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1. 2506 Post-discharge opioid prescriptions and their association with healthcare utilization in the Vanderbilt Inpatient Cohort Study

Author

Justin Scott Liberman, Lauren R. Samuels, Kathryn M. Goggins, Sunil Kripalani, and Christianne Roumie

Subjects
Medicine
Abstract

OBJECTIVES/SPECIFIC AIMS: Opioid prescribing is common and increasing in certain areas of the country with known risk of misuse and dependence. Our study examined the association of opioid prescription at discharge after hospitalization for acute coronary syndrome (ACS) or acute decompensated heart failure (ADHF) with emergency department (ED) care or all-cause readmission, intended healthcare utilization (follow-up with physician within 30 d of discharge and cardiac rehab participation), and all-cause mortality. METHODS/STUDY POPULATION: The Vanderbilt Inpatient Cohort Study is a prospective cohort of hospitalized patients age >18 enrolled with either ACS or ADHF between 2011 and 2015 (index hospitalization). We then excluded those who died during the index hospitalization, patients with hospitalization

Published
2018
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2. Unexpected diagnosis resulting from presentation with Chronic Obstructive Pulmonary Disease (COPD) exacerbation

Author

B Casserly, M Goggins, and C Farrell

Subjects
medicine.medical_specialty, Bronchocele, business.industry, Copd exacerbation, Squamous cell carcinoma, Internal medicine, Bronchoscopy, Carcinoid tumour, Medicine, Pulmonary disease, Presentation (obstetrics), business
Abstract

A bronchocele (bronchial mucocele) is a cystic formation caused by impacted mucoid secretion within the bronchial tree. Non-obstructive causes include bronchiectasis, cystic fibrosis, and asthma while obstructive causes include foreign bodies, benign strictures, congenital bronchial atresia, and in rare cases neoplasms. We describe the case of a 79-year-old male presented with increasing shortness of breath and pleuritic chest pain. He was treated for an infective exacerbation of chronic obstructive pulmonary disease (COPD). He was a current smoker with greater than a 40-year pack history. D-dimers were elevated at 1.49 and he underwent a computed tomography pulmonary angiogram that showed lobulated mass in the right lower lobe suggestive of a bronchocele. The patient underwent a bronchoscopy that demonstrated findings consistent carcinoid tumor. Transbronchial biopsies surprisingly revealed moderately differentiated squamous cell carcinoma. In rare cases, neoplasms have been associated with bronchoceles emphasising the importance of bronchoscopy (for direct visualisation) and biopsy in the workup. Keywords:Bronchocele; Bronchoscopy; Carcinoid tumour; Squamous cell carcinoma

Published
2019
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3. Validation of histomolecular classification utilizing histological subtype, MUC1, and CDX2 for prognostication of resected ampullary adenocarcinoma

Author

Burcu Saka, N Neishaboori, Neda Rezaee, Michael J. Overman, Aaron J. Schueneman, Huamin Wang, Sun M. Lee, Gauri R. Varadhachary, Anirban Maitra, M. Goggins, Christopher L. Wolfgang, Volkan Adsay, and Joe Ensor

Subjects
Adult, Male, Ampulla of Vater, Cancer Research, medicine.medical_specialty, Pathology, Colorectal cancer, ampullary adenocarcinoma, Common Bile Duct Neoplasms, Perineural invasion, MUC1, Adenocarcinoma, Gastroenterology, Cohort Studies, Breast cancer, Internal medicine, medicine, Humans, CDX2 Transcription Factor, Lung cancer, Molecular Diagnostics, Aged, Aged, 80 and over, Homeodomain Proteins, business.industry, Mucin-1, Histology, Middle Aged, Prognosis, medicine.disease, digestive system diseases, Staining, Oncology, CDX2, Immunohistochemistry, Female, Liver cancer, business, prognostic, histomolecular phenotype
Abstract

Background: Outcomes for ampullary adenocarcinomas are heterogeneous, and numerous methods of categorisation exist. A histomolecular phenotype based on histology, caudal-type homeodomain transcription factor 2 (CDX2) staining and Mucin 1 (MUC1) staining has recently been tested and validated in two cohorts. We attempt to validate this classification in a large patient population. Methods: Tissue samples from 163 patients with resected ampullary adenocarcinoma were classified based on histology and immunohistochemical expression of CDX2 and MUC1. A pancreaticobiliary histomolecular classification (PB) was defined as a sample with pancreaticobiliary histology, positive MUC1 and negative CDX2 expression. Results: There were 82 deaths; median follow-up of 32.4 months; and median overall survival of 87.7 (95% CI 42.9–109.5) months. PB comprised 28.2% of the cases. Factors associated with overall survival were histological subtype (P=0.0340); T1/2 vs T3/4 (P=0.001); perineural (P

Published
2015
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4. Predictors of Health Care System and Physician Distrust in Hospitalized Cardiac Patients

Author

Charu Gupta, Susan P. Bell, Jonathan S. Schildcrout, Sarah Fletcher, Kathryn M. Goggins, Sunil Kripalani, and null for the Vanderbilt Inpatient Cohort

Subjects
Adult, Male, medicine.medical_specialty, Health (social science), media_common.quotation_subject, education, Population, Health literacy, Library and Information Sciences, Trust, Article, Social support, health services administration, Adaptation, Psychological, Health care, Humans, Medicine, Prospective Studies, Acute Coronary Syndrome, Psychiatry, Socioeconomic status, health care economics and organizations, Aged, media_common, Heart Failure, Inpatients, Physician-Patient Relations, education.field_of_study, Distrust, business.industry, Communication, Public Health, Environmental and Occupational Health, Social Support, Middle Aged, humanities, Health Literacy, Multivariate Analysis, behavior and behavior mechanisms, Female, Observational study, business, Attitude to Health, Psychosocial
Abstract

Trusting relationships among patients, physicians, and the health care system is important in encouraging self-care behaviors in cardiovascular patients. This study aimed to assess the prevalence of health care system and physician distrust in this population, compare the 2 forms of distrust, and describe the demographic, socioeconomic, and psychosocial predictors of high distrust. A total of 1,232 hospitalized adults with acute coronary syndrome or heart failure were enrolled in a prospective, observational study assessing health care system distrust and physician distrust. High health care system distrust (35%) was observed across the population, with lower levels of interpersonal physician distrust (16%). In a multivariate analysis, poor social support and coping skills were strong predictors of both health care system (p=.026, p=.003) and physician distrust (p

Published
2014
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5. Health Literacy, Numeracy, and Other Characteristics Associated With Hospitalized Patients' Preferences for Involvement in Decision Making

Author

Kathryn M. Goggins, Kenneth A. Wallston, Samuel Nwosu, Jonathan S. Schildcrout, Liana Castel, Sunil Kripalani, and null for the Vanderbilt Inpatient Cohort

Subjects
Adult, Male, Health (social science), Health literacy, Disease, Library and Information Sciences, Trust, Article, Social support, Sex Factors, Numeracy, Health care, Humans, Medicine, Prospective Studies, Patient participation, Aged, Inpatients, business.industry, Communication, Public Health, Environmental and Occupational Health, Social Support, Patient Preference, Mathematical Concepts, Middle Aged, Educational attainment, Health Literacy, Cardiovascular Diseases, Multivariate Analysis, Educational Status, Female, Patient Participation, business, Attitude to Health, Clinical psychology, Cohort study
Abstract

Little research has examined the association of health literacy and numeracy with patients' preferred involvement in the problem-solving and decision-making process in the hospital. Using a sample of 1,249 patients hospitalized with cardiovascular disease from the Vanderbilt Inpatient Cohort Study (VICS), we assessed patients' preferred level of involvement using responses to two scenarios of differing symptom severity from the Problem-Solving Decision-Making Scale. Using multivariable modeling, we determined the relationship of health literacy, subjective numeracy, and other patient characteristics with preferences for involvement in decisions, and how this differed by scenario. The authors found that patients with higher levels of health literacy desired more participation in the problem-solving and decision-making process, as did patients with higher subjective numeracy skills, greater educational attainment, female gender, less perceived social support, or greater health care system distrust (p

Published
2014
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6. Tumour epithelial vimentin expression and outcome of pancreatic ductal adenocarcinomas

Author

Seung-Mo Hong, Kimberly Walter, Adriana Handra-Luca, M. Goggins, Christopher L. Wolfgang, and Ralph H. Hruban

Subjects
Adult, Male, Cancer Research, Pathology, medicine.medical_specialty, Pancreatic disease, Vimentin, macromolecular substances, Epithelium, 03 medical and health sciences, 0302 clinical medicine, vimentin, Pancreatectomy, medicine, Carcinoma, Biomarkers, Tumor, Humans, pancreas, Molecular Diagnostics, 030304 developmental biology, Aged, Aged, 80 and over, 0303 health sciences, Tissue microarray, adenocarcinoma, biology, business.industry, Cancer, Middle Aged, medicine.disease, Prognosis, Immunohistochemistry, Survival Analysis, Pancreatic Neoplasms, medicine.anatomical_structure, Oncology, Tissue Array Analysis, 030220 oncology & carcinogenesis, biology.protein, Adenocarcinoma, Female, business, Pancreas, Carcinoma, Pancreatic Ductal
Abstract

Purpose: Tumour epithelial vimentin expression is a marker of mesenchymal differentiation and may be a useful marker of carcinomas with more aggressive behaviour. The aim of this study was to determine the extent and prognostic significance of vimentin expression in pancreatic ductal adenocarcinomas. Methods: Vimentin expression was detected by immunohistochemistry on tissue microarrays of surgically resected pancreatic ductal adenocarcinomas from 387 patients. The percentage of vimentin-immunolabelled neoplastic cells was correlated with outcome and with clinico–pathological factors using the Kaplan–Meier method and Cox multivariate survival models. Results: In all, 45% of primary pancreatic adenocarcinomas contained neoplastic cells that expressed vimentin, and in 27.5% of the cancers >10% of cells expressed vimentin. Vimentin expression was correlated with poor histological differentiation. By both uni- and multivariate survival analysis, neoplastic vimentin expression (P

Published
2011

7. Seasonal variation of vitamin D in patients on hemodialysis

Author

S. Bhat, Ajay Gupta, M. Goggins, D. S. Rao, and R. Tolouian

Subjects
Adult, Male, medicine.medical_specialty, medicine.medical_treatment, Population, Prevalence, Gastroenterology, vitamin D deficiency, Renal Dialysis, Risk Factors, Internal medicine, medicine, Vitamin D and neurology, Humans, Renal osteodystrophy, education, Aged, Retrospective Studies, Aged, 80 and over, Analysis of Variance, Hyperparathyroidism, education.field_of_study, Chi-Square Distribution, business.industry, General Medicine, Middle Aged, Vitamin D Deficiency, medicine.disease, Endocrinology, Nephrology, Kidney Failure, Chronic, Female, Secondary hyperparathyroidism, Seasons, Hemodialysis, business
Abstract

Background: Seasonal and racial differences in serum 25-hydroxyvitamin D levels have been studied extensively in the general population but not in patients with end-stage renal disease (ESRD). Methods: Serum 25-hydroxyvitamin D levels, the best available index of vitamin D nutrition, was measured at the end of summer (September) in 142 chronic hemodialysis patients and again at the end of winter (April) in 73 of these 142 patients, to determine the prevalence and risk factors for vitamin D deficiency. Results: The prevalence of vitamin D depletion, as defined by serum 25-hydroxy-vitamin D level of less than 20 ng/ml (50 nmol/l), was 54% at the end of summer and further increased to 86% by the end of winter (p < 0.0001 summer vs. winter). We observed that women and African-Americans had a greater prevalence of hypovitaminosis D (p < 0.0002 and p < 0.001 for both comparisons, respectively). Surprisingly, diabetic status, age, and the duration of ESRD were not associated with a significant increase in risk of vitamin D depletion. Conclusion: Vitamin D depletion is present in about half of ESRD patients with marked seasonal variations. Patients with ESRD should have more frequent assessments of their vitamin D nutrition by serum 25-hydroxyvitamin D levels, and vitamin D supplementation should be routinely prescribed, which may prevent many of the complications related to vitamin D deficiency and secondary hyperparathyroidism.

Published
2010
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8. Aberrant methylation of suppressor of cytokine signalling-1 (SOCS-1) gene in pancreatic ductal neoplasms

Author

M. Goggins, Ralph H. Hruban, Gloria H. Su, Fikret Sahin, Noriyoshi Fukushima, and Norihiro Sato

Subjects
Adult, Male, Transcriptional Activation, Cancer Research, Pancreatic disease, Pancreatic Intraepithelial Neoplasia, pancreatic ductal adenocarcinoma, Suppressor of Cytokine Signaling Proteins, Biology, CpG island methylation, SOCS-1, 03 medical and health sciences, 0302 clinical medicine, Suppressor of Cytokine Signaling 1 Protein, Pancreatic cancer, medicine, JAK/STAT pathway, Biomarkers, Tumor, Tumor Cells, Cultured, Humans, 030304 developmental biology, Aged, Regulation of gene expression, Aged, 80 and over, 0303 health sciences, IL-6, Reverse Transcriptase Polymerase Chain Reaction, Intracellular Signaling Peptides and Proteins, Genetics and Genomics, Ductal carcinoma, DNA Methylation, Middle Aged, medicine.disease, 3. Good health, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, Repressor Proteins, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, DNA methylation, Cancer research, CA19-9, Female, Pancreas, Carrier Proteins, Carcinoma, Pancreatic Ductal
Abstract

The suppressor of cytokine signalling-1 (SOCS-1) gene is frequently silenced in human hepatocellular carcinoma by aberrant methylation. The aim of this study was to determine if SOCS-1 is inactivated in pancreatic ductal neoplasms, and to investigate if aberrant methylation of this gene affected the Janus kinase/signal transducers and activators of transcription (JAK/STAT) pathway. Aberrant methylation in the CpG island of the SOCS-1 gene was detected in six of 19 (31.6%) human pancreatic cancer cell lines using methylation-specific PCR, and was associated with a loss or reduction of gene expression in five of the six methylated cell lines. Thirteen of 60 pancreatic ductal adenocarcinomas (21.7%) and two of 34 intraductal papillary mucinous neoplasms (IPMNs) (5.9%) had methylated SOCS-1. In contrast, SOCS-1 methylation was not seen in pancreatic normal ductal epithelia (zero out of 15), in pancreatic intraepithelial neoplasia (PanINs) (zero out of 49) or in the IPMNs without infiltrating cancer (zero out of 20). 5-Aza-2'-deoxycytidine treatment of the SOCS-1-methylated pancreatic cancer cell lines led to restoration of SOCS-1 gene expression. Interleukin-6, which has been shown to act through the JAK/STAT pathway to increase cell growth, induced modest time and dose-dependent cell proliferation in a SOCS-1-methylated cell line (PL10, P=0.015) but not in two unmethylated cell lines. These results indicate that loss of SOCS-1 gene is associated with transcriptional silencing and may have growth-promoting effects, and that its methylation is a useful marker of pancreatic cancer.

Published
2003

9. AGA abstracts 612-S988

Author

Sanjay B. Jagannath, Marcia Irene Canto, Noriyoshi Fukushima, Christophe Rosty, M. Goggins, M. Yeatman, and H. Niiyama

Subjects
medicine.anatomical_structure, Hepatology, business.industry, Aberrant methylation, Gastroenterology, Cancer research, Medicine, business, Pancreas
Published
2002
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10. Role of tumor markers and mutations in cells and pancreatic juice in the diagnosis of pancreatic cancer

Author

Ralph H. Hruban, M. Tascilar, Eric Caspers, P. D. J. Sturm, G. J. A. Offerhaus, and M. Goggins

Subjects
Pancreatic disease, business.industry, Hematology, medicine.disease, medicine.disease_cause, medicine.anatomical_structure, Oncology, Pancreatic cancer, Pancreatic juice, medicine, Cancer research, CA19-9, KRAS, Pancreas, business, Survival rate, Tumor marker
Abstract

Summary Background: Unresectability at the time of presentation is the most important reason for the poor survival rate of pancreatic carcinoma. Molecular-based tests might improve the early detection of pancreatic cancer at a time when surgical resection is still an option for cure. Methods:The literature was reviewed concerning the role of molecular-based tests applied to sources other than pancreatic tissue itself, including ERCP-samples, blood and stool, with emphasis on the detection of K-ras mutations and mutant p53 gene product. Results:K-ras mutations have been succesfully detected in ERCP brush samples, leading to an increase of the sensitivity and improvement of the diagnostic yield. When pancreatic juice and duodenal fluid are tested for K-ras mutations, the yield is less. Kras mutations can also be detected in the blood, especially in patients with larger tumors. The presence of K-ras mutations proved also to be useful in discriminating benign and malignant liver nodules, i.e. when during surgery there is suspicion of liver metastases of pancreatic cancer.The accumulation of p53 gene product to immunochemically detectable levels in ERCP brush samples also increases the sensitivity of conventional light microscopy. Other molecular markers such as telomerase and TIMP-1 may prove to be useful too, but await more extensive evaluation.

Published
1999
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11. Determinants of health after hospital discharge: rationale and design of the Vanderbilt Inpatient Cohort Study (VICS)

Author

Abby G, Meyers, Amanda, Salanitro, Kenneth A, Wallston, Courtney, Cawthon, Eduard E, Vasilevskis, Kathryn M, Goggins, Corinne M, Davis, Russell L, Rothman, Liana D, Castel, Katharine M, Donato, John F, Schnelle, Susan P, Bell, Jonathan S, Schildcrout, Chandra Y, Osborn, Frank E, Harrell, and Sunil, Kripalani

Subjects
Heart Failure, Male, Inpatients, Patient discharge, Social Determinants of Health, Patient readmission, Health Status, Social Support, Health literacy, Continuity of Patient Care, Middle Aged, Severity of Illness Index, Patient Outcome Assessment, Self Care, Hospitalization, Study Protocol, Transitions of care, Humans, Female, Prospective Studies, Acute Coronary Syndrome, Social determinants, Aged, Quality of Health Care
Abstract

Background The period following hospital discharge is a vulnerable time for patients when errors and poorly coordinated care are common. Suboptimal care transitions for patients admitted with cardiovascular conditions can contribute to readmission and other adverse health outcomes. Little research has examined the role of health literacy and other social determinants of health in predicting post-discharge outcomes. Methods The Vanderbilt Inpatient Cohort Study (VICS), funded by the National Institutes of Health, is a prospective longitudinal study of 3,000 patients hospitalized with acute coronary syndromes or acute decompensated heart failure. Enrollment began in October 2011 and is planned through October 2015. During hospitalization, a set of validated demographic, cognitive, psychological, social, behavioral, and functional measures are administered, and health status and comorbidities are assessed. Patients are interviewed by phone during the first week after discharge to assess the quality of hospital discharge, communication, and initial medication management. At approximately 30 and 90 days post-discharge, interviewers collect additional data on medication adherence, social support, functional status, quality of life, and health care utilization. Mortality will be determined with up to 3.5 years follow-up. Statistical models will examine hypothesized relationships of health literacy and other social determinants on medication management, functional status, quality of life, utilization, and mortality. In this paper, we describe recruitment, eligibility, follow-up, data collection, and analysis plans for VICS, as well as characteristics of the accruing patient cohort. Discussion This research will enhance understanding of how health literacy and other patient factors affect the quality of care transitions and outcomes after hospitalization. Findings will help inform the design of interventions to improve care transitions and post-discharge outcomes.

Published
2013

12. Expression of CD44 and its variants on gastric epithelial cells of patients with Helicobacter pylori colonisation

Author

X, Fan, A, Long, M, Goggins, P W, Keeling, and D, Kelleher

Subjects
Adult, Male, medicine.medical_treatment, Lymphocyte, Peripheral blood mononuclear cell, Helicobacter Infections, Gastric mucosa, medicine, Humans, Lymphocytes, Aged, Helicobacter pylori, biology, Stomach, CD44, Gastroenterology, Middle Aged, Flow Cytometry, biology.organism_classification, Up-Regulation, Hyaluronan Receptors, medicine.anatomical_structure, Cytokine, Gastric Mucosa, Case-Control Studies, Immunology, biology.protein, Intraepithelial lymphocyte, Female, Research Article
Abstract

BACKGROUND--Studies have suggested that expression of the adhesion molecule CD44 may be of prognostic importance in gastric cancer. In addition, there is strong evidence that Helicobacter pylori has a role in gastric cancer. AIMS--To determine the expression of CD44 and its variants (v6, v9) and HLA class II molecules on human gastric epithelial cell and intraepithelial lymphocytes in patients with and without H pylori infection. PATIENTS--Eighteen patients (seven men and 11 women) attending for endoscopic evaluation because of upper gastrointestinal symptoms were included. An additional 10 patients (five men and five women) were analysed for CD44 variant expression). METHODS--Biopsy specimens were taken from the gastric antrum during endoscopy. Gastric epithelial cells and intraepithelial lymphocytes were examined by two colour flow cytometry and compared in patients with and without H pylori infection. RESULTS--Expression of CD44 and its variants (CD44 v9) was increased in epithelial cells but not in intraepithelial lymphocytes. Both epithelial cells and intraepithelial lymphocytes expressed higher levels of HLA class II molecules (DR and DP), possibly as a result of local cytokine production. Furthermore, results showed upregulation of CD44 on a gastric epithelial cell line (AGS) by cytokines and peripheral blood mononuclear cell supernatant. CONCLUSIONS--These data suggest that H pylori, either directly or through a local inflammatory response, is responsible for increased expression of CD44 and its variant CD44 v9. These data are of potential importance in relation to increased expression of CD44 and CD44 v9 on gastric carcinoma.

Published
1996
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13. Primordial germ cell as potent cell of origin of mucinous cystic neoplasms of the pancreas and mucinous ovarian tumors

Author

Michelle S. Hirsch, Ronny Drapkin, M. Goggins, Petros Tsantoulis, Allison F. Vitonis, Kevin M. Elias, Candace L. Kerr, Intidhar Labidi-Galy, Michael J. Birrer, Jason L. Hornick, Leona A. Doyle, and Daniel W. Cramer

Subjects
Oncology, medicine.medical_specialty, medicine.anatomical_structure, business.industry, Cell of origin, Internal medicine, Cancer research, Medicine, Primordial germ cell, Hematology, business, Pancreas
Published
2016
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14. Irish Society of Gastroenterology

Author

M. Woods, L. J. D. O’Donnell, B. Battistini, T. Warner, J. Vane, M. G. Fartming, J. Yaqoob, J. J. Wu, L. A. Norris, M. I. Khan, P. W. N. Keeling, D. Maguire, G. O’Sullivan, B. Harvey, B. Curran, Y. Xin∘, E. W. Kay, M. Leader, K. Henry, O. Crosbie, S. Norris, P. Costello, C. O’Farrelly, J. Hegarty, B. Kennedy, M. Duggan, R. Plant, E. K. Kenny-Walsh, P. Cotter, M. J. Whelton, M. Maloney, N. Noonan, M. Buckley, H. Hamilton, S. Beattie, C. O’Morain, B. McNamara, J. Cuffe, R. A. Barry, D. A. Collins, G. C. O’Sullivan, J. K. Collins, F. Shanahan, M. M. Skelly, H. E. Mulcahy, A. Troy, T. Connell, C. Duggan, M. J. Duffyt, K. Sheahan, D. P. O’Donoghue, H. X. Xia, D. Hyde, M. G. O’Brien, E. F. Fitzgerald, G. Lee, A. J. Hussey, T. J. Boyle, B. Garrihy, O. P. Clinton, O. J. McAnena, G. O’Sulllvan, H. Corby, V. Donnelly, C. O’Herlihy, P. R. O’Connell, T. Deignan, J. Kelly, N. P. Breslin, C. MacDonnell, J. O’Keeffe, K. Mills, U. Srinivasan, R. Willoughby, C. Feighery, B. Twohig, K. Gaynor, P. F. O’Regan, S. Duggan, H. P. Redmond, J. McCarthy, D. Bouchier-Hayes, Q. Y. Ma, K. E. Williamson, B. J. Rowlands, A. Tobin, R. Pilkington, M. O’Donnell, E. O’Shea, A. Conroy, G. Kaminski, A. Walsh, I. J. Temperley, D. Kelleher, D. G. Weir, M. K. Barry, E. D. Mulligan, M. A. Stokes, M. G. O’Riordain, T. F. Gorey, K. F. McGeeney, J. M. Fitzpatrick, R. W. G. Watson, J. H. Wang, F. Campbell, D. Bennett, E. Kavanagh, P. O. Gorman, P. O’Regan, M. M. I. Yassin, M. McCaigue, T. G. Parks, A. A. B. Barros D’Sa, M. Lawlor, S. McElwaine, M. A. Heneghan, M. Kerins, J. Goulding, E. L. Egan, F. M. Stevens, C. F. McCarthy, M. Quirke, A. M. Eustace-Ryan, S. Qureshi, E. Aziz, A. Maree, S. Collins, T. Browne, S. Ahmed, B. O. Sullibhan, P. Smith, F. Walker, F. O’Connor, E. Sweeney, R. J. Farrell, M. Morrint, M. Goggins, and J. G. McNulty

Subjects
medicine.medical_specialty, Irish, business.industry, Ophthalmology, language, medicine, Library science, General Medicine, business, language.human_language
Published
1995
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15. Irish Society of Gastroenterology

Author

P. K. Neelamakam, E. Brazil, S. Attwood, O. Traynor, J. Yaqoob, M. I. Khan, D. O’Toole, N. Noonan, C. Carey, D. Kelleher, D. G. Weir, P. W. N. Keeling, D. Monahan, L. Cogan, R. Willoughby, J. Jackson, A. Whelan, C. Feighery, G. Z. Kaminski, A. Conroy, S. Dooley, N. A. Parfrey, P. McEneaney, C. O’Morain, J. P. McGrath, R. C. Stuart, J. Hill, P. J. Byrne, C. Timon, S. C. S. Chung, A. VanHasselt, T. P. J. Hennessy, D. Hamilton, D. Mulcahy, D. Walsh, C. Farrely, W. Tormey, J. Fielding, G. Watson, A. Cherukuri, M. Maloney, D. O. Toole, M. Corcoran, J. Coffey, F. Butt, D. McAvinchey, P. V. Delaney, G. J. Burke, S. Youngprapakorn, U. Srinivasan, N. Leonard, C. O’Farrelly, C. O. Morain, C. A. Whelan, E. Barry, C. Collins, P. Costello, C. O’Herlihy, D. P. O’Donoghue, C. Clabby, J. McCarthy, E. Kenny-Walsh, M. J. Whelton, M. Morrin, F. Khan, P. Delaney, J. O’Keeffe, K. Mills, M. A. Bennett, E. W. Kay, H. Mulcahy, M. Leader, D. T. Croke, X. G. Fan, I. Khan, S. Keating, C. Morrison, M. Buckley, F. M. O’Reilly, C. Darby, M. G. Courtney, G. M. Murphy, J. F. Fielding, C. J. O’Boyle, T. J. Boyle, K. Mulhall, M. J. Kerin, D. Courtney, D. S. Quill, H. F. Given, S. Kehoe, R. Quirke, R. B. Stephens, S. Norris, G. McEntee, J. Hegarty, C. Farrelly, D. Thottaparambil, R. Thomas, G. Houghton, S. Sachithanandan, A. Geoghegan, S. Doyle, C. McCaul, T. N. Walsh, R. Farrell, B. Gusau, M. S. O’Mahoney, S. AlBloushi, J. Sachithanandan, J. Walshe, M. Carmody, J. Donohoe, A. G. Shattock, N. Parfrey, S. Lynch, L. Madrigal, J. McEntee, R. Murphy, Z. Ahmed, M. Ryan, C. Montwill, A. Morgan, P. Smith, F. Walker, A. Murphy, M. Moloney, S. McGrath, E. Taraneweh, A. K. Bhatia, D. O’Keeffe, P. McCarthy, E. Rajan, S. Albloushi, B. O’ Farrell, A. Shattock, D. Kearney, J. Lee, F. Gleeson, B. McNamara, J. Cuffe, G. C. O’Sullivan, B. J. Harvey, B. Curran, E. Kay, L. Lawler, S. E. A. Attwood, G. Bourke, J. Hyland, W. A. Owens, C. M. Loughrey, J. A. McAleer, K. G. McManus, J. F. Dillon, F. C. Wong, T. C. N. Lo, K. H. Chan, J. N. Plevris, N. D. C. Finlayson, J. D. Miller, I. A. D. Bouchier, P. C. Hayes, S. V. Walsh, L. J. Egan, C. E. Connolly, F. M. Stevens, E. L. Egan, C. F. McCarthy, Q. Y. Ma, G. D. Magee, J. E. Ardill, K. D. Buchanan, B. J. Rowlands, P. McGettigan, R. Chan, B. O’ Shea, J. McManus, J. Feely, J. Donoghue, N. Fanning, J. Mathias, P. Gillen, W. A. Tanner, F. B. V. Keane, D. M. Campbell, V. Donnelly, D. O’Connell, M. Behan, P. R. O’Connell, C. S. Ko, K. Mealy, B. M. Gusau, M. Goggins, J. Yakoub, R. J. Farrell, and N. Mahmud

Subjects
medicine.medical_specialty, Irish, business.industry, Ophthalmology, medicine, language, Library science, General Medicine, business, language.human_language
Published
1995
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16. Irish society for rheumatology Proceedings of Annual General Meeting held 14th October, 1994 at St. James’s Hospital, Dublin 8

Author

Donald McCarthy, B. Mulcahy, D. McGonagle, E. Workman, Hugh Mulcahy, F. McEvoy, N. Hall, M. Abuzakouk, E. Jones, E. B. Casey, P. Costello, G. D. Wright, R. Lovis, C. D’Arrigo, J. O. Hunter, M. Martin, E. Murphy, M. M. Skelly, M. Callaghan, C. Adams, S. D. Roberts, R. Gibney, Jill J. F. Belch, D. Mulherin, M. Goodfield, Y. Lu, R. McKane, B. L. Hazleman, J. Jackson, John Cookson, F. Shanahan, Eva M Doherty, E. Mullan, Cliona O'Farrelly, D. Byrne, Oliver FitzGerald, D. Foley-Nolan, A. L. Bell, A. Coumbe, E. Mulligan, R. Ryan, E. Case, A. H. Isdale, C. McCreary, Fergal O'Gara, D. Brophy, W. Bottomley, J. Brereton, A. O’Brien, Karl Gaffney, G. Molloy, C. O’Connor, J. Candal Couto, J. Guerin, A. Isdale, M. B. Finch, D. McGonigle, M. Goggins, L. Hemyrick, S. O’Briain, Gerard Bury, D. McGonagal, M. McDermott, S. R. McCann, P. C. Buchan, T. Costigan, M. E. T. Roberts, R. Pope, Alex Whelan, H. A. Bird, H. Salha, M. O. McCarron, A. Murphy, R. Kavanagh, Dermot Kelleher, C. Feighery, J. Dunne, M. Molloy, H. C. Gooi, D. J. Veal, J. I. O’Riordan, Mark J. Phelan, P. Kane, A. J. Taggart, R. Hopkins, Robert B. Sim, E. Bresnihan, V. Wright, G. Kirk, A. Bell, Douglas J. Veale, D. L. Kastner, A. Long, J. Eustace, S. M. Sant, F. Waldron-Lynch, Margaret McLaren, D. G. Weir, P. Nash, S. Donnelly, Malcolm D. Smith, A. Saunders, D. Kilmartin, P. V. Gardiner, S. Blades, J. A. McNally, D. P. O’Donoghue, A. Taggart, D R Blake, I. N. Bruce, Barry Bresnihan, and A. M. Forde

Subjects
medicine.medical_specialty, Irish, business.industry, Internal medicine, Ophthalmology, language, medicine, Library science, General Medicine, business, language.human_language, Rheumatology
Published
1995
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17. National scientific medical meeting 1995 abstracts

Author

S. Norris, C. Collins, J. Hegarty, C. O’Farrelly, J. Carton, L. Madrigal, D. P. O’Donoghue, H. Holloway, J. F. Fielding, W. Mullins, S. W. Hone, M. Donnelly, F. Powell, A. W. Blayney, E. A. Cahill, S. F. Daly, M. J. Turner, P. A. Sullivan, M. McLoughlin, M. M. Skelly, H. E. Mulcahy, T. Connell, C. Duggan, M. J. Duffy, A. Troy, K. Sheahan, A. Whelan, C. M. Herra, C. T. Keane, H. Johnson, B. Lee, E. Doherty, T. McDonnell, D. Mulherin, O. FitzGerald, B. Bresnihan, H. M. Hassett, A. Boyce, V. Greig, C. O’Herlihy, P. P. A. Smyth, E. F. Roche, I. McCormack, E. Tempany, M. J. Cullen, D. F. Smith, Y. McBrinn, B. Murray, R. Freaney, D. Keating, M. J. McKenna, J. A. O’Hare, H. Alam, Q. Raza, M. Geoghegan, S. Killalea, M. Hall, J. Feely, L. Kyne, B. O’Hara, M. Cullen, I. M. Rea, J. P. Donnelly, R. W. Stout, P. Lacey, M. J. Donnelly, J. McGrath, T. P. Hennessy, C. V. I. Timon, D. Hyde, H. X. Xia, M. Buckley, C. O’Morain, S. Keating, H. Xia, J. P. McGrath, R. C. Stuart, P. Lawlor, P. J. Byrne, T. N. Walsh, T. P. J. Hennessy, M. Duffy, M. Tubridy, J. Redmond, K. Monahan, R. P. Murphy, D. R. Headon, T. O’Gorman, F. M. O’Reilly, C. Darby, G. M. Murphy, A. Murphy, M. Codd, P. Dervan, D. Lawlor, S. O. Loughlin, N. Flanagan, R. Watson, L. Barnes, C. Kilgallen, E. Sweeney, A. Mynes, D. Mooney, I. Donoghue, O. Browne, J. A. Kirrane, D. McKenna, M. Young, E. O’Toole, S. O’Briain, U. Srinivasan, C. Feighery, N. Leonard, E. Jones, M. A. Moloney, D. G. Weir, M. Lawler, A. O’Neill, H. Gowing, D. Pamphilon, S. R. McCann, G. O’Toole, A. Orren, C. M. Seifer, D. C. Crowley, G. J. Sheehan, T. Deignan, J. Kelly, V. J. Tormey, J. Faul, C. Leonard, C. M. Burke, L. W. Poulter, S. Lynch, G. McEntee, O. Traynor, E. Barry, P. Costello, A. Keavney, R. Willoughby, C. O’Donnell, M. Cahill, A. Earley, P. Eustace, R. Osborne, C. Saidlear, B. Holmes, A. Early, A. P. Moran, A. Neisser, R. J. Polt, H. Bernheimer, M. Kainz, B. Schwerer, L. Gallagher, R. Firth, N. Kennedy, E. McGilloway, N. Tubridy, K. Shields, W. K. Cullen, M. J. Rowan, A. R. Moore, M. Rowan, D. Coakley, B. Lawlor, G. Swanwick, R. Al-Naeemi, R. Murphy, N. M. Codd, M. Goggins, N. P. Kennedy, B. L. Mallon, H. Mulcahy, M. Skelly, D. O. Donoghue, D. McCarthy, A. Saunders, D. J. Veale, J. J. F. Belch, D. Breathnach, E. Murphy, G. Kernohan, K. Gibson, A. G. Wilson, G. W. Duff, N. de Vries, L. B. A. van de Putte, J. Donoghue, F. O’Kelly, Z. Johnson, T. Maher, A. Moran, C. Keane, D. O’Neill, N. Horgan, J. M. Barragry, D. M. Campbell, M. Behan, P. R. O’Connell, V. S. Donnelly, D. Crowley, M. Geary, P. Boylan, M. Fanagan, K. Hickey, T. Teoh, M. Doyle, R. Harrison, D. Lyons, Y. Shenouda, M. Coughlan, P. McKenna, P. Lenehan, M. Foley, P. Kelehan, P. Ravichandran, M. Kelly, A. Conroy, C. Fitzpatrick, D. Egan, C. L. Regan, B. V. McAdam, P. McParland, G. A. FitzGerald, D. J. Fitzgerald, S. C. Sharma, K. Foran, C. Barry-Kinsella, R. F. Harrison, F. J. Gillespie, P. O’Mahony, M. Boyle, M. J. White, F. Donohoe, Y. Birrane, M. Naughton, R. B. Fitzsimons, M. Piracha, S. McConkey, E. Griffin, E. Hayes, T. Clarke, N. Parfrey, K. Butler, A. J. Malone, P. J. Kearney, P. F. Duggan, A. Lane, R. Keville, M. Turner, S. Barry, D. Sloan, S. Gallagher, M. Darby, P. Galligan, J. Stack, N. Walsh, M. O’Sullivan, M. Fitzgerald, D. Meagher, S. Browne, C. Larkin, P. Casey, E. O’Callaghan, S. Rooney, E. Walsh, M. Morris, T. Burke, M. Roe, C. Maher, M. Wrigley, M. Gill, M. Burgess, E. Corcoran, D. Walsh, B. Gilmer, C. B. Hayes, L. Thornton, J. Fogarty, R. Lyons, M. O’Connor, V. Delaney, K. Buckley, D. Lillis, V. Delany, C. Hayes, P. Dack, D. Igoe, H. J. O’Neill, P. Kelly, D. McKeown, L. Clancy, G. Varghese, S. Hennessy, J. J. Gilmartin, K. Birthistle, D. Carrington, H. Maguire, P. Atkinson, C. Foley-Nolan, M. Lynch, B. Cryan, D. Whyte, C. Conlon, V. Kucinskas, U. Usinskiene, I. Sakalyte, E. Dawson, K. Molloy, N. Goulden, J. Doyle, E. Lawlor, M. G. Harrington, N. El-Nageh, M. -L. Nolan, J. O’Riordan, G. Judge, G. Crotty, T. Finch, M. Borton, T. Barnes, O. Gilligan, G. Lee, R. Limmer, M. Madden, C. Bergin, A. O’Leary, F. Mulcahy, F. Wallis, M. Glennon, M. Cormican, U. NiRiain, M. Heiginbothom, F. Gannon, T. Smith, C. O’Sullivan, R. Hone, D. A. Caugant, C. A. P. Fijen, E. J. Van Schalkwyk, G. J. Coetzee, U. Ni Riain, M. G. Cormican, L. Park, J. Flynn, V. Regazzoli, M. Hayes, G. Nicholson, P. Higgins, N. Flynn, G. Corbett-Feeney, D. J. Conway, N. J. O’Higgins, S. Rajendiran, J. Byrne, E. Kilfeather, P. Dingle, M. Hunter, S. K. Al-Ghazal, P. Stanley, J. Palmer, A. Hong, P. Saxby, D. Sheehan, I. Regan, J. O’Mullane, M. Ni Chaoimh, M. Leahy, J. J. Heffron, M. Lehane, C. Keohane, N. O’Leary, M. Sheehan, E. Renny-Walsh, M. J. Whelton, C. T. Doyle, J. Webster, N. Benjamin, S. FitzGerald, J. S. Chadha, M. G. FitzGerald, G. R. FitzGerald, L. Hemeryck, P. McGettigan, J. Golden, N. Arthur, S. Y. Wen, P. Deegan, T. Cooke, G. I. Adebayo, P. Gaffney, M. Sinnot, D. O’Riordan, T. Hayes, C. M. O’Connor, M. X. FitzGerald, C. Costello, G. Finlay, J. Hayes, C. O’Connor, K. McMahon, S. Hone, J. Robertson, R. Coakley, S. O’Neill, M. Walsh, J. McCarthy, D. Lannon, A. E. Wood, R. Sharkey, E. Mulloy, M. Long, I. Kilgallen, V. Tormey, S. Horne, T. Feeney, Ó. Ó Muiré, M. J. Griffin, D. Hughes, A. Knaggs, D. Magee, C. McCrory, B. March, D. Phelan, M. White, J. Fabry, D. Buggy, C. Cooney, E. Aziz, D. O’Keefe, A. J. McShane, J. Boylan, E. Tobin, C. Motherway, F. Colreavy, N. Denish, R. Dwyer, A. Bergin, K. O’Brien, R. MacSullivan, K. D. Carson, W. P. Blunnie, D. C. Moriarty, B. Kinirons, B. Lyons, N. Cregg, W. Casey, K. P. Moore, S. A. Colbert, C. Ecoffey, D. O’Gorman, J. Fitzgerald, P. Diamond, M. B. Codd, D. D. Sugrue, J. Kellett, M. Tighe, C. J. McKenna, J. Galvin, H. A. McCann, A. Scallon, A. Fraser, M. Norton, G. Tomkin, I. Graham, A. Byrne, M. Maher, N. Moran, D. Fitzgerald, D. O’Callaghan, D. Coyle, A. G. Nugent, C. McGurk, G. D. Johnston, A. Nugent, B. Silke, N. Murphy, L. Jennings, D. Pratico, C. Doyle, T. Hennessy, H. McCann, D. Sugrue, S. Donnelly, A. Hennessy, C. Hartigan, D. MacDonald, S. Blake, D. McDonald, D. Dominque, S. R. McMechan, G. MacKenzie, J. Allen, G. T. Wright, G. J. Dempsey, M. Crawley, J. Anderson, A. A. J. Adgey, M. T. Harbinson, N. P. S. Campbell, C. M. Wilson, P. K. Ellis, E. M. McIlrath, A. McShane, T. V. Keaveny, K. Rabenstein, F. Scheller, D. Pfeiffer, C. Urban, I. Moser, G. Jobst, A. Manz, S. Verpoorte, F. Dempsey, D. Diamond, M. Smyth, E. Dempsey, V. Hamilton, J. Twomey, R. Crowley, L. Fenelon, F. Walsh, J. McCann, P. McDonagh, E. McGovern, D. Luke, K. Crowley, D. Mannion, D. Murphy, K. Clarkson, E. Carton, I. Leonard, D. O’Toole, M. Staunton, M. Griffin, D. Owens, P. Collins, A. Johnson, G. H. Tomkin, N. A. Herity, J. D. Allen, R. O’Moore, G. M. Crotty, M. DeArce, K. Nikookam, P. Keenan, D. Cregan, N. O’Meara, S. Forman, D. A. Cusack, and B. Farrell

Subjects
medicine.medical_specialty, business.industry, Family medicine, medicine, MEDLINE, General Medicine, business
Published
1995
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18. Irish Society of Gastroenterology

Author

P. O’Gorman, Cormac T. Taylor, John M. Fitzpatrick, M. G. Goggins, M. Madden, J. F. Fielding, B. T. Johnston, P. W. N. Keeling, N. Kieran, B. Curran, M. Maloney, Michael J. Duffy, N. Couse, Thomas F. Gorey, J. G. McNulty, M. Buckley, A. G. Shattock, M. O’Reilly, Mary B. Codd, M. M. Skelly, X. J. Fan, Éanna J Ryan, W. Mullins, W. O. Kirwan, A. K. Cherukuri, J. P. McGrath, B. Golden, G. Lee, John Hyland, M. A. Stokes, Peter A. Dervan, Patrick J. Byrne, S. Al-Bloushi, H. Holloway, Diarmuid O'Donoghue, K. M. Murphy, S. McGrath, D. H. Osborne, N. I. McDougall, E. W. Kay, J. Lennon, D. O’Donovan, G. O'Sullivan, T. N. Walsh, Colm O'Morain, P. K. Ellis, C. Doyle, A. O’Farrell, A. P. Moran, J. K. Collins, T. Carroll, G. O. Sullivan, Ciaran O’Reilly, F. M. O’Reilly, F. Mulcahy, A. S. Browne, J. Kelly, I. Khan, C. Kanduru, Peter J. Kelly, A. Murphy, Michael G. Harrington, T. Deignan, T. C. K. Tham, A. Quinn, C. O. Farrelly, P. V. Delaney, N. M. Codd, M. Leader, J. Morgan, Gerald C. O'Sullivan, E. Casey, M. P. Ryan, M. A. Bennett, C. G. M. Gahan, A. Long, P. MacMathuna, T. V. McCarthy, Y. Sharifi, M. C. Regan, Fergus Shanahan, B. J. O’Farrell, F. O’Brien, G. S. A. McDonald, T. Mulcahy, T. P. J. Hennessy, E. Jones, Dermot Kelleher, M. G. Courtney, C. B. O. Suilleabhain, K. J. Farrell, E. Rajan, Evelyn P. Murphy, R. G. P. Watson, G. Burke, A. Kitching, E. Fitzgerald, Andrew H.G. Love, E. J. Walsh, Michael Kennedy, Alan W. Baird, Mohamed Abuzakouk, Prakash Madhavan, Sally Ann Lynch, Martin J. O’Sullivan, Simon Keely, W. J. Primrose, D. Maguire, X. G. Fan, M. Goggins, M. C. Prabhakar, Hugh Mulcahy, R. J. McFarland, Seamus Morris, G. Thornton, Colm Bergin, Donald G. Weir, G. J. McKee, Cliona O'Farrelly, D. Royston, P. Neary, D. A. Egan, J. O’Shea, C. Carey, R. Merriman, Frank Kee, L. English, D. P. O’Donoghue, R. W. G. Watson, S. O’Briain, E. Mulligan, S. Reid, P. Quinn, Richard J. Farrell, P. Horgan, T. Gorey, M. I. Khan, Brian J. Harvey, Jiang Huai Wang, Nicholas P. Kennedy, J. S. A. Collins, David Bouchier-Hayes, N. Noonan, J. Crowe, P. R. O'Connell, Henry Paul Redmond, E. M. Mcllrath, F. Khan, D. T. Crake, and C. Feighery

Subjects
medicine.medical_specialty, business.industry, Section (typography), Library science, General Medicine, Cork, engineering.material, language.human_language, Irish, Ophthalmology, language, medicine, engineering, business
Published
1994
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19. Interfacial layer development in hot-dip galvanneal coatings on interstitial free (IF) steel

Author

C. E. Jordan, K. M. Goggins, and Arnold R. Marder

Subjects
Materials science, Carbon steel, Annealing (metallurgy), Metallurgy, Alloy, Metals and Alloys, chemistry.chemical_element, Crystal growth, Zinc, engineering.material, Condensed Matter Physics, Galvanization, Galvannealed, symbols.namesake, Coating, chemistry, Mechanics of Materials, engineering, symbols
Abstract

During the annealing of hot-dip galvanized coatings on interstitial free (IF) steel, an interfacial layer was found to develop and grow at the steel/coating interface. The interfacial layer followed a three-step growth process in which there was initial rapid growth up to a thickness of approximately 1.0 µm, followed by a period of essentially no growth with continued zinc and iron interdiffusion into the coating, and finally renewed growth at long time (60 second) anneals. The interfacial layer did not inhibit zinc and iron interdiffusion or the development of the Fe-Zn alloy layer. Coating iron content increased rapidly before the interfacial layer grew to a thickness of 1.0 µm, however, once the coating reached a total iron content in excess of 11.0 wt pct, interfacial layer growth became active and coating iron content increased only slightly with continued annealing. Although powdering of the coating as evaluated by a 60 deg bend test was generally found to increase with an increase in interfacial layer thickness, particularly in excess of 1.0 µm, no definitive relationship between interfacial layer thickness and powdering was found. The thickness of this interfacial layer, however, can be used as an indicator of formability performance.

Published
1994
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20. National Scientific Medical Meeting 1994 Abstracts

Author

M. J. Turner, J. Upton, T. P. J. Hennessy, P. Kelehan, A. D. Crockard, Paul A. McGettigan, M. Grouden, Y. A. Cusack, Catherine Curran, B. Cryan, C. Pidgeon, T. G. Cooke, E. Shorten, B. M. Kinsella, P. Sweeney, A. Southey, S. G. Richardson, M. Sheehan, E. R. Horwitz, J. Belch, E. Griffin, E. Healy, A. Oakhill, H. Johnson, P. Shah, A. Kinsella, P. A O’Connell, P. Humphries, P. Lenehan, S. Fanning, C. N. Pidgeon, D. Pamphilon, M. T. P. Caldwell, B. Tuohy, P. Dack, J. Murphy, P. Gaffney, Fiona M. Stevens, C. Bergin, A. Locasciulli, G. Nolan, M. Kearns, D. F. Smith, J. P. H. Fee, I. Reid, Muiris X. Fitzgerald, T. Cawley, G. Swanwick, U. Kondaveeti, F. Davidson, A. Early, D. Noone, S. Farrell, A. Hale, C. M. Costello, L. English, Colm O'Herlihy, B. Crowley, J. F. Lyons, P. Kent, D. Coakley, M. Geary, L. J. Egan, M. Hogan, G. A. FitzGerald, P. White, R. Merriman, Mary Leader, M. Fitzgerald, N. AlAnsari, H. P. Singh, N. Mahmud, Sarah Rogers, T. Conlon, J. O’Shea, C. Larkin, Norman Delanty, L. Maguire, J. Mahady, J. T. Ennis, E. Creamer, R. P. Kernan, I. Temperley, M. Hargrove, J. Joseph Walshe, J. M. T. Redmond, B. Gilmer, Michael Hutchinson, J. Woof, K. D. Carson, C. Darby, D. Lyons, Michael T. Dawson, G. Gibson, A. B. Atkinson, J. A. Lawson, N. Ryall, D. S. O’Briain, R. Pilkington, W. Blunnie, T. Donoghue, D. M. O’Hanlon, S. Coulter-Smith, James R. Docherty, G. Mortimer, Enda W. McDermott, C. Conlon, T. Cooke, B. Hennelly, P. Boylan, P. Lawlor, S. Young, B. Marsh, R. J. Cunney, S. Lynch, W. O’Connor, M. C. Prabhakar, G. Dempsey, C. Fitzpatrick, L. Boissel, P. O’Callaghan, Terry J. Smith, B. P. McMahon, F. M. Ryan, D. Allcut, Sinead O’Neill, Emer Shelley, M. Coca-Prados, J. Lawson, E. G. Smyth, J. Geraghty, C. A. Whelan, M. Goggins, R.J. Cunney, B. McGeeney, A. J. Cunningham, P. Eustace, K. Carson, B. Sheridan, D. Powell, C. Foley-Nolan, P. M. Byrne, L. Barnes, G. King, C. Cullen, Maria A. O'Connell, Shaun Gallagher, G. J. Fitzpatrick, J. Mulhall, M. G. Mott, E. Shanahan, S. Murphy, D. Buggy, Cliona O'Farrelly, M. Buckley, T. M. Murray, G. McQuoid, D. O’Riordain, P. M. Bell, P. McNamara, P. Byrne, M. P. Colgan, S. Hone, T. J. McKenna, R. McManus, D. O’Neill, M. R. N. Darling, Aaj Adgey, P. Campbell, T. Finch, M. Robson, H. C. Loughrey, P. Foster, C. O’Keane, G. I. Adebayo, J. McEnri, J. D. Allen, Martin Cormican, C. Timon, E. O’Mongain, V. S. Donnelly, E. Corcoran, J. J. Gilmartin, M.J. Duffy, Brian J. Harvey, Peter P.A. Smyth, J. O. L DeLancey, Desmond J. Fitzgerald, J. Wang, T. Larkin, C. Barry-Kinsella, T. O’Connell, E. O’Callaghan, A Jefferson, G. D. Johnston, N. Shepard, A. L. Kennedy, I. M. Rea, C. F. McCarthy, D. Kerr, Margaret McLaren, G. Z. Kaminski, Hugh Staunton, P. Grainger, M. Norton, F. Lavin, B. F. McAdam, M. Maguire, R. Rafferty, M. Caldwell, R. Hone, C. M. MacDonagh-White, Dermot Kelleher, R. Namushi, G. MacKenzie, Michael J. Kerin, James Bernard Walsh, Mark Lawler, A. K. Cherukuri, U. Fearon, M. Doran, S. Orwa, J. Liu, N. Al fnAnsari, A. P. Heaney, K. Tipton, M. Glennon, H. Grimes, S. Hamilton, C. Smith, C. M. Kilgallen, Thomas Barry, R. Horgan, C. Saidtéar, V. Urbach, A. B. P. Cullinane, M. A. Christie, K. Daly, L. Madrigal, D. R. Hadden, C. McCreary, Q. Razza, Catherine Hayes, T. Walsh, T. Clarke, E. T. Burke, S. Liston, D. Mulherin, M. P. Reilly, D. Tansey, N. Cannon, V. P. Coffey, A. A. El-Magbri, D. P. O’Donoghue, P. W. N. Keeling, Jack Phillips, L. Condren, Jill J. F. Belch, J. R. Anderson, B. McAdam, Reza Mofidi, F. Hegarty, J. Kavanagh, Frances J. Hayes, D. Murray, E. Holmes, J. Fenton, J. Strattan, G. D. Wright, D. H. Hill, H. G. Nelson, A. C. Moloney, J. Goh, C. S. McArdle, G. Loughrey, J. Phillips, J. Fennell, T. Aherne, J. Stronge, S. Lewis, Kieran Sheahan, T. Markham, Madeline Murphy, P. J. Byrne, B. Harding, R. Hitchcock, M. Bourke, J. McSweeney, K. Colgan, Z. Johnson, D. Cotter, R. F. Harrison, Patricia Fitzpatrick, J. Feely, J. Crowe, H. F. Given, A. Mofidi, M. Hynes, E. B. McNamara, Michael J. Turner, T. Woods, Blánaid Hayes, J. Tyrrell, E. O’Toole, G. G. Lavery, A. M. Deveney, A. J. McShane, O. Bradley, B. Blackwood, O. White, L. W. Poulter, H. Maguire, E. S. Prosser, N. Dowd, Michael Kennedy, Peter J. Kelly, John J. O'Leary, K. Hickey, B. C. Morrow, P. Oslizlok, Malachi J. McKenna, J. Fabry, R. Chander, D. Clarke, C. O’Sullivan, M. O’Reilly, M. M. Young, F. Abuaisha, Clare O'Connor, N. A. Herity, J. Toland, D. Buckley, G. Kirk, E. Maguire, Cecily Kelleher, I. Hillary, H. D. Alexander, R. Keimowitz, L. H. Murray, S. Hennessy, D. Whyte, K. Holmes, M. S. Robson, J. Stratton, Conor T. Keane, B. Kanagaratnam, A. Heffernan, J. Golden, Anthony O'Grady, A. Tobin, J. I. O’Riordan, D. Sloan, Niall O'Higgins, A. Vance, A. Foot, B. Murphy, F. Mulvany, P. C. Sham, J. Higgins, P. M. Mercer, G. Browne, Y. Young, H. J. Gallagher, Thomas F. Gorey, A. Lane, Nollaig A. Parfrey, P. R. O’Connell, J. O’Neill, J. Adgey, Z. Imam, R. O’Sullivan, D. Maguire, L. Thornton, L. Drury, Douglas J. Veale, M. Reilly, M. Eljamel, A. W. Murphy, J. Laundon, M. Reidy, E. Ryan, A. Bacigalupo, C. O’Shaughnessy, B. Silke, R. A. Greene, J. P. McGrath, Connail McCrory, C. T. Keane, S. McMechan, J. Strangeways, T. O’Gorman, Malcolm D. Smith, M. Madden, G. Nicholson, B. O’Shea, A. McCann, M. Foley, G. Gearty, J. Hosseini, R. O’Moore, A. Taylor, A. M. Hetherton, Elizabeth Smyth, John V. Reynolds, J. A. B. Keogh, John Bonnar, D. Cafferty, D. Graham, J. R. Lennon, Barry Bresnihan, B. Denham, R. Holliman, M. B. O’Connor, Y. K. Tay, Padraic MacMathuna, M. S. Eljamel, H. Osborne, G. Shanik, S. M. Lavelle, R. Watson, Premkumar, M. Byrne, Fionnuala M. McAuliffe, S. Sharif, S. Killalea, E. Zimmermann, K. Kengasu, D. Duff, A. Hickey, D. McShane, J. Fogarty, M. Geoghegan, G. O’Reilly, T. Scott, P. Killeen, T. Kinsella, E. McIlrath, Helen M. Byrne, M. Borton, R. A. Rusk, J. M. McGinley, P. L. Yeoh, D. Warde, R. Stanwell-Smith, John Newell, M. Greer, David J. Brayden, E. M. Lavelle, C. D’Arrigo, J. McManus, R. Gonsalves, Barbara Murray, P. Murphy, G. D’Arcy, Camillus K. Power, N. Hughes, P. M. E. McCormack, R. Dwyer, N. Iman, R. B. Fitzsimons, S. C. Sharma, M. Carmody, Stewart R. Walsh, Gillian M. Murphy, E. McGuinness, L. Kevin, E. Barrett, S. K. Cunningham, A. Orren, S. Ni Scanaill, Karl Gaffney, P. McCormack, M. Martin, J. Malone, E. L. Egan, M. J. Walshe, D. Walsh, S. Kaf Al-Ghazal, M. Kuliszewski, S. Blankson, J. R. Sutherst, M. Lynch, M. T. Thornton, I. Boylan, Fiona Mulcahy, Oliver FitzGerald, T. N. Walsh, Y. Wen, K. McQuaid, D. R. McCance, M. Hall, U. Ni Riain, J. Hollyer, Michael Walsh, J. Donohoe, J. Doherty, D. Carney, D. J. Moore, S. E. Lawlor, K. Birthistle, H. S. Khoo Tan, A. M. Powell, G. Boyle, C. Burke, D. Veale, E. Lawlor, L. Zimmerman, M. Stewart, L. Hemeryck, Conor Burke, Irene B. Hillary, A. Pooransingh, K. Butler, P. W. Johnston, Daniel Rawluk, N. Foreman, M. J. Conran, B. L. Sheppard, P. Gilligan, D. Keane, E. Mulligan, D. Phelan, J. G. Kelly, J. Stack, Y. McBrinn, E. Sweeney, S. Calvert, E. A. Maguire, E. Keane, D. McKeogh, M. Post, S. N. Tham, P. Connolly, A. C. Gordon, Frank Gannon, Rosemarie Freaney, C. Collins, J. F. Malone, B. Moule, C. Saidlear, Seamus Sreenan, S. Teahan, J. McCann, J. Dixon, C. Quigley, J. L. Waddington, D. Maher, I. Graham, Diarmaid Hughes, S. Thomas, A. O’Leary, K. Carroll, A. M. Bourke, J. Candal Couto, N. Nolan, R. Harper, D. P. O’Brien, T. C. M. Morris, E. O’Leary, Michael M. Maher, M. White, C. Hallahan, N. Ni Scannlain, Colm O'Morain, E. Hayes, Luke Clancy, B. Stuart, P. Crean, J. Dowling, I. Cree, M. A. Heneghan, B. Cassidy, C. A. Barnes, Donald G. Weir, J. Flynn, E. Clarke, J. Stinson, N. Gardiner, R. Mulcahy, B. J. Harvey, Gerald C. O'Sullivan, G. S. A. McDonald, P. Costigan, P. O’Connor, D. Carrington, J. Goulding, C. Sheehan, A. Kitching, Conleth Feighery, M. LaFoy, E. Coleman, S. Pathmakanthan, C. Condon, S. B. Grimes, J. M. O’Donoghue, J. Hildebrand, Gerard Bury, A. W. Clare, S. Feely, S. R. McCann, J. A. O’Hare, B. E. Kelly, A. Moloney, M. Donnelly, D. O’Meara, and A. Chan

Subjects
medicine.medical_specialty, business.industry, Family medicine, Human immunodeficiency virus (HIV), Medicine, General Medicine, business, medicine.disease_cause
Published
1994
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21. Irish society for rheumatology

Author

Diarmuid Mulherin, Oliver FitzGerald, Barry Bresnihan, I. N. Bruce, J. A. McNally, A. L. Bell, G. Yanni, A. Cauli, S. Challacombe, G. S. Panayi, D. Foley-Nolan, M. Akil, M. Anthony, D. Cundall, J. Bourne, R. Arthur, M. A. Chamberlain, P. Byrne, N. Mahon, H. Robinson, S. M. Sant, S. Donnelly, L. Barnes, R. Watson, E. B. Casey, D. E. Edgar, S. A. McMillan, S. K. Conlan, T. A. McNeill, M. Abuzakouk, C. Feighery, E. Jones, S. O’Briain, M. Goggins, D. G. Weir, E. Casey, C. O’Farrelly, D. Kelleher, A. Murphy, D. J. Veale, G. Kirk, M. McLaren, J. J. F. Belch, M. J. Daly, J. Murphy, M. Lynch, S. McKernan, R. Sothinathan, C. Blake, M. Garrett, I. S. Gourley, B. Bresnihan, O. FitzGerald, G. Cunnane, C. Bergin, A. Cherukuri, D. Mulherin, N. Hall, B. Mulcahy, M. Molloy, M. Phelan, F. O’Gara, F. McConnell, F. Shanahan, M. Heffernan, and P. Neary

Subjects
medicine.medical_specialty, Irish, business.industry, Rheumatoid arthritis, Family medicine, Internal medicine, medicine, language, General Medicine, medicine.disease, business, language.human_language, Rheumatology
Published
1994
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22. Epidemiology

Author

B. Fixa, O. Komárková, K. Krejsek, J. Bures, Z. Nozicka, W. Giorcelli, M. Rodi, G. Camisasca, R. G. Martinotti, M. A. Mendall, P. M. Goggin, Nicola Molineaux, Joanne Levy, T. Toosy, D. Strachan, T. C. Northfield, T. Vorobjova, V. Vassiljev, K. Kisand, T. Wadström, R. Uibo, R. B. Zotz, S. G. Xu, G. von Recklinghausen, P. Meusers, H. Goebell, K. H Rhee, H. S. Youn, S. K. Paik, W. K. Lee, M. J. Cho, C. K. Park, Yuyuan Li, Pinjin Hu, Guoguang Du, Zhijin Wong, Stuart L. Hazell, Hazel M. Mitchell, J. D. de Korwin, P. Remot, Ph Hartemann, A. Catelle, M. C. Conroy, J. Schmitt, M. Stolte, E. Wellens, B. Bethke, M. Ritter, H. Eidt, S. Veldhuyzen van Zanten, L. Best, G. Bezanson, T. Marrie, E. Poniewierka, G. Gosciniak, T. Matysiak-Budnik, M. Quatrini, F. Boni, A. R. Baldassarri, A. De Vecchi, C. Castelnovo, E. Viganò, L. Tenconi, P. A. Bianchi, A. Carlucci, G. Ferrini, I Bianco, G. Larcinese, A. Di Sciascio, G. F. Fly, T. Hauge, J. Persson, L. G. V. Coelho, M. M. Teixeira, M. C. F. Passos, C. B. Givisiez, C. M. F. R. Santos, C. J. S. Rodrigues, Y. Chausson, L. P. Castro, Hannu Hyvärinen, Kari Seppälä, Eero Kivilaakso, Timo Kosunen, Martin Gormse, A. Pilotto, F. Vianello, D. Tornaboni, P. Dotto, G. Battaglia, F. Binda, F. Di Mario, P. M. Donisi, M. Pasini, M. E. Benve-nuti, V. Stracca-Pansa, M. Pasquino, H. Jablonowski, H. Szelényi, K. J. Hengels, G. Strohmeyer, N. Banatvala, K. Mayo, F. Megraud, R. Jennings, J. J. Deeks, R. A. Feldman, G. Bulighin, A. Ederie, S. Pilati, G. Franzin, G. Zamboni, M. Maran, R. Musola, A. Tobin, R. C. Hackman, G. B. McDonald, N. Fatela, J. Melo Cristino, L. Monteiro, F. Ramalho, A. Saragoça, M. J. Salgado, M. Cameiro de Moura, S. Pretolani, G. Gasbarrini, F. Bonvicini, M. Baraldini, E. Tonelli, M. R. A. Gatto, G. C. Ghironzi, F. M égraud, S. Bouchard, W. Lubcvzumiska-Kowalska, Z. Knapik, J. Meenan, M. Goggins, C. Shahi, P. W. N. Keeling, C. Keane, D. G. Weir, D. Vaira, M. Miglioli, P. Mulè, J. Holten, M. Menegati, G. Biasco, M. Vergura, A. Nannetti, L. Barbara, A. Boschini, M. Begnini, M. Menegatti, C. Ghira, A. D’Errico, D. G. Evans, M. A. Asnicar, D. J. Evans, D. Y. Graham, C. H. Lee, M. Coschieri, T. Fosse, M. C. St. Paul, J. R. Michiels, J. P. Delmont, J. L. Péroux, C. Pradier, P. Rampai, P. Pazzi, A. Merighi, S. Gamberini, R. Scarliarini, R. Bicochi, M. Libanore, G. Bisi, and S. Gulllini

Subjects
General Medicine
Published
1992
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23. Pathology of incipient pancreatic cancer

Author

Ralph H. Hruban, Robb E. Wilentz, G. J. A. Offerhaus, Charles J. Yeo, Scott E. Kern, and M. Goggins

Subjects
Pathology, medicine.medical_specialty, Pancreatic disease, Tumor suppressor gene, business.industry, Hematology, Hyperplasia, medicine.disease_cause, medicine.disease, Lesion, medicine.anatomical_structure, Oncology, Pancreatic cancer, medicine, Cancer research, Carcinoma, medicine.symptom, Carcinogenesis, business, Pancreas
Abstract

Background: An understanding ofincipient pancreatic neoplasia is an essential foundation for the future development of effective screening tests for pancreatic cancer. Only when we understand early pancreatic neoplasms will we be able to detect tumors that are curable with surgical resection. Method: Two approaches have helped define incipient pancreatic neoplasia. First, the histologic examination of pancreata has helped identify the most common histologic lesions in pancreatic tissues adjacent to infiltrating carcinomas. The assumption is that some of these lesions represent the precursors to the infiltrating cancers. Second, advances in molecular genetics now make it possible to define the genetic alterations present in small lesions. The demonstration that a suspected precursor lesion and an infiltrating pancreatic carcinoma share the same genetic alterations would help establish that the lesion is indeed a precursor to infiltrating pancreatic carcinoma.

Published
1999
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25. Genetics of the FANCA gene in familial pancreatic cancer

Author

Gloria M. Petersen, Kathleen M. Murphy, M. Goggins, S. T. Martin, Kieran Brune, F J Couch, Juliet Philips, Ralph H. Hruban, Charles J. Yeo, and Carmelle D Rogers

Subjects
Male, Colorectal cancer, Population, DNA Mutational Analysis, Heteroduplex Analysis, Gene mutation, Biology, Breast cancer, Pancreatic tumor, FANCG, Pancreatic cancer, Genetics, medicine, Humans, Genetic Predisposition to Disease, education, Genetics (clinical), Aged, education.field_of_study, Fanconi Anemia Complementation Group A Protein, DNA, Neoplasm, Sequence Analysis, DNA, Middle Aged, medicine.disease, FANCA, DNA-Binding Proteins, Pancreatic Neoplasms, Mutation, Female, Online Mutation Report
Abstract

Fanconi anaemia (FA) is a rare autosomal recessive disease that is characterised by bone marrow failure, pancytopenia, and an increased susceptibility to cancers. Recently, D’Andrea and coworkers identified biallelic BRCA2 gene mutations as a cause of FA.1 Because of the role of BRCA2 gene mutations in pancreatic cancer development, their findings suggested other members of the FA pathway may be targeted for genetic inactivation in pancreatic cancer. Indeed, somatic and inherited mutations of FANCC and somatic mutations in FANCG were subsequently identified in patients with apparently sporadic pancreatic cancer.2 These data led to analysis of the FANCC and FANCG genes in the germline of families with multiple pancreatic cancers, but no mutations were identified.3 In most populations, FANCA is the most commonly mutated gene in patients with FA.4–14 In this study we determined if FANCA gene mutations predispose to the development of familial pancreatic cancer. ### Subjects Lymphocyte DNA was analysed from patients with familial pancreatic cancer enrolled in the National Familial Pancreatic Tumor Registry.15 Patients with pancreatic cancer were selected if they had at least two or more first degree relatives with pancreatic cancer (mean (SD) age of 66.7 (12.3) years, males 50.3%). Variants were analysed in 110 additional patients with familial pancreatic cancer. To determine the carrier frequency of c.2574C>G (p.Ser868Arg), we analysed three control populations: healthy spouses of patients with familial pancreatic cancer (115 samples from spouses with a mean (SD) age of 66.9 (11.3) years, males 43.1%), patients who had undergone cholecystectomy (65 samples matched in age with sporadic cases) for non-malignant disease at Johns Hopkins Hospital, and individuals undergoing routine screening colonoscopy (668 samples) at the Mayo Clinic. The mean age of the colonoscopy controls was similar to our pancreatic cancer population (mean (SD) age of 59.3 (12.3) years, males 52.9%). …

Published
2004

26. The dichotomy in the preinvasive neoplasia to invasive carcinoma sequence in the pancreas: differential expression of MUC1 and MUC2 supports the existence of two separate pathways of carcinogenesis

Author

Kambiz Merati, Robb E. Wilentz, Daniel S. Longnecker, Ralph H. Hruban, David S. Klimstra, M. Goggins, N. Volkan Adsay, Aleodor A. Andea, Fazlul H. Sarkar, and Christine A. Iocobuzio-Donahue

Subjects
Pathology, medicine.medical_specialty, Mucin 2, Biology, digestive system, Pathology and Forensic Medicine, Immunoenzyme Techniques, medicine, Carcinoma, Biomarkers, Tumor, Humans, MUC1, Mucin-2, Intraductal papillary mucinous neoplasm, Mucin, Mucin-1, Mucins, medicine.disease, digestive system diseases, Pancreatic Neoplasms, medicine.anatomical_structure, Dysplasia, Immunohistochemistry, Pancreas, Carcinoma in Situ, Carcinoma, Pancreatic Ductal
Abstract

Emerging evidence suggests a dichotomy in the dysplasia-CIS-invasive carcinoma sequence in the pancreas. Pancreatic intraepithelial neoplasms (PanINs; small, incidental duct lesions) progress to invasive ductal adenocarcinomas (5-y survival of15%), whereas intraductal papillary mucinous neoplasms (large, intraductal tumors with ductal dilatation) are often associated with colloid carcinoma (5-y survival of55%). We explored the relationship of these lesions by examining the expression of MUC1 and MUC2, glycoproteins reportedly reflecting "aggressive" and "indolent" phenotypes in pancreas cancer, respectively. Immunohistochemical labeling with MUC1 (clone Ma695) and MUC2 (clone Ccp58) antibodies was performed on PanINs (n = 43), intraductal papillary mucinous neoplasms (n = 74), ductal adenocarcinomas (n = 136), and colloid carcinomas (n = 15). Fifty-four percent of the intraductal papillary mucinous neoplasms expressed MUC2, whereas none of the PanINs did. In contrast, PanINs, especially higher grade lesions, were often positive for MUC1 (61% of PanIN 3), whereas the expression of this glycoprotein was infrequent in intraductal papillary mucinous neoplasms (20%). This dichotomy was further accentuated in the invasive carcinomas with which these two preinvasive pathways are respectively associated: all colloid carcinomas were MUC2+ (100%) and MUC1- (0%), whereas the labeling pattern was the reverse for ductal adenocarcinomas: 63% were MUC1+ and only 1% were MUC2+. These results support a dichotomy in the dysplasia-CIS sequence in the pancreas. Because these two pathways often lead to different types of invasive carcinomas, this is an invaluable model for the study of carcinogenesis. The findings here also support the previous impression that MUC2 (the mucin associated with gel formation) is a marker of the "indolent" pathway (intraductal papillary mucinous neoplasm and colloid carcinoma), whereas MUC1 (the glycoprotein known to have an inhibitory role in cell-cell and cell-stroma interactions as well as in immunoresistance of tumor cells) is a marker of the "aggressive" pathway (PanIN to ductal adenocarcinoma).

Published
2002

27. Immunohistochemical labeling for the Dpc4 gene product is a specific marker for adenocarcinoma in biopsy specimens of the pancreas and bile duct

Author

M. Goggins, G. J. A. Offerhaus, Pedram Argani, M. Tascilar, Ralph H. Hruban, Renee Altink, Robb E. Wilentz, John L. Cameron, T. A. Sohn, Charles J. Yeo, and Other departments

Subjects
Male, medicine.medical_specialty, Pathology, Pancreatic disease, Biology, Adenocarcinoma, Gastroenterology, Gene product, Bile Ducts, Extrahepatic, Internal medicine, Biopsy, medicine, Carcinoma, Biomarkers, Tumor, Humans, Fluorescent Antibody Technique, Indirect, Aged, Smad4 Protein, medicine.diagnostic_test, Bile duct, Reproducibility of Results, General Medicine, Middle Aged, medicine.disease, digestive system diseases, Neoplasm Proteins, DNA-Binding Proteins, Pancreatic Neoplasms, medicine.anatomical_structure, Bile Duct Neoplasms, Trans-Activators, Immunohistochemistry, Female, Pancreas
Abstract

We immunohistochemically labeled 72 biopsy specimens from the extrahepatic biliary tree and pancreas for Dpc4 protein and correlated expression with histologic diagnosis and patient follow-up. Specimens were classified histologically as follows: nonneoplastic, 35; neoplastic, 22; atypical, 15. Loss of expression of Dpc4 protein was identified in 12 specimens; 11 were histologically diagnostic of carcinoma. The 12th specimen was from a patient whose biopsy specimen initially was diagnosed as "atypical," but clinical follow-up revealed adenocarcinoma. Of the 12 atypical biopsy specimens with intact expression for Dpc4, follow-up later revealed that 10 were adenocarcinoma. Loss of expression of Dpc4 protein was never identified in a benign specimen. Immunohistochemical labeling for the Dpc4 gene product is a specific marker of carcinoma in biopsy specimens of the pancreas and extrahepatic bile ducts and is marginally helpful in classifying atypical specimens. The sensitivity for carcinoma is low. This latter finding is not unexpected, because the DPC4 tumor suppressor gene is inactivated in only about half of pancreatic and biliary malignant neoplasms. Importantly, loss of Dpc4 expression has been reported in in situ carcinomas, suggesting that loss of expression should not be equated with invasive carcinoma.

Published
2002

28. Identification and characterization of differentially methylated CpG islands in pancreatic carcinoma

Author

T, Ueki, M, Toyota, H, Skinner, K M, Walter, C J, Yeo, J P, Issa, R H, Hruban, and M, Goggins

Subjects
Adult, Aged, 80 and over, Antimetabolites, Antineoplastic, Cyclin G1, Reverse Transcriptase Polymerase Chain Reaction, Enkephalins, Adenocarcinoma, DNA Methylation, Middle Aged, Cyclin G, Pancreatic Neoplasms, Cyclins, Azacitidine, Humans, CpG Islands, Protein Precursors, Aged, Microsatellite Repeats
Abstract

To identify CpG islands differentially methylated in pancreatic adenocarcinoma, we used methylated CpG island amplification (MCA) coupled with representational difference analysis. Of 42 CpG islands identified by MCA/representational difference analysis, 7 CpG islands [methylated in carcinoma of the pancreas (MICP)] were differentially methylated in a panel of eight pancreatic cancer cell lines compared with normal pancreas. In a larger panel of 75 pancreatic adenocarcinomas, these 7 MICPs (ppENK, Cyclin G, ZBP, MICP25, 27, 36, and 38) were methylated in 93, 3, 9, 15, 48, 19, and 41% of cancers, respectively, by methylation-specific PCR but not in any of 15 normal pancreata. In pancreatic cancer cell lines, methylation of ppENK, a gene with known growth suppressive properties, was associated with transcriptional silencing that was reversible with 5-aza-2'-deoxycytidine treatment. Relationships between the methylation patterns of pancreatic adenocarcinomas and their clinicopathological features were also determined. Larger pancreatic cancers and those from older patients (P = 0.017) harbored more methylated loci than smaller tumors and those from younger patients (P = 0.017). ppENK, MICP25, and 27 were variably methylated in normal gastric, duodenal, and colonic mucosae. These data indicate that aberrant methylation of ppENK and its transcriptional repression is a common event in pancreatic carcinogenesis.

Published
2001

29. Molecular pathology of pancreatic cancer

Author

R H, Hruban, C, Iacobuzio-Donahue, R E, Wilentz, M, Goggins, and S E, Kern

Subjects
Pancreatic Neoplasms, Humans, Genes, Tumor Suppressor, Oncogenes, DNA, Mitochondrial
Abstract

Until recently, pancreatic cancer was a poorly understood disease. Research in the past decade has shown conclusively, however, that pancreatic cancer is primarily genetic in nature. Inactivation with a variety of tumor-suppressor genes such as p16, DPC4, and p53, coupled with activation of oncogenes such as K-ras, are a few of the mutations that trigger the growth of cancerous cells. Understanding these mutations is critical to a better understanding of familial pancreatic cancer and to the development of gene-based screening tests and therapies. In this article, we review the genetic alterations identified in pancreatic cancer and provide examples of how this information can be applied to patient care.

Published
2001

30. Familial pancreatic cancer

Author

A P, Klein, R H, Hruban, K A, Brune, G M, Petersen, and M, Goggins

Subjects
BRCA2 Protein, Male, Pancreatic Neoplasms, Neoplastic Syndromes, Hereditary, Risk Factors, Odds Ratio, Humans, Family, Female, Genetic Predisposition to Disease, Registries, Biomarkers, Cyclin-Dependent Kinase Inhibitor p16, Germ-Line Mutation, Genes, Dominant
Abstract

Pancreatic cancer is the fourth leading cause of cancer death in both men and women in the United States and will be responsible for an estimated 28,900 deaths in 2001. Relatively little is known of its etiology, and the only well-established risk factor is cigarette smoking. Studies over the past 3 decades have shown that 4%-16% of patients with pancreatic cancer have a family history of the disease. A small fraction of this aggregation can be accounted for in inherited cancer syndromes, including familial atypical multiple-mole melanoma, Peutz-Jeghers syndrome, hereditary breast-ovarian cancer, hereditary pancreatitis, and hereditary nonpolyposis colorectal cancer. These syndromes arise as a result of germline mutations in the BRCA2, pl6 (familial atypical multiple-mole melanoma), mismatch repair (hereditary nonpolyposis colorectal cancer), and STK11 (Peutz-Jeghers syndrome) genes. In addition, hereditary plays a role in predisposing certain patients with apparently sporadic pancreatic cancer. Many patients with pancreatic cancers caused by a germline mutation in a cancer-causing gene do not have a pedigree that is suggestive of a familial cancer syndrome. A recent prospective analysis of the pedigrees in the National Familial Pancreatic Tumor Registry found that individuals with a family history of pancreatic cancer in multiple first-degree relatives have a high risk of pancreatic cancer themselves. The identification of such high-risk individuals will help clinicians target screening programs and develop preventive interventions with the hope of reducing the mortality of pancreatic cancer in these families.

Published
2001

31. Increased risk of incident pancreatic cancer among first-degree relatives of patients with familial pancreatic cancer

Author

A C, Tersmette, G M, Petersen, G J, Offerhaus, F C, Falatko, K A, Brune, M, Goggins, E, Rozenblum, R E, Wilentz, C J, Yeo, J L, Cameron, S E, Kern, and R H, Hruban

Subjects
Family Health, Male, Pancreatic Neoplasms, Risk, Models, Statistical, Time Factors, Age Factors, Humans, Female, Registries, Middle Aged, Aged
Abstract

It has been estimated that familial aggregation and genetic susceptibility play a role in as many as 10% of patients with pancreatic cancer (PC). The quantified prospective risk of PC among first-degree relatives of PC patients has not been investigated. Families enrolled in the National Familial Pancreas Tumor Registry (NFPTR) prior to September 1, 1998 were followed to estimate the risk and incidence of PC among first-degree relatives of patients with PC. Analyses were performed separately on kindreds with at least two first-degree relatives with PC (familial pancreatic carcinoma (PC); n = 150) at the time the kindred was enrolled in the NFPTR and on kindreds without a pair of affected first-degree relatives (sporadic PC; n = 191). A subanalysis was performed on familial PC kindreds containing three or more affected members at the time of enrollment in the NFPTR (n = 52). Risk was estimated by comparing observed new cases of PC during the observation period with expected numbers based on the United States population-based Surveillance, Epidemiology and End Results program data. Incidence was estimated using person-years risk analyses. During the observational period, six incident PCs developed in the first-degree relatives: two in the sporadic PC kindreds, and four in the familial PC kindreds. The PC risk in the sporadic PC kindreds was not significantly greater than expected [observed/expected = 6.5 (95% CI = 0.78-23.3)] with an incidence rate of 24.5/10(5)/ year. There was a significantly increased 18-fold risk (95% CI = 4.74-44.5) of PC among first-degree relatives in familial PC kindreds, with an incidence of 76.0/10(5)/year. In the subset of familial PC kindreds with three or more affected family members at the time of enrollment, there was a 57-fold (95% CI = 12.4-175) increased risk of PC and an incidence of 301.4/10(5)/year compared with the Surveillance, Epidemiology and End Result age-adjusted incidence of PC in the U.S. (8.8/10(5)/year). When stratified by age, the risk was largely confined to relatives over the age of 60. This study is the first analysis of incident PC occurring in familial PC kindreds. The risk and incidence of PC is exceptionally high among at-risk first-degree relatives in familial PC kindreds in which at least three first-degree relatives have already been diagnosed with PC. Familial PC kindreds are a reasonable high-risk group for PC screening and chemoprevention research.

Published
2001

33. Progression model for pancreatic cancer

Author

R H, Hruban, M, Goggins, J, Parsons, and S E, Kern

Subjects
Pancreatic Neoplasms, Disease Progression, Humans, Carcinoma, Pancreatic Ductal
Published
2000

34. Genetic, immunohistochemical, and clinical features of medullary carcinoma of the pancreas: A newly described and characterized entity

Author

R E, Wilentz, M, Goggins, M, Redston, V A, Marcus, N V, Adsay, T A, Sohn, S S, Kadkol, C J, Yeo, M, Choti, M, Zahurak, K, Johnson, M, Tascilar, G J, Offerhaus, R H, Hruban, and S E, Kern

Subjects
Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Epstein-Barr Virus Infections, Herpesvirus 4, Human, Proto-Oncogene Proteins, Humans, neoplasms, Pancreas, In Situ Hybridization, Adaptor Proteins, Signal Transducing, Aged, Aged, 80 and over, Family Health, nutritional and metabolic diseases, Nuclear Proteins, Middle Aged, Immunohistochemistry, Survival Analysis, digestive system diseases, Neoplasm Proteins, DNA-Binding Proteins, Pancreatic Neoplasms, Genes, ras, MutS Homolog 2 Protein, Phenotype, Carcinoma, Medullary, Multivariate Analysis, Mutation, RNA, Viral, Female, Carrier Proteins, MutL Protein Homolog 1, Microsatellite Repeats, Regular Articles
Abstract

Medullary carcinomas of the pancreas are a recently described, histologically distinct subset of poorly differentiated adenocarcinomas that may have a unique pathogenesis and clinical course. To further evaluate these neoplasms, we studied genetic, pathological, and clinical features of 13 newly identified medullary carcinomas of the pancreas. Nine (69%) of these had wild-type K-ras genes, and one had microsatellite instability (MSI). This MSI medullary carcinoma, along with three previously reported MSI medullary carcinomas, were examined immunohistochemically for Mlh1 and Msh2 expression, and all four expressed Msh2 but did not express Mlh1. In contrast, all of the medullary carcinomas without MSI expressed both Msh2 and Mlh1. Remarkably, the MSI medullary carcinoma of the pancreas in the present series arose in a patient with a synchronous but histologically distinct cecal carcinoma that also had MSI and did not express Mlh1. The synchronous occurrence of two MSI carcinomas suggests an inherited basis for the development of these carcinomas. Indeed, the medullary phenotype, irrespective of MSI, was highly associated with a family history of cancer in first-degree relatives (P < 0.001). Finally, one medullary carcinoma with lymphoepithelioma-like features contained Epstein-Barr virus-encoded RNA-1 by in situ hybridization. Therefore, because of medullary carcinoma’s special genetic, immunohistochemical, and clinical features, recognition of the medullary variant of pancreatic adenocarcinoma is important. Only by classifying medullary carcinoma as special subset of adenocarcinoma can we hope to further elucidate its unique pathogenesis.

Published
2000

35. BRCA2 is inactivated late in the development of pancreatic intraepithelial neoplasia: evidence and implications

Author

M, Goggins, R H, Hruban, and S E, Kern

Subjects
BRCA2 Protein, Pancreatic Neoplasms, Genes, ras, endocrine system diseases, DNA Mutational Analysis, Mutation, Humans, Loss of Heterozygosity, DNA, Neoplasm, Carcinoma in Situ, Neoplasm Proteins, Transcription Factors, Regular Articles
Abstract

Patients harboring germline BRCA2 mutations are at an increased risk of developing pancreatic cancer. We investigated the prevalence of biallelic inactivation of BRCA2 in the presumed precursors to invasive pancreatic ductal carcinomas, pancreatic intraepithelial neoplasia (PanIN). Surgical resection specimens from three patients with germline BRCA2 mutations who developed pancreatic ductal adenocarcinoma were studied. Fourteen PanINs were needle-microdissected from paraffin-embedded tissue. DNA was isolated from these microdissected tissues and amplified by primer-mediated pre-amplification. Loss of heterozygosity at the BRCA2 locus was determined by polymerase chain reaction amplification and cycle sequencing. The presence of the wild-type alleles was evaluated at the nucleotide positions of the germline BRCA2 mutations. The K-ras gene was sequenced at codon 12 and 13 to confirm the efficacy of microdissection. By histological evaluation the prevalence of PanINs in these patients was not notably elevated. Loss of the wild-type allele of BRCA2 was present in one high-grade PanIN (PanIN 3), but in none of 13 low-grade PanINs (PanIN 1). In contrast, K-ras mutations were detectable in 7 of the 14 PanINs. These results suggest that biallelic inactivation of the BRCA2 gene is a relatively late event in pancreatic tumorigenesis. In contrast to classical molecular progression models of tumorigenesis, the inactivation of the wild-type allele in a carrier of a recessive tumor susceptibility gene may not always be the first somatic event during the molecular evolution of a cancer. The necessity for earlier genetic alterations before biallelic inactivation of a recessive tumor susceptibility gene such as BRCA2 may explain why affected carriers have normal numbers of neoplastic precursor lesions, a relatively low phenotypic penetrance, and late age of onset of pancreatic and other cancers.

Published
2000

36. Hypermethylation of multiple genes in pancreatic adenocarcinoma

Author

T, Ueki, M, Toyota, T, Sohn, C J, Yeo, J P, Issa, R H, Hruban, and M, Goggins

Subjects
Tissue Inhibitor of Metalloproteinase-3, Receptors, Retinoic Acid, Transplantation, Heterologous, Adenocarcinoma, DNA Methylation, Pancreatic Neoplasms, Calcium Channels, T-Type, Death-Associated Protein Kinases, O(6)-Methylguanine-DNA Methyltransferase, Calcium-Calmodulin-Dependent Protein Kinases, Humans, Apoptosis Regulatory Proteins, Promoter Regions, Genetic, Thrombospondins, Pancreas, Dinucleoside Phosphates
Abstract

Hypermethylation of CpG islands is a common mechanism by which tumor suppressor genes are inactivated. We studied 45 pancreatic carcinomas and 14 normal pancreata for aberrant DNA methylation of CpG islands of multiple genes and clones using methylation-specific PCR (MSP) and bisulfite-modified sequencing. Using MSP, we detected aberrant methylation of at least one locus in 60% of carcinomas. The genes analyzed included RARbeta (methylated in 20%), p16 (18%), CACNA1G (16%), TIMP-3 (11%), E-cad (7%), THBS1 (7%), hMLH1 (4%), DAP kinase (2%), and MGMT (0%). In addition, aberrant methylation was found in three CpG islands (MINT31, -1, and -2) in 38, 38, and 14% of carcinomas, respectively. Hypermethylation was largely confined to the carcinomas with only three loci (E-cad, DAP kinase, and MINT2) harboring methylation in some normal pancreata (36, 21, and 14%, respectively). Simultaneous methylation of at least four loci was observed in 5 of 36 (14%) pancreatic adenocarcinomas. We defined this subgroup of pancreatic adenocarcinomas as "CpG island-methylator-phenotype positive (CIMP+)." Two of four carcinomas with microsatellite instability harbored promoter hypermethylation of hMLH1, and both cases were CIMP+. Thus, we conclude that many pancreatic carcinomas hypermethylate a small percentage of genes, whereas a subset displays a CIMP+ phenotype.

Published
2000

37. Pathology of incipient pancreatic cancer

Author

R H, Hruban, R E, Wilentz, M, Goggins, G J, Offerhaus, C J, Yeo, and S E, Kern

Subjects
BRCA2 Protein, Pancreatic Neoplasms, Genes, ras, Genes, p16, Humans, Genes, p53, Neoplasm Proteins, Transcription Factors
Abstract

An understanding of incipient pancreatic neoplasia is an essential foundation for the future development of effective screening tests for pancreatic cancer. Only when we understand early pancreatic neoplasms will we be able to detect tumors that are curable with surgical resection.Two approaches have helped define incipient pancreatic neoplasia. First, the histologic examination of pancreata has helped identify the most common histologic lesions in pancreatic tissues adjacent to infiltrating carcinomas. The assumption is that some of these lesions represent the precursors to the infiltrating cancers. Second, advances in molecular genetics now make it possible to define the genetic alterations present in small lesions. The demonstration that a suspected precursor lesion and an infiltrating pancreatic carcinoma share the same genetic alterations would help establish that the lesion is indeed a precursor to infiltrating pancreatic carcinoma.A spectrum of intraductal proliferations in the pancreas has been found associated with infiltrating adenocarcinoma of the pancreas. These lesions, called "duct lesions," have even been identified in pancreata years before patients develop infiltrating carcinoma. Molecular genetic analysis of these lesions has revealed that they frequently harbor many of the same alterations present in infiltrating carcinoma of the pancreas. These alterations include activation of K-ras and inactivation of p16, p53 and, rarely BRCA2.From these morphologic and molecular observations, we can now develop a progression model for the development of infiltrating carcinoma of the pancreas. Infiltrating carcinomas of the pancreas may arise from pancreatic duct lesions, and the progression of duct lesions to infiltrating cancer is associated with the accumulation of generalized and specific genetic alterations.

Published
1999

38. Familial pancreatic cancer

Author

R H, Hruban, G M, Petersen, M, Goggins, A C, Tersmette, G J, Offerhaus, F, Falatko, C J, Yeo, and S E, Kern

Subjects
BRCA2 Protein, Pancreatic Neoplasms, Genes, p16, Humans, Breast Neoplasms, Female, Colorectal Neoplasms, Hereditary Nonpolyposis, Dysplastic Nevus Syndrome, Neoplasm Proteins, Transcription Factors
Abstract

For many years anecdotal case reports have suggested that pancreatic cancer aggregates in some families.Two recent advances have established that this is in fact the case. First, large registries, such as the National Familial Pancreas Tumor Registry (NFPTR) at Johns Hopkins, have identified a number of families in which multiple family members have been diagnosed with pancreatic cancer. As a result, the patterns of inheritance of pancreatic cancer can now be studied on a scale not possible before. Second, advances in molecular genetic techniques make it possible to test members of these families for germline mutations in known candidate cancer causing genes. As a result, some of the genetic alterations responsible for the familial aggregation of pancreatic cancer have been identified in some families.The NFPTR has enrolled 362 families in which at least one family member has been diagnosed with pancreatic cancer. These include 151 families in which at least two first-degree relatives have been diagnosed with pancreatic cancer. Analysis of these families has revealed that even second-degree relatives of patients from these families are at increased risk of developing pancreatic cancer. In addition, a number of kindreds which exhibit aggregation of cancer have been tested for germline mutations in known cancer causing genes. Germline mutations in BRCA2 have been shown to predispose to both breast and pancreatic cancer, germline mutations in p16 to melanoma and pancreatic cancer (the FAMMM syndrome), and genetic mutations in STK11/LKB1 to pancreatic cancer in patients with the Peutz-Jeghers Syndrome (PJS).Pancreatic cancer aggregates in some families, and relatives of patients with pancreatic cancer have an increased risk of developing pancreatic cancer themselves. The genetic basis for the familial aggregation of pancreatic cancer has been shown to be germline mutations in known cancer causing genes in some of these families.

Published
1999

39. Progress in cancer genetics: lessons from pancreatic cancer

Author

M, Goggins, S E, Kern, J A, Offerhaus, and R H, Hruban

Subjects
Chromosome Aberrations, Pancreatic Neoplasms, Genes, ras, DNA Repair, Humans, Genes, Tumor Suppressor, DNA Methylation
Abstract

In the near future advances in the molecular basis of cancer are expected to facilitate cancer diagnosis, to rationalize treatment, to facilitate screening, and to identify individuals requiring cancer prevention strategies.The literature was reviewed concerning the genetic alterations that contribute to pancreatic cancer development.Virtually all pancreatic cancers have inactivation of the p16 pathway, and the majority inactivate the TGF beta/DPC4 and p53 tumor-suppressive pathways. Pancreatic cancers with mismatch repair deficiency have a characteristic histology and may have an improved prognosis. The recently discovered tumor suppressor genes, ALK-5, MKK4, and STK11 (the gene responsible for Peutz-Jeghers syndrome) are all targeted for mutation in a small proportion of sporadic pancreatic cancers. Germline mutations of the BRCA2 gene are present in 5-10% of patients with pancreatic cancer. Typically such patients do not have a family history of pancreatic cancer and are mistaken as patients with sporadic disease. Five to 10% of patients with pancreatic cancer have first-degree relatives that will develop pancreatic cancer. Some such families also have a family history of melanoma and harbor germline p16 mutations. However, the gene(s) responsible for much of the inherited predisposition to pancreatic cancer remain to be identified.Further advances in pancreatic cancer molecular genetics are needed to facilitate the development of molecular screening tests, to identify additional familial susceptibility genes, and to identify targets for rational therapeutic targeting.

Published
1999

40. Role of tumor markers and mutations in cells and pancreatic juice in the diagnosis of pancreatic cancer

Author

M, Tascilar, E, Caspers, P D, Sturm, M, Goggins, R H, Hruban, and G J, Offerhaus

Subjects
Pancreatic Neoplasms, Genes, ras, DNA Repair, Genes, p16, Mutation, Biomarkers, Tumor, Humans
Abstract

Unresectability at the time of presentation is the most important reason for the poor survival rate of pancreatic carcinoma. Molecular-based tests might improve the early detection of pancreatic cancer at a time when surgical resection is still an option for cure.The literature was reviewed concerning the role of molecular-based tests applied to sources other than pancreatic tissue itself, including ERCP-samples, blood and stool, with emphasis on the detection of K-ras mutations and mutant p53 gene product.K-ras mutations have been successfully detected in ERCP brush samples, leading to an increase of the sensitivity and improvement of the diagnostic yield. When pancreatic juice and duodenal fluid are tested for K-ras mutations, the yield is less. K-ras mutations can also be detected in the blood, especially in patients with larger tumors. The presence of K-ras mutations proved also to be useful in discriminating benign and malignant liver nodules, i.e. when during surgery there is suspicion of liver metastases of pancreatic cancer. The accumulation of p53 gene product to immunochemically detectable levels in ERCP brush samples also increases the sensitivity of conventional light microscopy. Other molecular markers such as telomerase and TIMP-1 may prove to be useful too, but await more extensive evaluation.Molecular-based tests may be of value in the early detection of pancreatic cancer and might therefore contribute to a better patient survival rate.

Published
1999

41. Transplantation without maintenance corticosteroids in 1-haplotype and 2-haplotype HLA matched living-related renal transplant recipients treated with mycophenolate mofetil and cyclosporine

Author

M. Goggins, K. K. Venkat, M. Mozes, W. Kupin, Marwan S Abouljoud, F Escobar, and V Douzdjian

Subjects
medicine.drug_class, medicine.medical_treatment, Human leukocyte antigen, Mycophenolate, Adrenal Cortex Hormones, Azathioprine, medicine, Living Donors, Humans, Family, Transplantation, Chemotherapy, Kidney, business.industry, Histocompatibility Testing, Haplotype, Mycophenolic Acid, Ciclosporin, Kidney Transplantation, medicine.anatomical_structure, Haplotypes, Immunology, Cyclosporine, Corticosteroid, Surgery, Drug Therapy, Combination, business, Immunosuppressive Agents, medicine.drug
Published
1999

42. Genetic alterations of the transforming growth factor beta receptor genes in pancreatic and biliary adenocarcinomas

Author

M, Goggins, M, Shekher, K, Turnacioglu, C J, Yeo, R H, Hruban, and S E, Kern

Subjects
Male, Activin Receptors, Genes, p16, Carcinoma, Ductal, Breast, Receptor, Transforming Growth Factor-beta Type II, Loss of Heterozygosity, Adenocarcinoma, Middle Aged, Protein Serine-Threonine Kinases, DNA-Binding Proteins, Pancreatic Neoplasms, Biliary Tract Neoplasms, Transforming Growth Factor beta, Mutation, Trans-Activators, Humans, Female, Receptors, Transforming Growth Factor beta, Aged, Smad4 Protein
Abstract

Transforming growth factor beta (TGF-beta) is an extracellular ligand that binds to a heterodimeric receptor, initiating signals that regulate growth, differentiation, and apoptosis. Many cancers, including pancreatic cancer, harbor defects in TGF-beta signaling and are resistant to TGF-beta-mediated growth suppression. Genetic alterations of DPC4, which encodes a DNA binding protein that is a downstream component of the pathway, most frequently occur in pancreatic and biliary carcinomas. We searched for other targets of mutation of the TGF-beta pathway in these cancers. We report somatic alterations of the TGF-beta type I receptor gene ALK-5. Homozygous deletions of ALK-5 were identified in 1 of 97 pancreatic and 1 of 12 biliary adenocarcinomas. A germ-line variant of ALK-5, presumably a polymorphism, was identified, but no somatic intragenic mutations were identified upon sequencing of all coding regions of ALK-5. Somatic alterations of the TGF-beta type II receptor gene (TGFBR2) were identified in 4 of 97 (4.1%) pancreas cancers, including a homozygous deletion in a replication error-negative cancer and three homozygous frameshift mutations of the poly(A) tract of the TGF-beta type II receptor in replication error-positive cancers. We also studied other related type I receptors of the TGF-beta superfamily. In a panel of pancreas cancers preselected for loss of heterozygosity at the ALK-1 locus, sequencing of all coding exons of the ALK-1 gene revealed no alterations. No homozygous deletions were detected in the ALK-1, ALK-2, ALK-3, or ALK-6 genes in a panel of 86 pancreatic cancer xenografts and 11 pancreatic cancer and 22 breast cancer cell lines. The rate of genetic inactivation of TGF-beta pathway members was determined in 45 pancreatic cancers. Eighty-two % of these pancreatic cancers had genetic inactivation of the DPC4, p15, ALK-5, or TGFBR2 genes. Our results indicate that the TGF-beta type I and type II receptor genes are selective targets of genetic inactivation in pancreatic and biliary cancers.

Published
1998

43. Inactivation of the p16 (INK4A) tumor-suppressor gene in pancreatic duct lesions: loss of intranuclear expression

Author

R E, Wilentz, J, Geradts, R, Maynard, G J, Offerhaus, M, Kang, M, Goggins, C J, Yeo, S E, Kern, and R H, Hruban

Subjects
Pancreatic Neoplasms, Genes, p16, Humans, Genes, Tumor Suppressor, Adenocarcinoma, Pancreas
Abstract

Pancreatic adenocarcinoma develops from histologically identifiable intraductal lesions that undergo a series of architectural, cytological, and genetic changes. Limited genetic evidence recently suggested that the p16 gene plays a role in the progression of these "duct lesions." Duct lesions were identified in pancreata from 33 pancreaticoduodenectomies performed for infiltrating adenocarcinoma. All of these infiltrating adenocarcinomas were previously shown to contain alterations in the p16 gene or its promoter. Monoclonal and polyclonal anti-p16 antibodies were used for histological immunodetection. One hundred twenty-six duct lesions were identified. Nine (30%) of 30 flat, 4 (27%) of 15 papillary, 37 (55%) of 67 papillary with atypia, and 10 (71%) of 14 carcinoma in situ duct lesions showed loss of p16 expression. These included 30% of the flat lesions versus 53% of the nonflat lesions and 29% of the nonatypical lesions versus 58% of the atypical lesions. For both comparisons, the differences were statistically significant (P = 0.036 and P = 0.003, respectively). Loss of p16 expression occurs more frequently, but not exclusively, in higher-grade duct lesions. These data support the hypothesis that pancreatic duct lesions are neoplastic and that they represent the precursors of infiltrating adenocarcinoma. Immunohistochemical detection of p16 provides a new technology to study the genetic alterations in and stages of progression of large numbers of morphologically defined pancreatic duct lesions.

Published
1998

44. Pancreatic adenocarcinomas with DNA replication errors (RER+) are associated with wild-type K-ras and characteristic histopathology. Poor differentiation, a syncytial growth pattern, and pushing borders suggest RER+

Author

M, Goggins, G J, Offerhaus, W, Hilgers, C A, Griffin, M, Shekher, D, Tang, T A, Sohn, C J, Yeo, S E, Kern, and R H, Hruban

Subjects
Adult, Aged, 80 and over, DNA Replication, Male, DNA, Neoplasm, Adenocarcinoma, Middle Aged, Immunohistochemistry, Pancreatic Neoplasms, Genes, ras, Karyotyping, Humans, Keratins, Female, Aged, Microsatellite Repeats, Research Article
Abstract

The clinical and pathological features of carcinomas of the pancreas with DNA replication errors (RER+) have not been characterized. Eighty-two xenografted carcinomas of the pancreas were screened for DNA replication errors using polymerase chain reaction amplification of microsatellite markers. Cases with microsatellite instability in at least two markers of a minimum of five tested were considered RER+. RER status was correlated with histological appearance, karyotype of the carcinomas when available, K-ras mutational status, and patient outcome. Three (3.7%) of the eighty-two carcinomas were RER+. In contrast to typical gland-forming adenocarcinomas of the pancreas, all three RER+ carcinomas were poorly differentiated and had expanding borders and a prominent syncytial growth pattern. Neither a Crohn's-like lymphoid infiltrate nor extracellular mucin production were prominent. Ductal adenocarcinomas of the pancreas typically contain a mutant K-ras gene, yet all three RER+ carcinomas had wild-type K-ras. One of the three RER+ carcinomas was karyotyped and showed a near diploid pattern. All three of the RER+ tumors were removed via Whipple resection. One of the three patients is free of disease 16 months after pancreaticoduodenectomy, one is alive and free of tumor at 52 months but developed two colon carcinomas during this period, and the third died of pancreatic cancer at 4 months. None of the three patients had a family history of colorectal carcinoma. A review of the K-ras wild-type carcinomas in a previously characterized series of pancreatic carcinomas with known K-ras mutational status identified two additional cancers with poor differentiation, a syncytial growth pattern, and pushing borders. Both of the cancers were diploid and both patients were longterm survivors (over 5 years). The inclusion of such patients in previous prognostic studies of pancreas cancer may explain the failure of histological grade to be a predictor of prognosis. These data suggest that DNA replication errors occur in a small percentage of resected carcinomas of the pancreas and that wild-type K-ras gene status and a medullary phenotype characterized by poor differentiation, and expanding pattern of invasion, and syncytial growth should suggest the possibility of DNA replication errors in carcinomas of the pancreas.

Published
1998

45. Analysis of PTEN/MMAC1 alterations in aerodigestive tract tumors

Author

K, Okami, L, Wu, G, Riggins, P, Cairns, M, Goggins, E, Evron, N, Halachmi, S A, Ahrendt, A L, Reed, W, Hilgers, S E, Kern, W M, Koch, D, Sidransky, and J, Jen

Subjects
Lung Neoplasms, Chromosomes, Human, Pair 10, Tumor Suppressor Proteins, DNA Mutational Analysis, Transplantation, Heterologous, PTEN Phosphohydrolase, Loss of Heterozygosity, DNA, Neoplasm, Digestive System Neoplasms, Phosphoric Monoester Hydrolases, Neoplasm Proteins, Pancreatic Neoplasms, Head and Neck Neoplasms, Carcinoma, Non-Small-Cell Lung, Carcinoma, Squamous Cell, Humans, Protein Tyrosine Phosphatases, Gene Deletion, Neoplasm Transplantation, Microsatellite Repeats
Abstract

PTEN/MMAC1 is a candidate tumor suppressor gene recently identified at chromosomal band 10q23. It is mutated in sporadic brain, breast, and prostate cancer and in the germ line of patients with hereditary Cowden disease. We searched for genetic alterations of the PTEN/MMAC1 gene in 39 primary head and neck cancers (HNSCCs), 42 primary non-small cell lung cancers (NSCLCs), 80 pancreatic cancer xenografts, and 37 cell lines and xenografts from colon, lung, and gastric cancers. Microsatellite analysis revealed loss of heterozygosity at markers near the gene in 41% of primary HNSCCs, 50% of NSCLCs, and 39% of the pancreatic cancers. Three cases of HNSCCs displayed homozygous deletion involving the gene. We sequenced the entire coding region of the PTEN/MMAC1 gene in the remaining tumors displaying loss of heterozygosity and found one terminating mutation in a HNSCC sample. Thus, a second inactivation event was observed in 4 of 39 primary HNSCC cases. By use of a protein truncation assay, one terminating mutation was also identified in one of eight NSCLC cell lines. Our results suggest that PTEN/MMAC1 gene inactivation plays a role in the genesis of some tumor types.

Published
1998

46. Tumor-suppressive pathways in pancreatic carcinoma

Author

E, Rozenblum, M, Schutte, M, Goggins, S A, Hahn, S, Panzer, M, Zahurak, S N, Goodman, T A, Sohn, R H, Hruban, C J, Yeo, and S E, Kern

Subjects
BRCA2 Protein, Male, Heterozygote, DNA Mutational Analysis, DNA, Neoplasm, Adenocarcinoma, Genes, p53, Neoplasm Proteins, DNA-Binding Proteins, Pancreatic Neoplasms, Genes, ras, Trans-Activators, Humans, Female, Genes, Tumor Suppressor, Carrier Proteins, Cyclin-Dependent Kinase Inhibitor p16, Sequence Deletion, Smad4 Protein, Transcription Factors
Abstract

During tumorigenesis, positive selection is exerted upon those tumor cells that alter rate-limiting regulatory pathways. A corollary of this principle is that mutation of one gene abrogates the need for alteration of another gene in the same pathway and also that the coexistence in a single tumor of mutations in different genes implies their involvement in distinct tumor-suppressive pathways. We studied 42 pancreatic adenocarcinomas for genetic alterations in the K-ras oncogene and the p16, p53, and DPC4 tumor suppressor genes. All of them had the K-ras gene mutated. Thirty-eight % of the tumors had four altered genes, another 38% had three altered genes, 15% had two altered genes, and 8% of the tumors had one altered gene. Interestingly, we noted a high concordance of DPC4 and p16 inactivations (P = 0.007), suggesting that the genetic inactivation of p16 increases the selective advantage of subsequent mutation in DPC4. No statistically significant association was identified between the alteration of these cancer genes and pathological or clinical parameters. This type of multigenic analysis in human tumors may serve to substantiate experimental tumor models and thus increase our understanding of the truly physiologically relevant tumor-suppressive pathways that are abrogated during human tumorigenesis.

Published
1997

47. Separate risk factors for the development of transplant glomerulopathy vs chronic tubulointerstitial rejection

Author

M. Lee, F Escobar, Marwan S Abouljoud, Raouf E. Nakhleh, K. K. Venkat, M. Goggins, W Kupin, and M. Mozes

Subjects
Graft Rejection, Male, medicine.medical_specialty, Nephrotic Syndrome, Time Factors, Body Surface Area, Kidney Glomerulus, Kidney, Gastroenterology, Risk Factors, Internal medicine, medicine, Humans, Risk factor, Kidney transplantation, Transplantation, Proteinuria, business.industry, Histocompatibility Testing, Glomerulonephritis, Transplant glomerulopathy, medicine.disease, Kidney Transplantation, Tissue Donors, Surgery, Creatinine, Female, medicine.symptom, business, Nephrotic syndrome, Immunosuppressive Agents, Kidney disease, Follow-Up Studies
Published
1997

48. Germline BRCA2 gene mutations in patients with apparently sporadic pancreatic carcinomas

Author

M, Goggins, M, Schutte, J, Lu, C A, Moskaluk, C L, Weinstein, G M, Petersen, C J, Yeo, C E, Jackson, H T, Lynch, R H, Hruban, and S E, Kern

Subjects
Adult, BRCA2 Protein, Male, Heterozygote, DNA Mutational Analysis, DNA, Neoplasm, Adenocarcinoma, Neoplasm Proteins, Pancreaticoduodenectomy, Pancreatic Neoplasms, Jews, Tumor Cells, Cultured, Humans, Female, Codon, Pancreas, Alleles, Sequence Deletion, Transcription Factors
Abstract

Germline mutations in BRCA2 predispose carriers to the development of breast, ovarian, and a variety of other cancers. The original localization of the BRCA2 gene was aided by its homozygous deletion in a pancreatic carcinoma; indeed, an excess of pancreatic carcinoma has been seen in some BRCA2 cancer families. To determine the involvement of BRCA2 in pancreatic carcinomas, we screened for BRCA2 alterations in an unselected panel of 41 adenocarcinomas of the pancreas (30 pancreatic adenocarcinoma xenografts and 11 pancreatic cancer cell lines). Of the 15 (27%) that had allelic loss at the BRCA2 locus, 4 (9.8%) had abnormalities in the second allele upon screening of the entire BRCA2 gene by in vitro synthesized protein assay. Three of the four mutations were considered germline in origin (7.3% overall; two were confirmed in normal tissue, and one was the 6174delT mutation from the pancreatic cancer cell line CAPAN-1, for which normal tissue was unavailable). The identification of two 6174delT mutations in this series prompted us to evaluate the prevalence of this mutation in an overlapping consecutive series of 245 patients who underwent pancreatoduodenectomy for adenocarcinoma of the pancreas. Sequence analysis of this limited region of the gene identified two additional mutations: (a) one additional germline 6174delT mutation (2 of 245, 0.8% overall); and (b) a second nearby germline 6158insT mutation. One of the patients with a germline mutation had a single relative with breast cancer, and another had a single relative with prostate cancer. None had a family history of pancreatic cancer. The incidence of germline BRCA2 mutations in apparently sporadic pancreatic cancer may be at least as high as in breast or ovarian cancer. Our results suggest that some familial risks for carcinoma will be evident only through a population-based application of gene screening techniques because a low disease penetrance of the germline mutations in some families often evades clinical suspicion.

Published
1996

49. The immunology of coeliac disease

Author

M, Goggins, A, Whelan, and D, Kelleher

Subjects
Major Histocompatibility Complex, Celiac Disease, Genetic Linkage, HLA Antigens, Humans
Published
1996

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