Evolution of features of chronic pancreatitis during endoscopic ultrasound-based surveillance of individuals at high risk for pancreatic cancer

• Abstract
• Introduction
• Patients and methods
• Statistical methods
• Results
• Participant characteristics
• Interobserver agreement
• Characteristics associated with features of chronic pancreatitis
• Intra-individual change in detected features of chronic pancreatitis
• Discussion
• Conclusion
• References

Abstract

Background and study aims During endoscopic ultrasound (EUS)-based pancreatic ductal adenocarcinoma (PDAC)-surveillance in asymptomatic individuals, features of chronic pancreatitis (CP) are often detected. Little is known about the prevalence and progression of these features. The aim of this study was to quantify these features, assess the interobserver agreement, assess possible associated factors, and assess the natural course during 3 years of follow-up.

Patients and methods Two experienced endosonographers reviewed anonymized sequential EUS videos of participants in PDAC surveillance that were obtained in 2012 and 2015 for features of CP. Descriptives, agreement analyses, univariate and multivariate analyses for possible risk factors, and repeated measures analyses to assess intra-individual changes over time were performed.

Results A total of 42 EUS videos of 21 participants were reviewed. Any feature of CP was present in 86 % (2012) and 81 % (2015) of participants, with a mean of 2.5 features per individual. The overall interobserver agreement was almost perfect at 83 %. No baseline factors were significantly associated with features of CP. Features did not change over time, except for hyperechoic foci without shadowing, which decreased intra-individually (β = – 1.6, P = 0.005).

Conclusions This blinded study shows features of CP to be highly prevalent in individuals at high risk of developing pancreatic cancer. No baseline factors were associated with presence of these features. CP features did not increase intra-individually over a 3-year period. Longer follow-up and pathological examination of pancreatic resection specimens will be essential to learn whether EUS detection and follow-up of these CP features bear clinical relevance.

Introduction

Over the past decades, multiple centers have initiated surveillance programs in individuals at high risk of developing pancreatic ductal adenocarcinoma (PDAC) to evaluate the diagnostic yield of such surveillance programs and ultimately improve poor survival of PDAC [1] [2] [3] [4] [5] [6] [7] [8] [9] [10] [11] [12] [13]. As recommended by the Cancer of the Pancreas Screening (CAPS) Consortium, most surveillance programs entail annual magnetic resonance imaging (MRI) as well as endoscopic ultrasound (EUS) imaging of the pancreas [14]. The diagnostic yield for detection of high-grade dysplastic precursor lesions (i. e., pancreatic intraductal neoplasia (PanIN)-3 and intraductal papillary mucinous neoplasms (IPMN) with high-grade dysplasia) or early stage PDAC varies between studies with an overall diagnostic yield of about 10 % [15].

During EUS-based PDAC surveillance, cystic or solid lesions can be detected and features of chronic pancreatitis (CP) also are frequently observed. The clinical significance of these CP features in asymptomatic individuals is still unclear. Research suggests that these features might be related to emerging PanIN and IPMN lesions [16] [17], however, little is known about the prevalence and progression of these CP features detected in asymptomatic high-risk individuals. Therefore, the aim of this study was to quantify CP features in individuals participating in our EUS/MRI-based surveillance program by reviewing stored videos of sequential EUS examinations and assess their progress over a 3-year period. We also aimed to study interobserver agreement in our series and assess possible factors associated with presence of these CP features.

Patients and methods

Our PDAC surveillance program has been described in detail before [13]. In summary, annual surveillance is performed using EUS and MRI/MRCP in individuals at inherited or familial increased risk of developing PDAC (≥ 10 % life-time risk, i. e. all carriers of CDKN2A gene mutations, all Peutz-Jeghers syndrome patients, carriers of gene mutations in BRCA1, BRCA2, TP53 or mismatch repair genes with a family history of PDAC in at least two family members, and first-degree relatives of patients with familial pancreatic cancer [FPC]). All EUS-investigations are performed under conscious sedation with midazolam/fentanyl by experienced endosonographers using a curvilinear device. Images of the pancreas are obtained from the duodenum and stomach and are digitally recorded in real time with lossy compression.

For this study, all participants in PDAC surveillance at the Erasmus University Medical Center Rotterdam, The Netherlands, were included for whom two EUS videos were available 3 years apart (2012 and 2015). The images were anonymized for patient ID and date of investigation. Two highly experienced endosonographers (MB and JWP, each over 3500 career EUS investigations) individually reassessed the videos for features of CP: parenchymal features [18] were scored in the head, body and tail of the pancreas and ductal features [18] were scored in the body and tail, using a standardized Case Record Form. The EUS videos were randomly assigned a video number and were thus assessed in an order for which no correlation could be made between patient ID or date of investigation. Both endosonographers scored the videos separately, after which a consensus meeting was held to discuss individuals in whom there was a difference in scored features.

The study was approved by the local Ethical Committee and was conducted in accordance with the Declaration of Helsinki. All participants provided written informed consent prior to performance of any study procedures.

Statistical methods

Descriptive statistics were used to describe participants’ characteristics. A proportion of agreement was calculated to assess interobserver agreement for each feature of CP. We considered an agreement of 0.00 as poor, 0.01 – 0.20 as slight, 0.21 – 0.40 as fair, 0.41 – 0.60 as moderate, 0.61 – 0.80 as substantial and 0.81 – 0.99 as almost perfect agreement and 1.00 as perfect agreement [19].

Data after consensus agreement were analyzed using descriptive statistics and univariate (Chi-square test, Fisher’s exact test and independent t-test where appropriate) and multivariate analyses, to detect participants’ characteristics associated with a mean of ≥ 4 CP features on EUS assessments. Intra-individual changes over time were assessed with repeated measures, generalized estimated equations for ordinal outcomes, and with mixed-effect models (growth curve models) with maximum likelihood estimator and unstructured covariance matrix for longitudinal data (non-proportional analyses). To correct for multiple testing, we only report P values < 0.01 as statistically significant. For all statistical analyses, the Statistical Package for the Social Sciences was used (version 23.0, SPSS Institute, Chicago, IL).

Results

Participant characteristics

In 2012, EUS videos of 26 individuals participating in surveillance were stored, of whom 21 individuals had a follow-up EUS video available in 2015. These 21 individuals were included in the study and their characteristics are summarized in [Table 1]. The mean age of the 21 included individuals was 52, they were predominantly female and there were no excessive alcohol consumers or diabetic participants.

Review of the first EUS video showed any feature of chronic pancreatitis in 18 of 21 (86 %) participants, and in 17 (81 %) at review of the second video, 3 years later (as specified in [Table 2]). The mean number of CP features per participant was 2.5 (range 0 – 7). When the Rosemont classification [18] was applied, only 52 % of screened individuals had a normal EUS examination and three (7 %) fulfilled criteria for CP.

Interobserver agreement

Results of the interobserver agreement analyses are shown in [Table 3]. On almost all CP features, there was an almost perfect to perfect agreement between the two reviewers. Substantial agreement was reached for hyperechoic foci without shadowing overall (69 % agreement), in the head (69 % agreement) and in the tail of the pancreas (79 % agreement)), for lobularity without honeycombing overall (71 % agreement) and in the body of the pancreas (71 % agreement), and for hyperechoic main pancreatic duct margins overall (71 % agreement), and in the body of the pancreas (79 % agreement). Only moderate agreement was reached for stranding overall, and in the head of the pancreas (59.5 and 52.4 % agreement, respectively). Agreement for all CP features (taken together, all possible CP features in any location of the pancreas, i. e. the 29 items from [Table 3]) rated as almost perfect at 83 %.

Characteristics associated with features of chronic pancreatitis

[Table 4] shows the results of univariate and multivariate analyses regarding possible risk factors associated with detection of a mean of ≥ 4 features of CP on EUS. On univariate analysis, “age of the youngest relative affected by PDAC” was the only identified risk factor (P = 0.002), but it was not sustained after multivariate analysis.

Intra-individual change in detected features of chronic pancreatitis

Results of the repeated measures generalized estimated equations analyses of intra-individual change in CP features are shown in [Table 2]. Except for hyperechoic foci without shadowing, which decreased intra-individually (overall (β = – 1.6, standard error [SE] 0.6, P = 0.006) and, more specifically, in the head of the pancreas (β = – 2.1, SE 0.7, P = 0.005), CP features did not change in the 3 years. Also, the mean number of CP features and the Rosemont classification did not change. However, there was one individual, a 60-year-old woman without a known gene mutation (FPC), in whom in 2012 only 1 feature of CP was present (a cyst in the head of the pancreas), while in 2015, no less than 7 features were detected (hyperechoic foci with and without shadowing, lobularity with and without honeycombing, stranding, MPD calculi, and hyperechoic MPD margins) ([Fig. 1]). Unfortunately, this patient subsequently died of trauma.

None of the individuals in this series underwent surgery between 2012 and 2015. One individual, a 50-year-old male without a known gene mutation (FPC), had already undergone a distal pancreatectomy in 2011 as a consequence of two EUS-detected solid lesions. Prior to surgery, no features of CP were detected. The resection specimen harbored a panIN-2 lesion and diffuse foci with panIN-1B. The EUS videos of the remnant pancreas from 2012 and 2015 showed hyperechoic foci without shadowing and hyperechoic MPD margins in 2012; in 2015 only, stranding was detected.

Discussion

This study shows CP features to be highly prevalent in asymptomatic participants in PDAC surveillance, with a substantial to almost perfect interobserver agreement. Also, these features hardly changed over a 3-year course of follow-up. 

Since the start of our PDAC surveillance program in 2008, features of CP were often detected, but their clinical relevance was unclear. They have been associated with incipient or emerging PanIN and IPMN lesions producing lobular parenchymal atrophy resulting in CP-like changes [16] [17]. Therefore, to assess detection of features of CP, interobserver agreement for these features, factors associated with them, and above all, the natural course of these features over time during EUS-based surveillance for PDAC in high-risk individuals, we conducted this blinded single-center study in which we reviewed stored videos from EUS examinations in 2012 and 2015.

In our series, we showed CP features to be highly prevalent: 86 % (in 2012) and 81 % (in 2015) of individuals had an EUS feature of CP; only 52 % of individuals fell into the category “normal” when the Rosemont classification [18] was applied. This prevalence is much higher than described in a non-high-risk cohort. Petrone et al. [20] described 16.8 % of asymptomatic individuals undergoing EUS for an indication not related to pancreatico-biliary disease as having at least one ductal or parenchymal abnormality present. As the prevalence of CP features in our cohort at high risk of developing PDAC is this high, the alleged association between (progression) of specific EUS features and presence of PanIN or IPMN lesions bears particular interest.

Assessing the intra-individual change in CP features over our 3-year study period, the number of CP features, individual CP features and Rosemont classification did not change, except for a statistically significant intra-individual decrease in hyperechoic foci without shadowing. However, development and progression of precursor lesions into PDAC may take multiple years [21]. Continued follow-up of these individuals therefore is of pivotal importance. Eventually, pathological examination of resected pancreatic specimens, not yet available from individuals in the current study, are needed to further clarify the association and clinical relevance of EUS detection of CP features.

Our study revealed no baseline factors significantly associated with detection of a mean of ≥ 4 CP features. Even factors that are known to be associated with CP, including smoking and alcohol consumption [22] [23], were not associated with detection of CP features in our cohort. Although speculative, this could be related to the underlying pathophysiologic mechanism of chronic pancreatitis-like changes in individuals at high risk of developing pancreatic cancer. Studies suggest that (multifocal) PanIN and IPMN lesions produce obstructive lobular atrophy or the pancreatic parenchyma which is likely the source of the CP-like changes that follow in these patients [16] [17].

Our analyses into interobserver agreement for detection of CP features showed an excellent agreement for most of the CP features. Overall agreement between the two expert endosonographers was 83 % and rated as almost perfect. This is somewhat better than described in previous reports where a moderate to substantial agreement was described [24] [25] [26] (kappa-values of 0.46, 0.65 and agreement of 68 %, respectively). Our high interobserver agreement might be explained by the fact that our two reviewers are highly trained and experienced endosonographers.

To our knowledge, this is the first study to longitudinally assess features of CP in asymptomatic high-risk individuals participating in an EUS-based PDAC surveillance program. Another strength of this study is that two expert endosonographers reviewed the EUS recordings in a blinded fashion using a standardized case record form. However, this study also has some limitations. The number of participants was limited and the follow-up comprised 3 years. None of the participating individuals underwent surgery and we therefore lack definite diagnoses and pathological correlates. Consequently, it is not possible to determine the clinical relevance of the different EUS features of CP that were detected. Also, the Rosement classification was applied in our cohort. This classification was not designed for the purpose of diagnosing CP in asymptomatic patients at high risk of developing PDAC. Although individual criteria can be readily applied and followed in an asymptomatic cohort of high-risk individuals undergoing PDAC surveillance, its clinical relevance in this setting remains unclear. The total score also may be less relevant than development of individual features over time.

Conclusion

In conclusion, this blinded study, reviewing EUS videos of asymptomatic high-risk individuals participating in EUS-based PDAC surveillance, showed features of CP to be highly prevalent but stable over a 3-year period, with high interobserver agreement. We could not associate any baseline factors with detection of these CP features. Longer follow-up and, if available, pathological examination of pancreatic resection specimens will be essential to understanding the relationship between these CP features and development of malignancy, and whether detection of these features bears clinical relevance, for example, in setting the indication for resection or serving as a criterion of influence in determining the screening interval.

Competing interests

None

• References

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• 9 Vasen HF, Wasser M, van Mil A. et al. Magnetic resonance imaging surveillance detects early-stage pancreatic cancer in carriers of a p16-Leiden mutation. Gastroenterology 2011; 140: 850-856
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• 10 Al-Sukhni W, Borgida A, Rothenmund H. et al. Screening for pancreatic cancer in a high-risk cohort: an eight-year experience. J Gastrointest Surg 2012; 16: 771-783
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• 11 Potjer TP, Schot I, Langer P. et al. Variation in precursor lesions of pancreatic cancer among high-risk groups. Clin Cancer Res 2013; 19: 442-449
  CrossrefPubMedGoogle Scholar
• 12 Harinck F, Kluijt I, Poley JW. et al. Comparative yield of endosonography and magnetic resonance imaging in individuals at high-risk for pancreatic cancer. Gastroenterology 2009; 136: A147
  PubMedGoogle Scholar
• 13 Harinck F, Konings IC, Kluijt I. et al. A multicentre comparative prospective blinded analysis of EUS and MRI for screening of pancreatic cancer in high-risk individuals. Gut 2016; 65: 1505-1513
  CrossrefPubMedGoogle Scholar
• 14 Canto MI, Harinck F, Hruban RH. et al. International cancer of the pancreas screening (CAPS) consortium summit on the management of patients with increased risk for familial pancreatic cancer. Gut 2013; 62: 339-347
  CrossrefPubMedGoogle Scholar
• 15 Konings ICAW, Harinck F, Poley JW. et al. Surveillance of individuals at high risk to develop pancreatic cancer: where do we stand. Am Oncol Hematol Rev; 2014: 70-79
  PubMedGoogle Scholar
• 16 Brune K, Abe T, Canto M. et al. Multifocal neoplastic precursor lesions associated with lobular atrophy of the pancreas in patients having a strong family history of pancreatic cancer. Am J Surg Pathol 2006; 30: 1067-1076
  PubMedGoogle Scholar
• 17 Aimoto T, Uchida E, Nakamura Y. et al. Multicentric pancreatic intraepithelial neoplasias (PanINs) presenting with the clinical features of chronic pancreatitis. J Hepatobiliary Pancreat Surg 2008; 15: 549-553
  CrossrefPubMedGoogle Scholar
• 18 Catalano MF, Sahai A, Levy M. et al. EUS-based criteria for the diagnosis of chronic pancreatitis: the Rosemont classification. Gastrointest Endosc 2009; 69: 1251-1261
  CrossrefPubMedGoogle Scholar
• 19 Landis JR, Koch GG. The measurement of observer agreement for categorical data. Biometrics 1977; 33: 159-174
  CrossrefPubMedGoogle Scholar
• 20 Petrone MC, Arcidiacono PG, Perri F. et al. Chronic pancreatitis-like changes detected by endoscopic ultrasound in subjects without signs of pancreatic disease: do these indicate age-related changes, effects of xenobiotics, or early chronic pancreatitis?. Pancreatology 2010; 10: 597-602
  CrossrefPubMedGoogle Scholar
• 21 Yachida S, Iacobuzio-Donahue CA. Evolution and dynamics of pancreatic cancer progression. Oncogene 2013; 32: 5253-5260
  CrossrefPubMedGoogle Scholar
• 22 Irving HM, Samokhvalov AV, Rehm J. Alcohol as a risk factor for pancreatitis. A systematic review and meta-analysis. JOP 2009; 10: 387-392
  PubMedGoogle Scholar
• 23 Andriulli A, Botteri E, Almasio PL. et al. Smoking as a cofactor for causation of chronic pancreatitis: a meta-analysis. Pancreas 2010; 39: 1205-1210
  CrossrefPubMedGoogle Scholar
• 24 Del Pozo D, Poves E, Tabernero S. et al. Conventional versus Rosemont endoscopic ultrasound criteria for chronic pancreatitis: interobserver agreement in same day back-to-back procedures. Pancreatology 2012; 12: 284-287
  CrossrefPubMedGoogle Scholar
• 25 Stevens T, Lopez R, Adler DG. et al. Multicenter comparison of the interobserver agreement of standard EUS scoring and Rosemont classification scoring for diagnosis of chronic pancreatitis. Gastrointest Endosc 2010; 71: 519-526
  CrossrefPubMedGoogle Scholar
• 26 Kalmin B, Hoffman B, Hawes R. et al. Conventional versus Rosemont endoscopic ultrasound criteria for chronic pancreatitis: comparing interobserver reliability and intertest agreement. Can J Gastroenterol 2011; 25: 261-264
  CrossrefPubMedGoogle Scholar

Corresponding author

• References

• 1 Schneider R, Slater EP, Sina M. et al. German national case collection for familial pancreatic cancer (FaPaCa): ten years experience. Fam Cancer 2011; 10: 323-330
  CrossrefPubMedGoogle Scholar
• 2 Canto MI, Hruban RH, Fishman EK. et al. Frequent detection of pancreatic lesions in asymptomatic high-risk individuals. Gastroenterology 2012; 142: 796-804 ; quiz e714-795
  CrossrefPubMedGoogle Scholar
• 3 Kimmey MB, Bronner MP, Byrd DR. et al. Screening and surveillance for hereditary pancreatic cancer. Gastrointestinal endoscopy 2002; 56: S82-86
  CrossrefPubMedGoogle Scholar
• 4 Canto MI, Goggins M, Yeo CJ. et al. Screening for pancreatic neoplasia in high-risk individuals: An EUS-based approach. Clin Gastroenterol Hepatol 2004; 2: 606-621
  CrossrefPubMedGoogle Scholar
• 5 Canto MI, Goggins M, Hruban RH. et al. Screening for Early Pancreatic Neoplasia in High-Risk Individuals: A Prospective Controlled Study. Clin Gastroenterol Hepatol 2006; 4: 766-781
  CrossrefPubMedGoogle Scholar
• 6 Poley JW, Kluijt I, Gouma DJ. et al. The yield of first-time endoscopic ultrasonography in screening individuals at a high risk of developing pancreatic cancer. Am J Gastroenterol 2009; 104: 2175-2181
  CrossrefPubMedGoogle Scholar
• 7 Verna EC, Hwang C, Stevens PD. et al. Pancreatic cancer screening in a prospective cohort of high-risk patients: A comprehensive strategy of imaging and genetics. Clin Cancer Res 2010; 16: 5028-5037
  CrossrefPubMedGoogle Scholar
• 8 Ludwig E, Olson SH, Bayuga S. et al. Feasibility and yield of screening in relatives from familial pancreatic cancer families. Am J Gastroenterol 2011; 106: 946-954
  CrossrefPubMedGoogle Scholar
• 9 Vasen HF, Wasser M, van Mil A. et al. Magnetic resonance imaging surveillance detects early-stage pancreatic cancer in carriers of a p16-Leiden mutation. Gastroenterology 2011; 140: 850-856
  CrossrefPubMedGoogle Scholar
• 10 Al-Sukhni W, Borgida A, Rothenmund H. et al. Screening for pancreatic cancer in a high-risk cohort: an eight-year experience. J Gastrointest Surg 2012; 16: 771-783
  CrossrefPubMedGoogle Scholar
• 11 Potjer TP, Schot I, Langer P. et al. Variation in precursor lesions of pancreatic cancer among high-risk groups. Clin Cancer Res 2013; 19: 442-449
  CrossrefPubMedGoogle Scholar
• 12 Harinck F, Kluijt I, Poley JW. et al. Comparative yield of endosonography and magnetic resonance imaging in individuals at high-risk for pancreatic cancer. Gastroenterology 2009; 136: A147
  PubMedGoogle Scholar
• 13 Harinck F, Konings IC, Kluijt I. et al. A multicentre comparative prospective blinded analysis of EUS and MRI for screening of pancreatic cancer in high-risk individuals. Gut 2016; 65: 1505-1513
  CrossrefPubMedGoogle Scholar
• 14 Canto MI, Harinck F, Hruban RH. et al. International cancer of the pancreas screening (CAPS) consortium summit on the management of patients with increased risk for familial pancreatic cancer. Gut 2013; 62: 339-347
  CrossrefPubMedGoogle Scholar
• 15 Konings ICAW, Harinck F, Poley JW. et al. Surveillance of individuals at high risk to develop pancreatic cancer: where do we stand. Am Oncol Hematol Rev; 2014: 70-79
  PubMedGoogle Scholar
• 16 Brune K, Abe T, Canto M. et al. Multifocal neoplastic precursor lesions associated with lobular atrophy of the pancreas in patients having a strong family history of pancreatic cancer. Am J Surg Pathol 2006; 30: 1067-1076
  PubMedGoogle Scholar
• 17 Aimoto T, Uchida E, Nakamura Y. et al. Multicentric pancreatic intraepithelial neoplasias (PanINs) presenting with the clinical features of chronic pancreatitis. J Hepatobiliary Pancreat Surg 2008; 15: 549-553
  CrossrefPubMedGoogle Scholar
• 18 Catalano MF, Sahai A, Levy M. et al. EUS-based criteria for the diagnosis of chronic pancreatitis: the Rosemont classification. Gastrointest Endosc 2009; 69: 1251-1261
  CrossrefPubMedGoogle Scholar
• 19 Landis JR, Koch GG. The measurement of observer agreement for categorical data. Biometrics 1977; 33: 159-174
  CrossrefPubMedGoogle Scholar
• 20 Petrone MC, Arcidiacono PG, Perri F. et al. Chronic pancreatitis-like changes detected by endoscopic ultrasound in subjects without signs of pancreatic disease: do these indicate age-related changes, effects of xenobiotics, or early chronic pancreatitis?. Pancreatology 2010; 10: 597-602
  CrossrefPubMedGoogle Scholar
• 21 Yachida S, Iacobuzio-Donahue CA. Evolution and dynamics of pancreatic cancer progression. Oncogene 2013; 32: 5253-5260
  CrossrefPubMedGoogle Scholar
• 22 Irving HM, Samokhvalov AV, Rehm J. Alcohol as a risk factor for pancreatitis. A systematic review and meta-analysis. JOP 2009; 10: 387-392
  PubMedGoogle Scholar
• 23 Andriulli A, Botteri E, Almasio PL. et al. Smoking as a cofactor for causation of chronic pancreatitis: a meta-analysis. Pancreas 2010; 39: 1205-1210
  CrossrefPubMedGoogle Scholar
• 24 Del Pozo D, Poves E, Tabernero S. et al. Conventional versus Rosemont endoscopic ultrasound criteria for chronic pancreatitis: interobserver agreement in same day back-to-back procedures. Pancreatology 2012; 12: 284-287
  CrossrefPubMedGoogle Scholar
• 25 Stevens T, Lopez R, Adler DG. et al. Multicenter comparison of the interobserver agreement of standard EUS scoring and Rosemont classification scoring for diagnosis of chronic pancreatitis. Gastrointest Endosc 2010; 71: 519-526
  CrossrefPubMedGoogle Scholar
• 26 Kalmin B, Hoffman B, Hawes R. et al. Conventional versus Rosemont endoscopic ultrasound criteria for chronic pancreatitis: comparing interobserver reliability and intertest agreement. Can J Gastroenterol 2011; 25: 261-264
  CrossrefPubMedGoogle Scholar