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105. Osteopontin expression in lung cancer

Author

Chambers, Ann F., primary, Wilson, Sylvia M., additional, Kerkvliet, Nancy, additional, O'Malley, Frances P., additional, Harris, John F., additional, and Casson, Alan G., additional

Published
1996
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119. Loss of imprinting of the insulin-like growth factor II (IGF2) gene in esophageal normal and adenocarcinoma tissues.

Author

Ronghua Zhao, De Coteau, John F., Geyer, C. Ronald, Mei Gao, Hengmi Cui, and Casson, Alan G.

Subjects
GENOMIC imprinting, GENE expression, TUMORS, EPITHELIAL cells, CARCINOGENESIS
Abstract

To evaluate loss of imprinting (LOI) and expression of the IGF2 gene in matched esophageal normal and adenocarcinoma tissues, we studied a prospective cohort of 77 patients who underwent esophageal resection between 1998 and 2003. IGF2 imprinting status was determined by reverse transcription–polymerase chain reaction (PCR) following ApaI digestion, and quantitative PCR was used to evaluate IGF2 expression, which was correlated with clinicopathologic findings, disease-free and overall survival. In total, 32% (14/44) of informative tissues showed loss of IGF2 imprinting, with a strong correlation between the tumor and normal esophageal epithelia (Kappa = 0.89, P < 0.01). Normal epithelia with LOI had increased expression of IGF2 [median: 2.91, 95% confidence interval (CI): 0.93–5.06] compared with imprinted normal epithelia (median: 1.13, 95% CI: 0.85–1.39) (P = 0.03). In contrast, tumors with LOI had significantly reduced IGF2 expression (median: 1.87, 95% CI: 0.53–5.21) compared with normally imprinted tumors (median: 6.79, 95% CI: 3.39–15.89) (P = 0.016). Patients below the age of 65 years with normally imprinted tumors had significantly reduced 5 year disease-free survival (DFS) (24%) compared with patients whose tumors had LOI for IGF2 (55%) (P = 0.03). Cox regression analysis showed that IGF2 overexpression was associated with significantly reduced disease-free survival (P = 0.04). We conclude that in a subgroup of younger patients, loss of IGF2 imprinting was associated with improved outcome following esophageal resection. Expression of IGF2 in esophageal adenocarcinoma and normal esophageal epithelia depended on imprinting status and tissue type, suggesting novel molecular regulatory mechanisms in esophageal tumorigenesis. [ABSTRACT FROM PUBLISHER]

Published
2009
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121. Waiting for surgery from the patient perspective.

Author

Carr, Tracey, Teucher, Ulrich, Mann, Jackie, and Casson, Alan G.

Abstract

The aim of this study was to perform a systematic review of the impact of waiting for elective surgery from the patient perspective, with a focus on maximum tolerance, quality of life, and the nature of the waiting experience. Searches were conducted using Medline, PubMed, CINAHL, EMBASE, and HealthSTAR. Twenty-seven original research articles were identified which included each of these three themes. The current literature suggested that first, patients tend to state longer wait times as unacceptable when they experienced severe symptoms or functional impairment. Second, the relationship between length of wait and health-related quality of life depended on the nature and severity of proposed surgical intervention at the time of booking. Third, the waiting experience was consistently described as stressful and anxiety provoking. While many patients expressed anger and frustration at communication within the system, the experience of waiting was not uniformly negative. Some patients experienced waiting as an opportunity to live full lives despite pain and disability. The relatively unexamined relationship between waiting, illness and patient experience of time represents an area for future research. [ABSTRACT FROM AUTHOR]

Published
2009

123. Alternative splicing of the FGF antisense gene: differential subcellular localization in human tissues and esophageal adenocarcinoma.

Author

Shuo Cheng Zhang, Barclay, Christie, Alexander, Leigh Ann, Geldenhuys, Laurette, Porter, Geoffrey A., Casson, Alan G., and Murphy, Paul R.

Subjects
ADENOCARCINOMA, CANCER patients, TUMORS, ONCOLOGY, GENETIC mutation, MESSENGER RNA
Abstract

Overexpression of FGF-2 is associated with tumor recurrence and reduced survival after surgical resection of esophageal cancer, and these risks are reduced in tumors co-expressing the FGF antisense (FGF-AS) RNA. The aim of this study was to characterize the expression of alternatively spliced FGF-AS transcripts and encoded nudix-motif proteins in normal human tissues and in esophageal adenocarcinoma, and to correlate their expression with clinicopathologic findings and outcome. Three alternatively spliced FGF-AS transcripts encoding GFG/NUDT6 isoforms with distinct N termini were detected in various human tissues including esophageal adenocarcinoma. Expression of each isoform as a fusion protein with enhanced green fluorescent protein revealed differential subcellular trafficking: hGFG a is localized to mitochondria by an N-terminal targeting sequence (MTS), whereas hGFG b and hGFG c were localized in the cytoplasm and nucleus. Mutation/deletion analysis confirmed that the predicted MTS was necessary and sufficient for mitochondrial compartmentalization. The predominant FGF-AS mRNA expressed in esophageal tumors was splice variant b. GFG immunoreactivity was detected in the cytoplasm of all esophageal adenocarcinomas and in 88% of tumor cell nuclei. Although we found a trend towards reduced disease-free survival in patients with FGF-2 overexpressing esophageal adenocarcinomas, significantly worse disease-free survival was noted among patients whose tumors did not also overexpress the FGF-AS b isoform ( p = 0.03). Tetracycline-inducible FGF-AS b expression in stably transfected human Seg-1 esophageal adenocarcinoma cells resulted in a significant suppression of steady state FGF-2 mRNA content and cell proliferation. Our data implicate the FGF-AS b isoform in modulation of FGF-2 expression and clinical outcome in esophageal adenocarcinoma. [ABSTRACT FROM AUTHOR]

Published
2007
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127. Contributors

Author

Abbas, Ghulam, Adelstein, David J., Aigner, Clemens, Alifano, Marco, Allen, Mark S., Altorki, Nasser K., Andrade, Rafael S., Andritsos, Michael J., Arruda, M. Janine, Ashiku, Simon K., Ashrafi, Ahmad S., Backer, Carl Lewis, Bains, Majit S., Baker, Mark E., Banki, Farzaneh, Bartlett, Nancy L., Battafarano, Richard J., Beauchamp, Gilles, Bello, Ricardo A., Bennett, W. Fred, Bergeron, Michel G., Bergeron, Yves, Bhalla, Sanjeev, Bizekis, Costas, Boland, Brendan J., Bousamra, Michael, Bradley, Jeffrey D., Brandolino, Mario, Bredenberg, Carl E., Bremner, Ross M., Bronner, Mary P., Bryant, Ayesha, Burack, Joshua H., Burgos, Raul, Bussières, Jean S., Campos, Javier H., Cannie, Mieke, Cassivi, Stephen D., Casson, Alan G., Castedo, Evaristo, Cerfolio, Robert James, Cetindag, Ibrahim Bulent, Chelly, Jacques E., Chiu, Priscilla, Christie, Neil A., Chung, Andy T.A., Claytor, R. Brannon, Cooper, Joel D., Costantini, Mario, Courcoulas, Anita P., D'Amico, Thomas A., Darling, Gail, Dartevelle, Philippe, de Hoyos, Alberto, de Perrot, Marc, De Wet, Charl J., Debeer, Anne, DeCamp, Malcolm M., Jr., Dehdashti, Farrokh, DeMeester, Steven R., DeMeester, Tom R., Deprest, Jan, Deschamps, Claude, Deslauriers, Jean, Detterbeck, Frank C., Díaz, Ismael A. Conti, Doné, Elise, Doody, Daniel P., Downey, Gregory P., Downey, Robert J., Ducko, Christopher T., Dumot, John A., Duncan, Brian W., Duranceau, André, Edmundowicz, Steven A., Einstein, David M., Ellis, F. Henry, Jr., Fadel, Elie, Fell, Stanley C., Fenske, Timothy S., Ferguson, Mark K., Fernandez, Felix G., Fernando, Hiran C., Ferraro, Pasquale, Ferri, Lorenzo E., Ferson, Peter F., Finks, Jonathan F., Finley, Richard J., Flores, Raja M., Fokin, Alexander A., Fortin, Dalilah, Fréchette, Éric, Gaissert, Henning A., Gamliel, Ziv, Gandhi, Sanjiv K., Ghefter, Mario C., Gierada, David S., Gilbert, Sebastien, Goldstein, Allan M., Govindan, Ramaswamy, Graeber, Geoffrey M., Grégoire, Jocelyn, Griffin, Noreen, Grillo, Hermes C., Grunenwald, Dominique, Gucciardo, Leonardo, Gullane, Patrick J., Hagen, Jeffrey A., Lee Hall, Bruce, Hantler, Charles, Harpole, David H., Jr., Harrison-Phipps, Karen, Haughey, Bruce H., Haustermans, Karin, Hazelrigg, Stephen R., Henschke, Claudia I., Herridge, Margaret S., Hiebert, Clement A., Holinger, Lauren, Hölscher, Arnulf H., Hoover, Susan J., Huang, Jasmine, Huddleston, Charles B., Hunter, John G., Iannettoni, Mark D., Ilson, David H., Inculet, Richard I., Irshad, Kashif, Jacobsohn, Eric, Jani, Jacques, Javidan-Nejad, Cylen, Jones, David R., Jones, William G., Jurkovich, Gregory, Kaiser, Larry R., Karmy-Jones, Riyad, Keller, Steven M., Kent, Michael S., Keshavjee, Shaf, Kesler, Kenneth A., Klepetko, Walter, Konstantakos, Anastasios, Korst, Robert J., Kozower, Benjamin D., Krakovitz, Paul, Krasna, Mark J., Kreisel, Daniel, Krishna, Priya D., Krupnick, Alexander S., Kucharczuk, John C., Kwong, King F., Landreneau, Rodney J., Lang, Florian, Langer, Jacob C., Lara-Guerra, Humberto, Lardinois, Didier, Law, Simon, Lefrak, Stephen S., Leighl, Natasha B., Leo, Francesco, Lerut, Antoon (Toni) E.M.R., Liebermann-Meffert, Dorothea, Linden, Philip A., Litle, Virginia R., Little, Sherard, Locadia, Mirjam, Losso, Luis C., Louie, Brian E., Low, Donald E., Luketich, James D., Lundell, Lars, Lutey, Barbara A., Macchiarini, Paolo, Mackinnon, Susan E., Maddaus, Michael A., Malthaner, Richard A., Mason, David P., Mathisen, Douglas J., Mattioli, Sandro, Mavroudis, Constantine, Maziak, Donna E., Mazur, Paul, McLoud, Theresa, McRae, Karen M., Mehran, Reza John, Mekhail, Tarek, Merritt, Robert E., Meyers, Bryan F., Meyerson, Shari L., Miller, Daniel L., Miller, Joseph I., Jr., Mineo, Tommaso C., Minsky, Bruce D., Moley, Jeffrey, Monnier, Philippe, Montano, Rachel, Moreira, Andre L., Morse, Christopher R., Mouroux, Jérôme, Müller, Nestor L., Mulligan, Michael, Murthy, Sudish C., Naunheim, Keith, Nelems, Bill, Ng, Calvin S.H., Nguyen, Ninh T., Nichols, Francis C., Novak, Christine B., Odell, Michael J., Ollyo, Jean-Baptiste, Onaitis, Mark W., Onders, Raymond P., Ong, Sharon, Orringer, Mark B., Ouellette, Denise, Pairolero, Peter C., Papsin, Blake C., Park, Bernard J., Parsons, Alden M., Partrick, David A., Pasche, Philippe, Pastorino, Ugo, Patel, Amit N., Patterson, G. Alexander, Pearson, F. Griffith, Peitzman, Andrew B., Pennathur, Arjun, Pera, Manuel, Peracchia, Alberto, Pereira, Sérgio Tadeu L.F., Peters, Jeffrey H., Pettiford, Brian, Phillips, Kacy, Pierre, Andrew F., Pompeo, Eugenio, Pop, Daniel, Poylin, Vitaliy, Propst, Evan J., Putnam, Joe B., Jr., Qadeer, Mohammed A., Raghu, Ganesh, Rayyan, Maissa, Razzuk, Linda M., Razzuk, Maruf A., Rendina, Erino A., Rice, Thomas W., Richter, Joel E., Ritter, Jon H., Rizk, Nabil P., Robicsek, Francis, Rocco, Gaetano, Rosati, Riccardo, Rosen, Clark A., Rusch, Valerie W., Salzman, Steve H., Sampliner, Richard E., Savary, Marcel, Sbragia, Lourenço, Schipper, Paul H., Schrump, David S., Sciurba, Frank C., Shepherd, Frances A., Shrager, Joseph B., Siegel, Barry A., Sihoe, Alan D.L., Singhal, Sunil, Slinger, Peter D., Smith, Philip W., Soper, Nathaniel J., Souza, Carolina A., Sprangers, Mirjam A.G., Stewart, Robert D., Stroobants, Sigrid G., Sugarbaker, David J., Sullivan, Erin A., Sundaresan, Sudhir R., Swanström, Lee L., Temes, R. Thomas, Tronc, François, Ugalde, Paula A., Urschel, Harold C., Jr., Vaezi, Michael F., Vallières, Eric, van Berge Henegouwen, Mark I., Van de Velde, Marc, van Lanschot, Jan J.B., Van Mieghem, Tim, Van Natta, Timothy L., Van Schoubroeck, Dominique, Varela, Andrés, Veeramachaneni, Nirmal K., Venissac, Nicolas, Venuta, Federico, Videtic, Gregory M.M., Vivó, Jorge Nin, Waddell, Thomas K., Walsh, Garrett L., Warren, William H., Waters, Paul F., Watson, Thomas J., Watts, Larry T., Weder, Walter, Wick, Mark R., Wigle, Dennis A., Wildes, Troy S., Wilkins, Earl Wayne, Jr., Withers, H. Rodney, Witterick, Ian, Wizorek, Joseph J., Wong, John, Wood, Douglas E., Wright, Cameron D., Wrightson, William, Ximenes-Netto, Manoel, Yang, Steve, Yankelevitz, David F., Yazbeck, Salam, Yim, Anthony P.C., Zakowski, Maureen, and Zuccaro, Gregory, Jr.

Published
2008
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128. <TOGGLE>ras</TOGGLE> mutation and expression of the <TOGGLE>ras</TOGGLE>-regulated genes osteopontin and cathepsin L in human esophageal cancer

Author

Casson, Alan G., Wilson, Sylvia M., McCart, J. Andrea, O'Malley, Frances P., Ozcelik, Hilmi, and Tsao, Ming-Sound

Abstract

As part of our ongoing studies to characterize molecular alterations in a well-defined series of surgically resected esophageal cancers, we examined the expression of 2 ras-regulated genes, whose products (osteopontin and cathepsin L) previously were shown to be associated with tumor invasion and metastasis. RNA was extracted from primary esophageal tumors (adenocarcinomas, 19; squamous-cell carcinomas, 6) and matched histologically normal esophageal mucosa from the distant resection margin. Northern analysis was used to quantitate RNA, relative to an 18S rRNA control, and immunohistochemistry to assess the tissue distribution of osteopontin. In addition, H-, K- and N-ras mutations were studied in the same tissues using PCR and hybridization with allele (mutant)-specific oligonucleotide probes. We demonstrated a K-ras mutation (codon 12, GTT) in one esophageal adenocarcinoma. The ras-regulated gene osteopontin was over-expressed in 100% of squamous-cell carcinomas and in 58% of adenocarcinomas relative to matched normal esophageal mucosa. Patterns of immunoreactivity for osteopontin protein also varied between squamous-cell carcinomas (tumor cell staining) and adenocarcinomas (predominantly tumor-infiltrating macrophages). Expression of cathepsin L also varied with esophageal tumor histology, with over-expression in 58% of primary esophageal adenocarcinomas and 33% of squamous-cell cancers. Int. J. Cancer 72:739–745, 1997. © 1997 Wiley-Liss, Inc.

Published
1997
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129. Polymorphisms Near TBX5 and GDF7 Are Associated With Increased Risk for Barrett’s Esophagus

Author

Al Dulaimi, David, Johnson, Matthew, Trynka, Gosia, Prenen, Hans, Atherfold, Paul, Li, Xinzhong, Vaughan, Tom L., Ye, Weimin, Love, Sharon, Van Der Laan, Luc J.W., Boulter, Lisa, Rathbone, Barrie, Shaheen, Nicholas J., Underwood, Tim, Decaestecker, John, Roylance, Rebecca, Chow, Wu, Reid, Brian J., Van Den Brande, Jan, Watson, Peter, Ang, Yeng, Monk, David, Bisschops, Raf, Farrant, Mark, Farnham, Garry, O'Sullivan, Jacintha, Dhar, Anjan, Bernstein, Leslie, Beales, Ian, Toxopeus, Eelke L., Wijmenga, Cisca, Hapeshi, Julie, Tucker, Art, Sanders, Scott, Nwokolo, Chuka, Moayyedi, Paul, Kadri, Sudarshan, Vermeire, Severine, Bird, Nigel C., Barr, Hugh, Ragunath, Krish, Gammon, Marilie D., Liu, Geoffrey, Briggs, Sarah, Castro Giner, Francesc, Harrison, Rebecca, Romero, Yvonne, Patel, Praful, Kelly, Sean, Krishnadath, Kausilia, Casson, Alan G., Cleynen, Isabelle, Macdonald, David, Beckett, Conrad, McGarrigle, Sarah A., Adams, Claire L., Fitzgerald, Rebecca, Reynolds, John V., Dixon, Andrew, Whiteman, David C., Kuipers, Ernst J., McManus, Ross, Wu, Anna H., Tomlinson, Ian, Wijnhoven, Bas P.L., Zietek, Barbara, Risch, Harvey A., Chegwidden, Laura, Rembacken, Bjorn, Mullins, Paul, Haigh, Chris, Corley, Douglas A., Verhaar, Auke P., Trudgill, Nigel, Ferry, David, Palles, Claire, Murray, Iain, Green, Elaine, Nanji, Manoj, Levine, David M., Maroo, Neera, Spaander, Manon C., Wajed, Shahjehan, Kovac, Michal, Sawyer, Elinor, McMurtry, Hugh, Hardie, Laura J., Gay, Laura, Findlay, John M., Paterson, Stuart, Peppelenbosch, Maikel P., Veitch, Andrew, Grimley, Charles, Macmathuna, Padraic, Onstad, Lynn, Koss, Konrad, Kelleher, Dermot, and Jankowski, Janusz

Subjects
3. Good health
Abstract

Background & AimsBarrett's esophagus (BE) increases the risk of esophageal adenocarcinoma (EAC). We found the risk to be BE has been associated with single nucleotide polymorphisms (SNPs) on chromosome 6p21 (within the HLA region) and on 16q23, where the closest protein-coding gene is FOXF1. Subsequently, the Barrett's and Esophageal Adenocarcinoma Consortium (BEACON) identified risk loci for BE and esophageal adenocarcinoma near CRTC1 and BARX1, and within 100 kb of FOXP1. We aimed to identify further SNPs that increased BE risk and to validate previously reported associations.MethodsWe performed a genome-wide association study (GWAS) to identify variants associated with BE and further analyzed promising variants identified by BEACON by genotyping 10,158 patients with BE and 21,062 controls.ResultsWe identified 2 SNPs not previously associated with BE: rs3072 (2p24.1; odds ratio [OR]= 1.14; 95% CI: 1.09–1.18; P= 1.8× 10−11) and rs2701108 (12q24.21; OR= 0.90; 95% CI: 0.86–0.93; P= 7.5× 10−9). The closest protein-coding genes were respectively GDF7 (rs3072), which encodes a ligand in the bone morphogenetic protein pathway, and TBX5 (rs2701108), which encodes a transcription factor that regulates esophageal and cardiac development. Our data also supported in BE cases 3 risk SNPs identified by BEACON (rs2687201, rs11789015, and rs10423674). Meta-analysis of all data identified another SNPassociated with BE and esophageal adenocarcinoma: rs3784262, within ALDH1A2 (OR= 0.90; 95% CI: 0.87–0.93; P=3.72× 10−9).ConclusionsWe identified 2 loci associated with risk of BE and provided data to support a further locus. The genes we found to be associated with risk for BE encode transcription factors involved in thoracic, diaphragmatic, and esophageal development or proteins involved in the inflammatory response.

130. MiRNA-Related SNPs and Risk of Esophageal Adenocarcinoma and Barrett’s Esophagus: Post Genome-Wide Association Analysis in the BEACON Consortium

Author

Reid, Brian J., Onstad, Lynn, Peters, Ulrike, Bird, Nigel C., Risch, Harvey A., Liu, Geoffrey, Romero, Yvonne, Ye, Weimin, Hardie, Laura J., Bernstein, Leslie, Levine, David M., Chow, Wong-Ho, Vaughan, Thomas L., Gammon, Marilie D., Wu, Anna H., Casson, Alan G., Whiteman, David C., Fitzgerald, Rebecca C., Buas, Matthew F., Shaheen, Nicholas J., and Corley, Douglas A.

Subjects
3. Good health
Abstract

Incidence of esophageal adenocarcinoma (EA) has increased substantially in recent decades. Multiple risk factors have been identified for EA and its precursor, Barrett’s esophagus (BE), such as reflux, European ancestry, male sex, obesity, and tobacco smoking, and several germline genetic variants were recently associated with disease risk. Using data from the Barrett’s and Esophageal Adenocarcinoma Consortium (BEACON) genome-wide association study (GWAS) of 2,515 EA cases, 3,295 BE cases, and 3,207 controls, we examined single nucleotide polymorphisms (SNPs) that potentially affect the biogenesis or biological activity of microRNAs (miRNAs), small non-coding RNAs implicated in post-transcriptional gene regulation, and deregulated in many cancers, including EA. Polymorphisms in three classes of genes were examined for association with risk of EA or BE: miRNA biogenesis genes (157 SNPs, 21 genes); miRNA gene loci (234 SNPs, 210 genes); and miRNA-targeted mRNAs (177 SNPs, 158 genes). Nominal associations (P0.50), and we did not find evidence for interactions between variants analyzed and two risk factors for EA/BE (smoking and obesity). This analysis provides the most extensive assessment to date of miRNA-related SNPs in relation to risk of EA and BE. While common genetic variants within components of the miRNA biogenesis core pathway appear unlikely to modulate susceptibility to EA or BE, further studies may be warranted to examine potential associations between unassessed variants in miRNA genes and targets with disease risk.

131. Polymorphisms near TBX5 and GDF7 are associated with increased risk for Barrett's esophagus

Author

Palles, Claire, Chegwidden, Laura, Li, Xinzhong, Findlay, John M, Farnham, Garry, Castro Giner, Francesc, Peppelenbosch, Maikel P, Kovac, Michal, Adams, Claire L, Prenen, Hans, Briggs, Sarah, Harrison, Rebecca, Sanders, Scott, MacDonald, David, Haigh, Chris, Tucker, Art, Love, Sharon, Nanji, Manoj, DeCaestecker, John, Ferry, David, Rathbone, Barrie, Hapeshi, Julie, Barr, Hugh, Moayyedi, Paul, Watson, Peter, Zietek, Barbara, Maroo, Neera, Gay, Laura, Underwood, Tim, Boulter, Lisa, McMurtry, Hugh, Monk, David, Patel, Praful, Ragunath, Krish, Al Dulaimi, David, Murray, Iain, Koss, Konrad, Veitch, Andrew, Trudgill, Nigel, Nwokolo, Chuka, Rembacken, Bjorn, Atherfold, Paul, Green, Elaine, Ang, Yeng, Kuipers, Ernst J, Chow, Wu, Paterson, Stuart, Kadri, Sudarshan, Beales, Ian, Grimley, Charles, Mullins, Paul, Beckett, Conrad, Farrant, Mark, Dixon, Andrew, Kelly, Sean, Johnson, Matthew, Wajed, Shahjehan, Dhar, Anjan, Sawyer, Elinor, Roylance, Rebecca, Onstad, Lynn, Gammon, Marilie D, Corley, Douglas A, Shaheen, Nicholas J, Bird, Nigel C, Hardie, Laura J, Reid, Brian J, Ye, Weimin, Liu, Geoffrey, Romero, Yvonne, Bernstein, Leslie, Wu, Anna H, Casson, Alan G, Fitzgerald, Rebecca, Whiteman, David C, Risch, Harvey A, Levine, David M, Vaughan, Tom L, Verhaar, Auke P, Van Den Brande, Jan, Toxopeus, Eelke L, Spaander, Manon C, Wijnhoven, Bas PL, Van Der Laan, Luc JW, Krishnadath, Kausilia, Wijmenga, Cisca, Trynka, Gosia, McManus, Ross, Reynolds, John V, O'Sullivan, Jacintha, MacMathuna, Padraic, McGarrigle, Sarah A, Kelleher, Dermot, Vermeire, Severine, Cleynen, Isabelle, Bisschops, Raf, Tomlinson, Ian, and Jankowski, Janusz

Subjects
Risk, Esophageal Neoplasms, Polymorphism, Single Nucleotide, 3. Good health, Growth Differentiation Factors, Intestinal Metaplasia, Barrett Esophagus, Susceptibility, Bone Morphogenetic Proteins, Humans, Genetic Predisposition to Disease, EAC, T-Box Domain Proteins, Cancer, Genome-Wide Association Study
Abstract

BACKGROUND & AIMS: Barrett's esophagus (BE) increases the risk of esophageal adenocarcinoma (EAC). We found the risk to be BE has been associated with single nucleotide polymorphisms (SNPs) on chromosome 6p21 (within the HLA region) and on 16q23, where the closest protein-coding gene is FOXF1. Subsequently, the Barrett's and Esophageal Adenocarcinoma Consortium (BEACON) identified risk loci for BE and esophageal adenocarcinoma near CRTC1 and BARX1, and within 100 kb of FOXP1. We aimed to identify further SNPs that increased BE risk and to validate previously reported associations. METHODS: We performed a genome-wide association study (GWAS) to identify variants associated with BE and further analyzed promising variants identified by BEACON by genotyping 10,158 patients with BE and 21,062 controls. RESULTS: We identified 2 SNPs not previously associated with BE: rs3072 (2p24.1; odds ratio [OR] = 1.14; 95% CI: 1.09-1.18; P = 1.8 × 10(-11)) and rs2701108 (12q24.21; OR = 0.90; 95% CI: 0.86-0.93; P = 7.5 × 10(-9)). The closest protein-coding genes were respectively GDF7 (rs3072), which encodes a ligand in the bone morphogenetic protein pathway, and TBX5 (rs2701108), which encodes a transcription factor that regulates esophageal and cardiac development. Our data also supported in BE cases 3 risk SNPs identified by BEACON (rs2687201, rs11789015, and rs10423674). Meta-analysis of all data identified another SNP associated with BE and esophageal adenocarcinoma: rs3784262, within ALDH1A2 (OR = 0.90; 95% CI: 0.87-0.93; P = 3.72 × 10(-9)). CONCLUSIONS: We identified 2 loci associated with risk of BE and provided data to support a further locus. The genes we found to be associated with risk for BE encode transcription factors involved in thoracic, diaphragmatic, and esophageal development or proteins involved in the inflammatory response.

132. Risk of Esophageal Adenocarcinoma Decreases With Height, Based on Consortium Analysis and Confirmed by Mendelian Randomization

Author

Casson, Alan G., Whiteman, David C., Thrift, Aaron P., Bird, Nigel C., Romero, Yvonne, Onstad, Lynn, Risch, Harvey A., Liu, Geoffrey, Gammon, Marilie D., Vaughan, Thomas L., Hardie, Laura J., Levine, David M., Chow, Wong Ho, Corley, Douglas A., Shaheen, Nicholas J., Ye, Weimin, Wu, Anna H., Bernstein, Leslie, and Reid, Brian J.

Subjects
2. Zero hunger, surgical procedures, operative, digestive system, digestive system diseases, 3. Good health
Abstract

Risks for some cancers increase with height. We investigated the relationship between height and risk of esophageal adenocarcinoma (EAC) and its precursor, Barrett’s esophagus (BE).

133. A genome-wide association study identifies new susceptibility loci for esophageal adenocarcinoma and Barrett's esophagus

Author

Levine, David M, Ek, Weronica E, Zhang, Rui, Liu, Xinxue, Onstad, Lynn, Sather, Cassandra, Lao-Sirieix, Pierre, Gammon, Marilie D, Corley, Douglas A, Shaheen, Nicholas J, Bird, Nigel C, Hardie, Laura J, Murray, Liam J, Reid, Brian J, Chow, Wong-Ho, Risch, Harvey A, Nyrén, Olof, Ye, Weimin, Liu, Geoffrey, Romero, Yvonne, Bernstein, Leslie, Wu, Anna H, Casson, Alan G, Chanock, Stephen J, Harrington, Patricia, Caldas, Isabel, Debiram-Beecham, Irene, Caldas, Carlos, Hayward, Nicholas K, Pharoah, Paul D, Fitzgerald, Rebecca C, Macgregor, Stuart, Whiteman, David C, and Vaughan, Thomas L

Subjects
Male, Esophageal Neoplasms, Genotype, Adenocarcinoma, Polymorphism, Single Nucleotide, digestive system diseases, 3. Good health, Barrett Esophagus, Genetic Loci, Case-Control Studies, Humans, Female, Genetic Predisposition to Disease, Genome-Wide Association Study
Abstract

Esophageal adenocarcinoma is a cancer with rising incidence and poor survival. Most such cancers arise in a specialized intestinal metaplastic epithelium, which is diagnostic of Barrett's esophagus. In a genome-wide association study, we compared esophageal adenocarcinoma cases (n = 2,390) and individuals with precancerous Barrett's esophagus (n = 3,175) with 10,120 controls in 2 phases. For the combined case group, we identified three new associations. The first is at 19p13 (rs10419226: P = 3.6 × 10(-10)) in CRTC1 (encoding CREB-regulated transcription coactivator), whose aberrant activation has been associated with oncogenic activity. A second is at 9q22 (rs11789015: P = 1.0 × 10(-9)) in BARX1, which encodes a transcription factor important in esophageal specification. A third is at 3p14 (rs2687201: P = 5.5 × 10(-9)) near the transcription factor FOXP1, which regulates esophageal development. We also refine a previously reported association with Barrett's esophagus near the putative tumor suppressor gene FOXF1 at 16q24 and extend our findings to now include esophageal adenocarcinoma.

136. Risk of Esophageal Adenocarcinoma Decreases With Height, Based on Consortium Analysis and Confirmed by Mendelian Randomization.

Author

Thrift, Aaron P., Risch, Harvey A., Onstad, Lynn, Shaheen, Nicholas J., Casson, Alan G., Bernstein, Leslie, Corley, Douglas A., Levine, David M., Chow, Wong–Ho, Reid, Brian J., Romero, Yvonne, Hardie, Laura J., Liu, Geoffrey, Wu, Anna H., Bird, Nigel C., Gammon, Marilie D., Ye, Weimin, Whiteman, David C., and Vaughan, Thomas L.

Abstract

Background & Aims Risks for some cancers increase with height. We investigated the relationship between height and risk of esophageal adenocarcinoma (EAC) and its precursor, Barrett's esophagus (BE). Methods We analyzed epidemiologic and genome-wide genomic data from individuals of European ancestry in the Barrett's and Esophageal Adenocarcinoma Consortium, from 999 cases of EAC, 2061 cases of BE, and 2168 population controls. Multivariable logistic regression was used to estimate odds ratios (OR) and 95% confidence intervals (95% CI) for associations between height and risks of EAC and BE. We performed a Mendelian randomization analysis to estimate an unconfounded effect of height on EAC and BE using a genetic risk score derived from 243 genetic variants associated with height as an instrumental variable. Results Height was associated inversely with EAC (per 10-cm increase in height: OR, 0.70; 95% CI, 0.62–0.79 for men and OR, 0.57; 95% CI 0.40–0.80 for women) and BE (per 10-cm increase in height: OR, 0.69; 95% CI, 0.62–0.77 for men and OR, 0.61; 95% CI, 0.48–0.77 for women). The risk estimates were consistent across strata of age, education level, smoking, gastroesophageal reflux symptoms, body mass index, and weight. Mendelian randomization analysis yielded results quantitatively similar to those from the conventional epidemiologic analysis. Conclusions Height is associated inversely with risks of EAC and BE. Results from the Mendelian randomization study showed that the inverse association observed did not result from confounding factors. Mechanistic studies of the effect of height on EAC and BE are warranted; height could have utility in clinical risk stratification. [ABSTRACT FROM AUTHOR]

Published
2014
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137. Nonsteroidal Anti-inflammatory Drug Use Reduces Risk of Adenocarcinomas of the Esophagus and Esophagogastric Junction in a Pooled Analysis.

Author

Liao, Linda M., Vaughan, Thomas L., Corley, Douglas A., Cook, Michael B., Casson, Alan G., Kamangar, Farin, Abnet, Christian C., Risch, Harvey A., Giffen, Carol, Freedman, Neal D., Chow, Wong–Ho, Sadeghi, Shahram, Pandeya, Nirmala, Whiteman, David C., Murray, Liam J., Bernstein, Leslie, Gammon, Marilie D., and Wu, Anna H.

Subjects
ESOPHAGEAL tumors, CANCER treatment, ADENOCARCINOMA, ESOPHAGOGASTRIC junction, BARRETT'S esophagus, NONSTEROIDAL anti-inflammatory agents, META-analysis, ASPIRIN, BODY mass index, TUMOR risk factors
Abstract

Background & Aims: Regular use of aspirin and other nonsteroidal anti-inflammatory drugs (NSAIDs) has been reported to reduce risks of esophageal adenocarcinoma (EAC) and esophagogastric junctional adenocarcinoma (EGJA). However, individual studies have been too small to accurately assess the effects of medication type, frequency, or duration of use. We performed a pooled analysis to investigate these associations. Methods: We performed a pooled analysis of 6 population-based studies within the Barrett''s and Esophageal Adenocarcinoma Consortium to evaluate the association between NSAID use and the risk of EAC and EGJA, using uniform exposure definitions. We collected information from 6 studies (5 case-control and 1 cohort), with a total of 1226 EAC and 1140 EGJA cases, on aspirin and/or NSAID use. Study-specific odds ratios (ORs) and 95% confidence intervals (CIs) were estimated using multivariate adjusted logistic regression models and then pooled using a random effects meta-analysis model. Results: Compared with nonusers, individuals who have used NSAIDs had a statistically significant reduced risk of EAC (OR, 0.68; 95% CI, 0.56–0.83); they also appeared to have a reduced risk of EGJA (OR, 0.83; 95% CI, 0.66–1.03). Similar reductions in risk were observed among individuals who took aspirin or nonaspirin NSAIDs. The highest levels of frequency (daily or more frequently) and duration (≥10 years) of NSAID use were associated with an approximately 40% reduction in risk of EAC, with ORs of 0.56 (95% CI, 0.43–0.73; P trend < .001) and 0.63 (95% CI, 0.45–0.90; P trend = .04), respectively. Conclusions: Although reverse causation could, in part, explain the inverse association observed between NSAID use and EAC risk, our pooled analysis suggests a possible role for NSAIDs in prevention of adenocarcinomas of the esophagus and esophagogastric junction. [Copyright &y& Elsevier]

Published
2012
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139. Integrative post-genome-wide association analysis of CDKN2A and TP53 SNPs and risk of esophageal adenocarcinoma.

Author

Buas, Matthew F., Levine, David M., Makar, Karen W., Utsugi, Heidi, Onstad, Lynn, Li, Xiaohong, Galipeau, Patricia C., Shaheen, Nicholas J., Hardie, Laura J., Romero, Yvonne, Bernstein, Leslie, Gammon, Marilie D., Casson, Alan G., Bird, Nigel C., Risch, Harvey A., Ye, Weimin, Liu, Geoffrey, Corley, Douglas A., Blount, Patricia L., and Fitzgerald, Rebecca C.

Subjects
*CYCLIN-dependent kinase inhibitors, *ESOPHAGEAL cancer risk factors, *P53 protein, *SINGLE nucleotide polymorphisms, *ADENOCARCINOMA, *GERM cells, *TUMOR suppressor genes, *DISEASE risk factors
Abstract

Integrating data from a large genome-wide association study, a prospective clinical cohort, and a laboratory-based functional assay, this study provides evidence that germline variants in the tumor suppressor CDKN2A may influence susceptibility for esophageal adenocarcinoma, an increasingly important cancer with poor survival.Incidence of esophageal adenocarcinoma (EA) in Western countries has increased markedly in recent decades. Although several risk factors have been identified for EA and its precursor, Barrett’s esophagus (BE), including reflux, Caucasian race, male gender, obesity, and smoking, less is known about the role of inherited genetic variation. Frequent somatic mutations in the tumor suppressor genes CDKN2A and TP53 were recently reported in EA tumors, while somatic alterations at 9p (CDKN2A) and 17p (TP53) have been implicated as predictors of progression from BE to EA. Motivated by these findings, we used data from a genome-wide association study of 2515 EA cases and 3207 controls to analyze 37 germline single nucleotide polymorphisms at the CDKN2A and TP53 loci. Three CDKN2A polymorphisms were nominally associated (P < 0.05) with reduced risk of EA: rs2518720 C>T [intronic, odds ratio 0.90, P = 0.0121, q = 0.3059], rs3088440 G>A (3′UTR, odds ratio 0.84, P = 0.0186, q = 0.3059), and rs4074785 C>T (intronic, odds ratio 0.85, P = 0.0248, q = 0.3059). None of the TP53 single nucleotide polymorphisms reached nominal significance. Two of the CDKN2A variants identified were also associated with reduced risk of progression from BE to EA, when assessed in a prospective cohort of 408 BE patients: rs2518720 (hazard ratio 0.57, P = 0.0095, q = 0.0285) and rs3088440 (hazard ratio 0.34, P = 0.0368, q = 0.0552). In vitro functional studies of rs3088440, a single nucleotide polymorphism located in the seed sequence of a predicted miR-663b binding site, suggested a mechanism whereby the G>A substitution may attenuate miR-663b-mediated repression of the CDKN2A transcript. This study provides the first evidence that germline variation at the CDKN2A locus may influence EA susceptibility. [ABSTRACT FROM AUTHOR]

Published
2014
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140. Germline Genetic Contributions to Risk for Esophageal Adenocarcinoma, Barrett's Esophagus, and Gastroesophageal Reflux.

Author

Ek, Weronica E., Levine, David M., DAmato, Mauro, Pedersen, Nancy L., Magnusson, Patrik K. E., Bresso, Francesca, Onstad, Lynn E., Schmidt, Peter T., Törnblom, Hans, Nordenstedt, Helena, Romero, Yvonne, Wong-Ho Chow, Murray, Liam J., Gammon, Marilie D., Liu, Geoffrey, Bernstein, Leslie, Casson, Alan G., Risch, Harvey A., Shaheen, Nicholas J., and Bird, Nigel C.

Subjects
*ESOPHAGEAL cancer, *BARRETT'S esophagus, *CANCER patients, *GASTROESOPHAGEAL reflux, *SINGLE nucleotide polymorphisms
Abstract

Background Esophageal adenocarcinoma (EA) is an increasingly common cancer with poor survival. Barrett's esophagus (BE) is the main precursor to EA, and every year 0.12% to 0.5% of BE patients progress to EA. BE typically arises on a background of chronic gastroesophageal reflux (GERD), one of the risk factors for EA. Methods We used genome-wide association data to investigate the genetic architecture underlying GERD, BE, and EA. We applied a method to estimate the variance explained (array heritability, h²g) and the genetic correlation (rg) between GERD, BE, and EA by considering all single nucleotide polymorphisms (SNPs) simultaneously. We also estimated the polygenic overlap between GERD, BE, and EA using a prediction approach. All tests were two- sided, except in the case of variance-explained estimation where one-sided tests were used. Results We estimated a statistically significant genetic variance explained for BE (h²g = 35%; standard error [SE] = 6%; one-sided P= 1 x 10-9) and for EA (h²g = 25 %; SE = 5%; one-sided P= 2 x 10-7).The genetic correlation between BE and EA was found to be high (rg = 1.0; SE = 0.37). We also estimated a statistically significant polygenic overlap between BE and EA (one-sided P = 1 x 10-6), which suggests, together with the high genetic correlation, that shared genes underlie the development of BE and EA. Conversely, no statistically significant results were obtained for GERD. Conclusions We have demonstrated that risk to BE and EA is influenced by many germline genetic variants of small effect and that shared polygenic effects contribute to risk of these two diseases. [ABSTRACT FROM AUTHOR]

Published
2013
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141. Body mass index in relation to oesophageal and oesophagogastric junction adenocarcinomas: a pooled analysis from the International BEACON Consortium.

Author

Hoyo, Cathrine, Cook, Michael B, Kamangar, Farin, Freedman, Neal D, Whiteman, David C, Bernstein, Leslie, Brown, Linda M, Risch, Harvey A, Ye, Weimin, Sharp, Linda, Wu, Anna H, Ward, Mary H, Casson, Alan G, Murray, Liam J, Corley, Douglas A, Nyrén, Olof, Pandeya, Nirmala, Vaughan, Thomas L, Chow, Wong-Ho, and Gammon, Marilie D

Subjects
*OBESITY risk factors, *ESOPHAGEAL perforation, *BODY mass index, *SYMPTOMS, *DATA analysis, *MEDICAL statistics, *META-analysis
Abstract

Background Previous studies suggest an association between obesity and oesophageal (OA) and oesophagogastric junction adenocarcinomas (OGJA). However, these studies have been limited in their ability to assess whether the effects of obesity vary by gender or by the presence of gastro-oesophageal reflux (GERD) symptoms.Methods Individual participant data from 12 epidemiological studies (8 North American, 3 European and 1 Australian) comprising 1997 OA cases, 1900 OGJA cases and 11 159 control subjects were pooled. Logistic regression was used to estimate study-specific odds ratios (ORs) and 95% confidence intervals (CIs) for the association between body mass index (BMI, kg/m2) and the risk of OA and OGJA. Random-effects meta-analysis was used to combine these ORs. We also investigated effect modification and synergistic interaction of BMI with GERD symptoms and gender.Results The association of OA and OGJA increased directly with increasing BMI (P for trend <0.001). Compared with individuals with a BMI <25, BMI &geq;40 was associated with both OA (OR 4.76, 95% CI 2.96–7.66) and OGJA (OR 3.07, 95% CI 1.89–4.99). These associations were similar when stratified by gender and GERD symptoms. There was evidence for synergistic interaction between BMI and GERD symptoms in relation to OA/OGJA risk.Conclusions These data indicate that BMI is directly associated with OA and OGJA risk in both men and women and in those with and without GERD symptoms. Disentangling the relationship between BMI and GERD will be important for understanding preventive efforts for OA and OGJA. [ABSTRACT FROM PUBLISHER]

Published
2012
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142. The importance of exposure rate on odds ratios by cigarette smoking and alcohol consumption for esophageal adenocarcinoma and squamous cell carcinoma in the Barrett's Esophagus and Esophageal Adenocarcinoma Consortium

Author

Lubin, Jay H., Cook, Michael B., Pandeya, Nirmala, Vaughan, Thomas L., Abnet, Christian C., Giffen, Carol, Webb, Penelope M., Murray, Liam J., Casson, Alan G., Risch, Harvey A., Ye, Weimin, Kamangar, Farin, Bernstein, Leslie, Sharp, Linda, Nyrén, Olof, Gammon, Marilie D., Corley, Douglas A., Wu, Anna H., Brown, Linda M., and Chow, Wong-Ho

Subjects
*SMOKING, *ALCOHOL drinking, *ESOPHAGEAL cancer, *ADENOCARCINOMA, *SQUAMOUS cell carcinoma, *BARRETT'S esophagus
Abstract

Abstract: Background: Cigarette smoking is associated with esophageal adenocarcinoma (EAC), esophagogastric junctional adenocarcinoma (EGJA) and esophageal squamous cell carcinoma (ESCC), and alcohol consumption with ESCC. However, no analyses have examined how delivery rate modifies the strength of odds ratio (OR) trends with total exposure, i.e., the impact on the OR for a fixed total exposure of high exposure rate for short duration compared with low exposure rate for long duration. Methods: The authors pooled data from 12 case–control studies from the Barrett''s Esophagus and Esophageal Adenocarcinoma Consortium (BEACON), including 1242 (EAC), 1263 (EGJA) and 954 (ESCC) cases and 7053 controls, modeled joint ORs for cumulative exposure and exposure rate for cigarette smoking and alcohol consumption, and evaluated effect modification by sex, body mass index (BMI), age and self-reported acid reflux. Results: For smoking, all sites exhibited inverse delivery rate effects, whereby ORs with pack-years increased, but trends weakened with increasing cigarettes/day. None of the examined factors modified associations, except for ESCC where younger ages at diagnosis enhanced smoking effects (P <0.01). For EAC and EGJA, ORs with drink-years exhibited inverse associations in <5drinks/day consumers and no association in heavier consumers. For ESCC, ORs with drink-years increased, with trends strengthening with greater drinks/day. There was no significant effect modification, except for EAC and EGJA where acid reflux mitigated the inverse associations (P =0.02). For ESCC, younger ages at diagnosis enhanced drinking-related ORs (P <0.01). Conclusions: Patterns of ORs by pack-years and drink-years, delivery rate effects and effect modifiers revealed common as well as distinct etiologic elements for these diseases. [Copyright &y& Elsevier]

Published
2012
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143. Cigarette Smoking and Adenocarcinomas of the Esophagus and Esophagogastric Junction: A Pooled Analysis From the International BEACON Consortium.

Author

Cook, Michael B., Kamangar, Farin, Whiteman, David C., Freedman, Neal D., Gammon, Marilie D., Bernstein, Leslie, Brown, Linda M., Risch, Harvey A., Weimin Ye, Sharp, Linda, Pandeya, Nirmala, Webb, Penelope M., Wu, Anna H., Ward, Mary H., Giffen, Carol, Casson, Alan G., Abnet, Christian C., Murray, Liam J., Corley, Douglas A., and Nyrén, Olof

Subjects
*ADENOCARCINOMA, *SMOKING, *HEALTH, *ESOPHAGOGASTRIC junction, *ESOPHAGEAL cancer, *PHYSIOLOGICAL effects of tobacco, *CIGARETTE smokers, *BARRETT'S esophagus
Abstract

Background Previous studies that showed an association between smoking and adenocarcinomas of the esophagus and esophagogastric junction were limited in their ability to assess differences by tumor site, sex, dose-response, and duration of cigarette smoking cessation. Methods We used primary data from 10 population-based case-control studies and two cohort studies from the Barrett's Esophagus and Esophageal Adenocarcinoma Consortium. Analyses were restricted to white non-Hispanic men and women. Patients were classified as having esophageal adenocarcinoma (n = 1540), esophagogastric junctional adenocarcinoma (n = 1450), or a combination of both (all adenocarcinoma; n = 2990). Control subjects (n = 9453) were population based. Associations between pack-years of cigarette smoking and risks of adenocarcinomas were assessed, as well as their potential modification by sex and duration of smoking cessation. Study-specific odds ratios (ORs) estimated using multivariable logistic regression models, adjusted for age, sex, body mass index, education, and gastroesophageal reflux, were pooled using a meta-analytic methodology to generate summary odds ratios. All statistical tests were two-sided. Results The summary odds ratios demonstrated strong associations between cigarette smoking and esophageal adenocarcinoma (OR = 1.96, 95% confidence interval [CI] = 1.64 to 2.34), esophagogastric junctional adenocarcinoma (OR = 2.18, 95% CI = 1.84 to 2.58), and all adenocarcinoma (OR = 2.08, 95% CI = 1.83 to 2.37). In addition, there was a strong dose-response association between pack-years of cigarette smoking and each outcome (P < .001). Compared with current smokers, longer smoking cessation was associated with a decreased risk of all adenocarcinoma after adjusting for pack-years (<10 years of smoking cessation: OR = 0.82, 95% CI = 0.60 to 1.13; and ≥10 years of smoking cessation: OR = 0.71, 95% CI = 0.56 to 0.89). Sex-specific summary odds ratios were similar. Conclusions Cigarette smoking is associated with increased risks of adenocarcinomas of the esophagus and esophagogastric junction in white men and women; compared with current smoking, smoking cessation was associated with reduced risks. [ABSTRACT FROM AUTHOR]

Published
2010
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144. A polymorphic variant of the insulin-like growth factor type I receptor gene modifies risk of obesity for esophageal adenocarcinoma

Author

Macdonald, Kimberley, Porter, Geoffrey A., Guernsey, Duane L., Zhao, Ronghua, and Casson, Alan G.

Subjects
*GENETIC polymorphisms, *BIOCHEMICAL variation, *SOMATOMEDIN, *OBESITY risk factors, *ADENOCARCINOMA, *ESOPHAGEAL cancer, *BARRETT'S esophagus, *GASTROESOPHAGEAL reflux
Abstract

Abstract: Background: To investigate potential biologic mechanisms underlying the association between obesity and risk for esophageal adenocarcinoma (EADC), we studied the frequency of a common polymorphism of the insulin-like growth factor I receptor (IGF-IR) gene in patients with either gastroesophageal reflux disease (GERD), premalignant Barrett esophagus (BE) and or invasive EADC. Methods: Using a well characterized series of 431 individuals enrolled in a case–control study, we studied the frequency of the IGF-IR gene polymorphism, G1013A. Results: On multivariate analysis controlling for age and gender, in comparison to asymptomatic controls, obese individuals with the polymorphic A-variant (G/A, A/A) were found to have significantly increased risk for EADC (OR 4.81; 95%CI 1.09–21.15), whereas obese individuals with the G/G variant were not at statistically significant increased risk (OR 2.69; 95%CI 0.41–17.62). Similarly, compared to asymptomatic controls, only obese individuals with the A-variant (G/A, A/A) were at increased risk for BE (OR 3.11; 95%CI 1.12–8.63), while obese individuals with the G/G variant were not at increased risk for BE (OR 2.91; 95%CI 0.69–12.15). Conclusion: We conclude that the common IGF-IR gene polymorphism G1013A modulates the risk of obesity for EADC, an effect most likely mediated by altered the receptor function by influencing gene transcription or mRNA stability. These findings further implicate the insulin-like growth factor axis in the molecular pathogenesis of EADC, and represent a plausible mechanistic link underlying the association between obesity and malignancy. [Copyright &y& Elsevier]

Published
2009
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145. Functional assessment of the cervical esophagus after gastric transposition and cervical esophagogastrostomy

Author

Koh, Paul, Turnbull, Geoffrey, Attia, Elhamy, LeBrun, Paul, and Casson, Alan G.

Subjects
*CERVICAL vertebrae, *ESOPHAGUS, *HYPOPHARYNX, *BARIUM
Abstract

Objectives: The aim of this exploratory study was to investigate swallowing and function of the cervical esophagus after esophageal resection and reconstruction. Methods: Nine patients (8 males, 1 female; median age 63 years), who underwent esophageal resection for adenocarcinoma, were studied from 6 to 40 months (median 18 months) postoperatively. For all patients, the upper gastrointestinal tract was reconstructed by transposing a narrow gastric tube through the posterior mediastinum to the left neck, where a semi-mechanical anastomosis to the cervical esophagus was performed. No patient had an anatomic obstruction to swallowing or stricture. The oral and pharyngeal phases of deglutition and function of the cervical esophagus were evaluated objectively by video barium swallow, esophagogastroscopy, velopharyngeal examination, manometry and balloon inflation in the cervical esophagus. Results: The median length of the cervical esophagus was 5 cm (range 3–7 cm). Mild reflux laryngopharyngitis was seen in all patients. Although all patients had an objective functional dysphagia measurement (American Speech-Language-Hearing Association) of 7 (normal), five reported subjective dysphagia. Four (of the five symptomatic) patients were found to have high pressure peristalitic activity (mean >100 mmHg) following balloon distention (10–30 ml) of the cervical esophagus, which was painful in three cases. Conclusions: We conclude that in the absence of an anatomic cause for dysphagia after cervical esophagogastrostomy, a functional etiology may be explained by hypertensive peristalsis resulting from distention of the remaining cervical esophageal remnant. These findings may further explain anecdotal reports of the efficacy of empiric dilation after upper gastrointestinal reconstruction when no stricture is seen. [Copyright &y& Elsevier]

Published
2004
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146. Polymorphisms near TBX5 and GDF7 are associated with increased risk for Barrett's esophagus.

Author

Palles C, Chegwidden L, Li X, Findlay JM, Farnham G, Castro Giner F, Peppelenbosch MP, Kovac M, Adams CL, Prenen H, Briggs S, Harrison R, Sanders S, MacDonald D, Haigh C, Tucker A, Love S, Nanji M, deCaestecker J, Ferry D, Rathbone B, Hapeshi J, Barr H, Moayyedi P, Watson P, Zietek B, Maroo N, Gay L, Underwood T, Boulter L, McMurtry H, Monk D, Patel P, Ragunath K, Al Dulaimi D, Murray I, Koss K, Veitch A, Trudgill N, Nwokolo C, Rembacken B, Atherfold P, Green E, Ang Y, Kuipers EJ, Chow W, Paterson S, Kadri S, Beales I, Grimley C, Mullins P, Beckett C, Farrant M, Dixon A, Kelly S, Johnson M, Wajed S, Dhar A, Sawyer E, Roylance R, Onstad L, Gammon MD, Corley DA, Shaheen NJ, Bird NC, Hardie LJ, Reid BJ, Ye W, Liu G, Romero Y, Bernstein L, Wu AH, Casson AG, Fitzgerald R, Whiteman DC, Risch HA, Levine DM, Vaughan TL, Verhaar AP, van den Brande J, Toxopeus EL, Spaander MC, Wijnhoven BP, van der Laan LJ, Krishnadath K, Wijmenga C, Trynka G, McManus R, Reynolds JV, O'Sullivan J, MacMathuna P, McGarrigle SA, Kelleher D, Vermeire S, Cleynen I, Bisschops R, Tomlinson I, and Jankowski J

Subjects
Barrett Esophagus etiology, Esophageal Neoplasms genetics, Genome-Wide Association Study, Humans, Risk, Barrett Esophagus genetics, Bone Morphogenetic Proteins genetics, Genetic Predisposition to Disease, Growth Differentiation Factors genetics, Polymorphism, Single Nucleotide, T-Box Domain Proteins genetics
Abstract

Background & Aims: Barrett's esophagus (BE) increases the risk of esophageal adenocarcinoma (EAC). We found the risk to be BE has been associated with single nucleotide polymorphisms (SNPs) on chromosome 6p21 (within the HLA region) and on 16q23, where the closest protein-coding gene is FOXF1. Subsequently, the Barrett's and Esophageal Adenocarcinoma Consortium (BEACON) identified risk loci for BE and esophageal adenocarcinoma near CRTC1 and BARX1, and within 100 kb of FOXP1. We aimed to identify further SNPs that increased BE risk and to validate previously reported associations., Methods: We performed a genome-wide association study (GWAS) to identify variants associated with BE and further analyzed promising variants identified by BEACON by genotyping 10,158 patients with BE and 21,062 controls., Results: We identified 2 SNPs not previously associated with BE: rs3072 (2p24.1; odds ratio [OR] = 1.14; 95% CI: 1.09-1.18; P = 1.8 × 10(-11)) and rs2701108 (12q24.21; OR = 0.90; 95% CI: 0.86-0.93; P = 7.5 × 10(-9)). The closest protein-coding genes were respectively GDF7 (rs3072), which encodes a ligand in the bone morphogenetic protein pathway, and TBX5 (rs2701108), which encodes a transcription factor that regulates esophageal and cardiac development. Our data also supported in BE cases 3 risk SNPs identified by BEACON (rs2687201, rs11789015, and rs10423674). Meta-analysis of all data identified another SNP associated with BE and esophageal adenocarcinoma: rs3784262, within ALDH1A2 (OR = 0.90; 95% CI: 0.87-0.93; P = 3.72 × 10(-9))., Conclusions: We identified 2 loci associated with risk of BE and provided data to support a further locus. The genes we found to be associated with risk for BE encode transcription factors involved in thoracic, diaphragmatic, and esophageal development or proteins involved in the inflammatory response., (Copyright © 2015 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published
2015
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147. Obesity and risk of esophageal adenocarcinoma and Barrett's esophagus: a Mendelian randomization study.

Author

Thrift AP, Shaheen NJ, Gammon MD, Bernstein L, Reid BJ, Onstad L, Risch HA, Liu G, Bird NC, Wu AH, Corley DA, Romero Y, Chanock SJ, Chow WH, Casson AG, Levine DM, Zhang R, Ek WE, MacGregor S, Ye W, Hardie LJ, Vaughan TL, and Whiteman DC

Subjects
Adenocarcinoma epidemiology, Adult, Aged, Barrett Esophagus complications, Barrett Esophagus epidemiology, Esophageal Neoplasms epidemiology, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Male, Middle Aged, Obesity complications, Obesity epidemiology, Precancerous Conditions epidemiology, Predictive Value of Tests, Risk Assessment, Risk Factors, Adenocarcinoma genetics, Barrett Esophagus genetics, Body Mass Index, Esophageal Neoplasms genetics, Mendelian Randomization Analysis, Obesity genetics, Polymorphism, Single Nucleotide, Precancerous Conditions genetics
Abstract

Background: Data from observational studies suggest that body mass index (BMI) is causally related to esophageal adenocarcinoma (EAC) and its precursor, Barrett's esophagus (BE). However, the relationships may be affected by bias and confounding., Methods: We used data from the Barrett's and Esophageal Adenocarcinoma Genetic Susceptibility Study: 999 patients with EAC, 2061 patients with BE, and 2169 population controls. We applied the two-stage control function instrumental variable method of the Mendelian randomization approach to estimate the unbiased, unconfounded effect of BMI on risk of EAC and BE. This was performed using a genetic risk score, derived from 29 genetic variants shown to be associated with BMI, as an instrument for lifetime BMI. A higher score indicates propensity to obesity. All tests were two-sided., Results: The genetic risk score was not associated with potential confounders, including gastroesophageal reflux symptoms and smoking. In the instrumental variable analyses (IV), EAC risk increased by 16% (IV-odds ratio [OR] = 1.16, 95% confidence interval [CI] = 1.01 to 1.33) and BE risk increased by 12% (IV-OR = 1.12, 95% CI = 1.00 to 1.25) per 1kg/m(2) increase in BMI. BMI was statistically significantly associated with EAC and BE in conventional epidemiologic analyses., Conclusions: People with a high genetic propensity to obesity have higher risks of esophageal metaplasia and neoplasia than people with low genetic propensity. These analyses provide the strongest evidence to date that obesity is independently associated with BE and EAC, and is not due to confounding or bias inherent in conventional epidemiologic analyses., (© The Author 2014. Published by Oxford University Press. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published
2014
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148. Identification and characterization of stemlike cells in human esophageal adenocarcinoma and normal epithelial cell lines.

Author

Zhao R, Quaroni L, and Casson AG

Subjects
Adenocarcinoma drug therapy, Adenocarcinoma genetics, Adenocarcinoma metabolism, Animals, Antigens, CD metabolism, Antineoplastic Agents pharmacology, Basic Helix-Loop-Helix Transcription Factors genetics, Basic Helix-Loop-Helix Transcription Factors metabolism, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Blotting, Western, Cell Line, Tumor, Cell Proliferation, Cisplatin pharmacology, Drug Resistance, Neoplasm, Epithelial Cells drug effects, Epithelial Cells metabolism, Esophageal Neoplasms drug therapy, Esophageal Neoplasms genetics, Esophageal Neoplasms metabolism, Flow Cytometry, Fluorouracil pharmacology, Gene Expression Regulation, Neoplastic, Humans, Immunohistochemistry, Integrin alpha6 metabolism, Mice, Mice, Nude, Mice, Transgenic, Neoplastic Stem Cells drug effects, Neoplastic Stem Cells metabolism, RNA, Messenger metabolism, Receptors, G-Protein-Coupled metabolism, Receptors, Transferrin metabolism, Reverse Transcriptase Polymerase Chain Reaction, Spheroids, Cellular, Time Factors, Tumor Burden, Xenograft Model Antitumor Assays, Adenocarcinoma pathology, Epithelial Cells pathology, Esophageal Neoplasms pathology, Neoplastic Stem Cells pathology
Abstract

Objective: Recent studies have suggested that human solid tumors may contain subpopulations of cancer stem cells with the capacity for self-renewal and the potential to initiate and maintain tumor growth. The aim of this study was to use human esophageal cell lines to identify and characterize putative esophageal cancer stem cell populations., Methods: To enrich stemlike cells, Het-1A (derived from immortalized normal esophageal epithelium), OE33, and JH-EsoAd1 (each derived from primary esophageal adenocarcinomas) were cultured using serum-free media to form spheres. A comprehensive analysis of parent and spheroid cells was performed by flow cytometry, Western blot analysis, immunohistochemistry and polymerase chain reaction array to study cancer stem cell-related genes, colony formation assays to assess clonogenicity, xenotransplantation to assess tumorigenicity, and 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assays to assess chemosensitivity to 5-fluorouracil and cisplatin., Results: For all cell lines, clonogenicity, tumorigenicity, and chemoresistance to 5-fluorouracil and cisplatin were significantly higher than for spheroid cells compared with parent cells. Spheroids exhibited an increased frequency of cells expressing integrin α6(bri)/CD71(dim), and Achaete-scute complex homolog 2 messenger RNA and protein were also significantly overexpressed in spheroid cells compared with parent cells., Conclusions: The higher clonogenicity, tumorigenicity, and drug resistance exhibited by spheroids derived from Het-1A, OE33, and JH-EsoAd1 reflects an enrichment of stemlike cell populations within each esophageal cell line. Esophageal cells enriched for integrin α6(bri)/CD71(dim) and/or overexpressing Achaete-scute complex homolog 2 would appear to represent at least a subpopulation of stemlike cells in Het-1A, OE33, and JH-EsoAd1., (Copyright © 2012 The American Association for Thoracic Surgery. Published by Mosby, Inc. All rights reserved.)

Published
2012
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149. Common variants at the MHC locus and at chromosome 16q24.1 predispose to Barrett's esophagus.

Author

Su Z, Gay LJ, Strange A, Palles C, Band G, Whiteman DC, Lescai F, Langford C, Nanji M, Edkins S, van der Winkel A, Levine D, Sasieni P, Bellenguez C, Howarth K, Freeman C, Trudgill N, Tucker AT, Pirinen M, Peppelenbosch MP, van der Laan LJ, Kuipers EJ, Drenth JP, Peters WH, Reynolds JV, Kelleher DP, McManus R, Grabsch H, Prenen H, Bisschops R, Krishnadath K, Siersema PD, van Baal JW, Middleton M, Petty R, Gillies R, Burch N, Bhandari P, Paterson S, Edwards C, Penman I, Vaidya K, Ang Y, Murray I, Patel P, Ye W, Mullins P, Wu AH, Bird NC, Dallal H, Shaheen NJ, Murray LJ, Koss K, Bernstein L, Romero Y, Hardie LJ, Zhang R, Winter H, Corley DA, Panter S, Risch HA, Reid BJ, Sargeant I, Gammon MD, Smart H, Dhar A, McMurtry H, Ali H, Liu G, Casson AG, Chow WH, Rutter M, Tawil A, Morris D, Nwokolo C, Isaacs P, Rodgers C, Ragunath K, MacDonald C, Haigh C, Monk D, Davies G, Wajed S, Johnston D, Gibbons M, Cullen S, Church N, Langley R, Griffin M, Alderson D, Deloukas P, Hunt SE, Gray E, Dronov S, Potter SC, Tashakkori-Ghanbaria A, Anderson M, Brooks C, Blackwell JM, Bramon E, Brown MA, Casas JP, Corvin A, Duncanson A, Markus HS, Mathew CG, Palmer CN, Plomin R, Rautanen A, Sawcer SJ, Trembath RC, Viswanathan AC, Wood N, Trynka G, Wijmenga C, Cazier JB, Atherfold P, Nicholson AM, Gellatly NL, Glancy D, Cooper SC, Cunningham D, Lind T, Hapeshi J, Ferry D, Rathbone B, Brown J, Love S, Attwood S, MacGregor S, Watson P, Sanders S, Ek W, Harrison RF, Moayyedi P, de Caestecker J, Barr H, Stupka E, Vaughan TL, Peltonen L, Spencer CC, Tomlinson I, Donnelly P, and Jankowski JA

Subjects
Adult, Aged, Case-Control Studies, Female, Gene Frequency, Genetic Loci, Genome-Wide Association Study, Humans, Linkage Disequilibrium, Male, Middle Aged, Models, Genetic, Barrett Esophagus genetics, Chromosomes, Human, Pair 16, Genetic Predisposition to Disease, Major Histocompatibility Complex, Polymorphism, Single Nucleotide
Abstract

Barrett's esophagus is an increasingly common disease that is strongly associated with reflux of stomach acid and usually a hiatus hernia, and it strongly predisposes to esophageal adenocarcinoma (EAC), a tumor with a very poor prognosis. We report the first genome-wide association study on Barrett's esophagus, comprising 1,852 UK cases and 5,172 UK controls in the discovery stage and 5,986 cases and 12,825 controls in the replication stage. Variants at two loci were associated with disease risk: chromosome 6p21, rs9257809 (Pcombined=4.09×10(-9); odds ratio (OR)=1.21, 95% confidence interval (CI)=1.13-1.28), within the major histocompatibility complex locus, and chromosome 16q24, rs9936833 (Pcombined=2.74×10(-10); OR=1.14, 95% CI=1.10-1.19), for which the closest protein-coding gene is FOXF1, which is implicated in esophageal development and structure. We found evidence that many common variants of small effect contribute to genetic susceptibility to Barrett's esophagus and that SNP alleles predisposing to obesity also increase risk for Barrett's esophagus.

Published
2012
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150. Alcohol intake and risk of oesophageal adenocarcinoma: a pooled analysis from the BEACON Consortium.

Author

Freedman ND, Murray LJ, Kamangar F, Abnet CC, Cook MB, Nyrén O, Ye W, Wu AH, Bernstein L, Brown LM, Ward MH, Pandeya N, Green AC, Casson AG, Giffen C, Risch HA, Gammon MD, Chow WH, Vaughan TL, Corley DA, and Whiteman DC

Subjects
Adenocarcinoma epidemiology, Adenocarcinoma pathology, Adult, Alcohol Drinking epidemiology, Esophageal Neoplasms epidemiology, Esophageal Neoplasms pathology, Female, Follow-Up Studies, Humans, Incidence, Male, Middle Aged, Retrospective Studies, Risk Factors, Surveys and Questionnaires, United States epidemiology, Young Adult, Adenocarcinoma etiology, Alcohol Drinking adverse effects, Esophageal Neoplasms etiology, Risk Assessment methods
Abstract

Background and Aims: Alcohol intake is a strong and well established risk factor for oesophageal squamous cell carcinoma (OSCC), but the association with oesophageal adenocarcinoma (OA) or adjacent tumours of the oesophagogastric junction (OGJA), remains unclear. Therefore, the association of alcohol intake with OSCC, OA, and OGJA was determined in nine case-control studies and two cohort studies of the Barrett's Esophagus and Esophageal Adenocarcinoma Consortium (BEACON)., Materials and Methods: Information was collected on alcohol intake, age, sex, education, body mass index, gastro-oesophageal reflux, and tobacco smoking from each study. Along with 10,854 controls, 1821 OA, and 1837 OGJA, seven studies also collected OSCC cases (n=1016). Study specific ORs and 95% CIs were calculated from multivariate adjusted logistic regression models for alcohol intake in categories compared to non-drinkers. Summary risk estimates were obtained by random effects models. Results No increase was observed in the risk of OA or OGJA for increasing levels of any of the alcohol intake measures examined. ORs for the highest frequency category (≥ 7 drinks per day) were 0.97 (95% CI 0.68 to 1.36) for OA and 0.77 (95% CI = 0.54 to 1.10) for OGJA. Suggestive findings linked moderate intake (eg, 0.5 to <1 drink per day) to decreased risk of OA (OR 0.63, 95% CI 0.41 to 0.99) and OGJA (OR 0.78, 95% CI 0.62 to 0.99). In contrast, alcohol intake was strongly associated with increased risk of OSCC (OR for ≥ 7 drinks per day 9.62, 95% CI 4.26 to 21.71)., Conclusions: In contrast to OSCC, higher alcohol consumption was not associated with increased risk of either OA or OGJA. The apparent inverse association observed with moderate alcohol intake should be evaluated in future prospective studies.

Published
2011
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