-num><urls><related-urls><url>;[34].Another interesting finding of our study was the high incidence of cholangiocarcinoma in the medium time period for cholelithiasis patients who had undergone ES/EPBD, especially in women and in patients older than 70 years. However, current guidelines do not suggest close follow-up in these patients.This study has two major limitations. First, this is a retrospective database cohort study that showed an increase in the further incidence of cholangiocarcinoma after EST/EPBD in cholelithiasis patients, but the true consequence of cholangiocarcinoma and ES/EPBD is unclear. Second, even though this is a one million representative database, the incidence of cholangiocarcinoma is so low that we only found 11 cases, 7 cases, and 37 cases in the ES/EPBD, cholecystectomy, and without intervention group, respectively, but the power of our results is still credible. We will try to initiate a prospective hospital-based cohort study in cholelithiasis patients, who underwent therapeutic intervention to clarify the consequence of cholangiocarcinoma in ES/EPBD and cholecystectomy patients.In conclusion, symptomatic cholelithiasis did increase the cholangiocarcinoma rate in our analysis, and patients with cholelithiasis who underwent cholecystectomy could reduce the incidence of subsequent cholangiocarcinoma, but the incidence is still significantly higher than the incidence in the normal population. Meanwhile, the patients with cholelithiasis who undergo ES/EPBD are at high risk of subsequent cholangiocarcinoma.ARTICLE HIGHLIGHTSResearch backgroundCholangiocarcinoma is a highly lethal disease. There are many well known risk factors of cholangiocarcinoma, most of them result from chronic biliary system inflammation, such as primary sclerosing cholangitis, choledochal cyst disease, specific parasite infection, cholelithiasis, chronic hepatitis B and C infection, diabetes mellitus and Helicobacter infection, but the impacts of advanced biliary interventions, like endoscopic sphincterotomy (ES), endoscopic papillary balloon dilatation (EPBD) and cholecystectomy, are inconsistence in previous literature. It is important to understand the major hypothesis result in cholangiocarcinoma. Research motivationWe focused on the most common disease, cholelithiasis, which can result in cholangiocarcinoma. We conducted this study using the National Health Insurance Research Database to clarify the risks of cholangiocarcinoma after ES/EPBD, cholecystectomy or no intervention for cholelithiasis.Research objectivesWe try to evaluate hospital base cholelithiasis retrospective cohort and analyzed further cholangiocarcinoma risk in patients underwent ES/EPBD, cholecystectomy or no intervention for cholelithiasis. Further studies, to clarify whether the inflammation location or the different methods of therapeutic managements affect the incidence of cholangiocarcinoma, are needed in this field.Research methodsBecause of cholangiocarcinoma is still a disease with very low incidence in normal population, we collect data of NHIRD 2004-2011 in Taiwan using one million random samples. We selected 7938 cholelithiasis cases as well as 23,814 control group cases (matched by sex and age in 1:3 ratio). The incidences of total and subsequent cholangiocarcinoma were calculated in ES/EPBD patients, cholecystectomy patients, cholelithiasis patients without intervention and normal population. This topic is hard to be analyzed because subsequent cholangiocarcinoma incidence is low and both cholelithiasis and the managements for cholelithiasis maybe influence the cholangiocarcinoma rate.Research resultsThere are 537 cases underwent ES/EPBD, 1743 cases underwent cholecystectomy and 5658 cases without intervention in our cholelithiasis cohort. Eleven (2.05%), 37 (0.65%) and 7 (0.40%) subsequent cholangiocarcinoma cases diagnosed in ES/EPBD, no intervention and cholecystectomy group respectively and the odds ratio for subsequent cholangiocarcinoma is 3.13 in ES/EPBD group and 0.61 in cholecystectomy group comparing with no intervention group. Research conclusionsSymptomatic cholelithiasis patients underwent cholecystectomy had the lowest incidence of subsequent cholangiocarcinoma, but the incidence is still higher than normal population. Patients underwent ES/EPBD are in a high risk of subsequent cholangiocarcinoma and a follow-up plane should be needed in these kinds of patients. The hypotheses of these results can be explained by both inflammation at bile ducts increases incidence of cholangiocarcinoma than inflammation at gallbladder, or cholecystectomy reduce recurrent biliary events in cholelithiasis patients and decrease future cholangiocarcinoma rates. We need a series studies to clarify this mystery we left today.Research perspectivesThe future direction of research is to evaluate choledocholithiasis patients, who underwent therapeutic endoscopic retrograde cholangiopancreatography with or without further cholecystectomy, and their subsequent cholangiocarcinoma incidence. 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J Viral Hepat 2009; 16: 860-866 [PMID: 19486279 DOI: 10.1111/j.1365-2893.2009.01141.x]P-Reviewer: Lan C S-Editor: Ji FF L-Editor: E-Editor: Specialty type: OncologyCountry of origin: TaiwanPeer-review report classificationGrade A (Excellent): 0Grade B (Very good): BGrade C (Good): 0Grade D (Fair): 0 Grade E (Poor): 0Figure 1 Case selection flow chart of one million nationwide representative data base. ES/EPBD: Endoscopic sphincterotomy/endoscopic papillary balloon dilatation; NHIRD: National Health Insurance Research Database.Figure 2 Cumulative risk of cholangiocarcinoma. The cases of cholangiocarcinoma within 6 mo after the therapeutic procedure or the diagnosis of cholelithiasis were excluded. ES/EPBD: Endoscopic sphincterotomy/endoscopic papillary balloon dilatation.Table 1 Demographic data of study and normal populationCholelithiasis group n = 7938Control group n = 23814P valueNSD, %NSD, %Age, mean (SD)Age, yr 18-49 50-69 > 7059.1538.8959.1378.6716.537.385.525.9559.1538.9459.1378.6716.537.385.525.951.000Gender Male Female3798414047.8552.15113941242047.8552.151.000Follow up time (mo), mean (SD)57.9621.4863.1215.6< 0.001Economic status MBS 1-3 times MBS Above 3 times MBS3963313682549.9239.5110.391121610217233647.1042.909.81< 0.001Place of residence City Countryside Remote village 5046274713163.5734.611.6515078840328763.3235.291.210.007Comorbidity CHB CHC HP DM ESRD CCDL CO IBD75454212823191865101199.506.831.6129.212.340.640.001.506674741314327357701842.801.990.5518.171.500.030.000.77< 0.001< 0.001< 0.001< 0.001< 0.001< 0.001NA< 0.001Cholangiocarcinoma Number (rate) Follow up time (months), mean (SD)14713.921.8521.963931.80.1621.48< 0.001< 0.001Cholangiocarcinoma after first 6 mo Number (rate) Follow up time (mo), mean (SD)5536.730.6920.573535.270.1519.94< 0.0010.860SD: Standard deviation; MBS: Minimum basic salary; CHB: Chronic hepatitis B; CHC: Chronic hepatitis C; HP: Helicobacter infection; DM: Diabetes mellitus; ESRD: End-stage renal disease; CCDL: Congenital cystic disease of liver; CO: Clonorchis Opisthorchis; IBD: Inflammatory bowel disease.Table 2 The comparisons of cholelithiasis patients underwent therapeutic endoscopic retrograde cholangiopancreatography, cholecystectomy or no intervention ES/EPBD n = 537Cholecystectomy n = 1743Without intervention n = 5658P valueNSD, %NSD, %NSD, %Age, mean (SD)64.3316.3356.9516.5359.3416.430.941Age, yr 18-4939.297.5938.267.6039.097.270.391 50-6960.005.2059.305.5658.995.530.559 > 7079.115.7378.015.5478.786.080.002Gender0.692 Male26449.1684348.36269147.56 Female27350.8490051.64296752.44Follow up time (mo), mean (SD)56.3022.2461.3818.4056.8822.27< 0.001Economic status0.160 MBS31959.40113765.23359063.45 1-3 times MBS20938.9257432.93196434.71 Above 3 times MBS91.68281.61941.66Place of residence 0.009 City29655.1285449.00281349.72 Countryside20538.1868139.07225039.77 Remote village 366.7020411.7058510.34Comorbidity CHB509.311377.8656710.020.026 CHC224.10734.194477.90< 0.001 HP112.05231.32941.660.433 DM16731.1047827.42167429.590.135 ESRD122.23372.121372.420.760 CCDL132.42120.69260.46< 0.001 CO00.0000.0000.00NA IBD61.12231.32901.590.540CholangiocarcinomaNumber of cholangiocarcinoma275.03150.861051.86< 0.001Number of cholangiocarcinoma after first 6 mo112.0570.40370.65< 0.001Odds ratio3.130.611.00 Number of cholangiocarcinoma after first 12 mo10 1.86 6 0.34 350.62 < 0.001Odds ratio 3.01 0.56 1.00 Time to diagnosis of cholangiocarcinoma (excluding case in initial 6 mo), month41.1722.5133.7023.3535.4619.080.698SD: Standard deviation; MBS: Minimum basic salary; CHB: Chronic hepatitis B; CHC: Chronic hepatitis C; HP: Helicobacter infection; DM: Diabetes mellitus; ESRD: End-stage renal disease; CCDL: Congenital cystic disease of liver; CO: Clonorchis Opisthorchis; IBD: Inflammatory bowel disease.Table 3 Incidence of cholangiocarcinoma amount patient with cholelithiasis underwent therapeutic endoscopic retrograde cholangiopancreatography, cholecystectomy or no intervention compared with normal population (excluding cholangiocarcinoma in the initial 6 mo)VariablesPerson-years at risk in study cohortPerson-years at risk in control cohortNo. of observed cases of cholangiocarcinoma in study cohortNo. of observed cases of cholangiocarcinoma in control cohortIncidence rate/1000 person-years (95%CI) in study cohortIncidence rate/1000 person-years (95%CI) in control cohortES/EPBDTotal 2519.33125339.2111354.37 (2.30-7.59)0.28 (0.20-0.38)Gender Male1252.1259176.603202.40 (0.61-6.52)0.34 (0.21-0.51) Female1267.2166162.618156.31 (2.93-11.99)0.23 (0.13-0.37)Age, yr 18-49561.7437789.95151.78 (0.09-8.78)0.13 (0.05-0.29) 50-69895.3248272.572142.23 (0.38-7.38)0.29 (0.17-0.48) > 701062.2739276.698167.53 (3.50-14.30)0.41 (0.24-0.65)CholecystectomyTotal8911.32125339.217350.79 (0.34-1.55)0.28 (0.20-0.38)Gender Male4187.5659176.603200.72 (0.18-1.95)0.34 (0.21-0.51) Female4723.7666162.614150.85 (0.27-2.04)0.23 (0.13-0.37)Age, yr 18-493173.2337789.95150.32 (0.02-1.55)0.13 (0.05-0.29) 50-693413.7648272.571140.29 (0.01-1.45)0.29 (0.17-0.48) > 702324.3339276.695162.15 (0.79-4.77)0.41 (0.24-0.65)Cholelithiasis without interventionTotal 26820.41125339.2137351.38 (0.99-1.88)0.28 (0.20-0.38)Gender Male12201.359176.6021201.72 (1.09-2.59)0.34 (0.21-0.51) Female14619.1166162.6116151.09 (0.65-1.74)0.23 (0.13-0.37)Age, yr 18-498423.7737789.95450.48 (0.15-1.15)0.13 (0.05-0.29) 50-6910889.0448272.5712141.10 (0.60-1.87)0.29 (0.17-0.48) > 707507.6039276.6921162.80 (1.78-4.20)0.41 (0.24-0.65)ES/EPBD: Endoscopic sphincterotomy/endoscopic papillary balloon dilatation. ................
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