Your search keyword '"Gruber, Stephen B"' showing total 86 results

1. Validation of a genetic-enhanced risk prediction model for colorectal cancer in a large community-based cohort

Author

Su, Yu-Ru, Sakoda, Lori C., Jeon, Jihyoun, Thomas, Minta, Lin, Yi, Schneider, Jennifer L., Udaltsova, Natalia, Lee, Jeffrey K., Lansdorp-Vogelaar, Iris, Peterse, Elisabeth F P, Zauber, Ann G., Zheng, Jiayin, Zheng, Yingye, Hauser, Elizabeth, Baron, John A., Barry, Elizabeth L., Bishop, D Timothy, Brenner, Hermann, Buchanan, Daniel D., Burnett-Hartman, Andrea, Campbell, Peter T., Casey, Graham, Castellví-Bel, Sergi, Chan, Andrew T., Chang-Claude, Jenny, Figueiredo, Jane C., Gallinger, Steven J., Giles, Graham G., Gruber, Stephen B., Gsur, Andrea, Gunter, Marc J., Hampe, Jochen, Hampel, Heather, Harrison, Tabitha A., Hoffmeister, Michael, Hua, Xinwei, Huyghe, Jeroen R., Jenkins, Mark A., Keku, Temitope O., Marchand, Loic Le, Li, Li, Lindblom, Annika, Moreno, Victor, Newcomb, Polly A., Pharoah, Paul D P, Platz, Elizabeth A., Potter, John D., Qu, Conghui, Rennert, Gad, Schoen, Robert E., Slattery, Martha L., Song, Mingyang, van Duijnhoven, Fränzel J B, van Guelpen, Bethany, Vodicka, Pavel, Wolk, Alicja, Woods, Michael O., Wu, Anna H., Hayes, Richard B., Peters, Ulrike, Corley, Douglas A., Hsu, Li, Su, Yu-Ru, Sakoda, Lori C., Jeon, Jihyoun, Thomas, Minta, Lin, Yi, Schneider, Jennifer L., Udaltsova, Natalia, Lee, Jeffrey K., Lansdorp-Vogelaar, Iris, Peterse, Elisabeth F P, Zauber, Ann G., Zheng, Jiayin, Zheng, Yingye, Hauser, Elizabeth, Baron, John A., Barry, Elizabeth L., Bishop, D Timothy, Brenner, Hermann, Buchanan, Daniel D., Burnett-Hartman, Andrea, Campbell, Peter T., Casey, Graham, Castellví-Bel, Sergi, Chan, Andrew T., Chang-Claude, Jenny, Figueiredo, Jane C., Gallinger, Steven J., Giles, Graham G., Gruber, Stephen B., Gsur, Andrea, Gunter, Marc J., Hampe, Jochen, Hampel, Heather, Harrison, Tabitha A., Hoffmeister, Michael, Hua, Xinwei, Huyghe, Jeroen R., Jenkins, Mark A., Keku, Temitope O., Marchand, Loic Le, Li, Li, Lindblom, Annika, Moreno, Victor, Newcomb, Polly A., Pharoah, Paul D P, Platz, Elizabeth A., Potter, John D., Qu, Conghui, Rennert, Gad, Schoen, Robert E., Slattery, Martha L., Song, Mingyang, van Duijnhoven, Fränzel J B, van Guelpen, Bethany, Vodicka, Pavel, Wolk, Alicja, Woods, Michael O., Wu, Anna H., Hayes, Richard B., Peters, Ulrike, Corley, Douglas A., and Hsu, Li

Abstract

BACKGROUND: Polygenic risk scores (PRS) which summarize individuals' genetic risk profile may enhance targeted colorectal cancer screening. A critical step towards clinical implementation is rigorous external validations in large community-based cohorts. This study externally validated a PRS-enhanced colorectal cancer risk model comprising 140 known colorectal cancer loci to provide a comprehensive assessment on prediction performance. METHODS: The model was developed using 20,338 individuals and externally validated in a community-based cohort (n = 85,221). We validated predicted 5-year absolute colorectal cancer risk, including calibration using expected-to-observed case ratios (E/O) and calibration plots, and discriminatory accuracy using time-dependent AUC. The PRS-related improvement in AUC, sensitivity and specificity were assessed in individuals of age 45 to 74 years (screening-eligible age group) and 40 to 49 years with no endoscopy history (younger-age group). RESULTS: In European-ancestral individuals, the predicted 5-year risk calibrated well [E/O = 1.01; 95% confidence interval (CI), 0.91-1.13] and had high discriminatory accuracy (AUC = 0.73; 95% CI, 0.71-0.76). Adding the PRS to a model with age, sex, family and endoscopy history improved the 5-year AUC by 0.06 (P < 0.001) and 0.14 (P = 0.05) in the screening-eligible age and younger-age groups, respectively. Using a risk-threshold of 5-year SEER colorectal cancer incidence rate at age 50 years, adding the PRS had a similar sensitivity but improved the specificity by 11% (P < 0.001) in the screening-eligible age group. In the younger-age group it improved the sensitivity by 27% (P = 0.04) with similar specificity. CONCLUSIONS: The proposed PRS-enhanced model provides a well-calibrated 5-year colorectal cancer risk prediction and improves discriminatory accuracy in the external cohort. IMPACT: The proposed model has potential utility in risk-stratified colorectal cancer prevention.

Published

2023

2. Genome-wide interaction study with smoking for colorectal cancer risk identifies novel genetic loci related to tumor suppression, inflammation, and immune response

Author

Carreras-Torres, Robert, Kim, Andre E., Lin, Yi, Díez-Obrero, Virginia, Bien, Stephanie A., Qu, Conghui, Wang, Jun, Dimou, Niki, Aglago, Elom K., Albanes, Demetrius, Arndt, Volker, Baurley, James W., Berndt, Sonja I., Bézieau, Stéphane, Bishop, D Timothy, Bouras, Emmanouil, Brenner, Hermann, Budiarto, Arif, Campbell, Peter T., Casey, Graham, Chan, Andrew T., Chang-Claude, Jenny, Chen, Xuechen, Conti, David V., Dampier, Christopher H., Devall, Matthew A M, Drew, David A., Figueiredo, Jane C., Gallinger, Steven, Giles, Graham G., Gruber, Stephen B., Gsur, Andrea, Gunter, Marc J., Harrison, Tabitha A., Hidaka, Akihisa, Hoffmeister, Michael, Huyghe, Jeroen R., Jenkins, Mark A., Jordahl, Kristina M., Kawaguchi, Eric, Keku, Temitope O., Kundaje, Anshul, Le Marchand, Loic, Lewinger, Juan Pablo, Li, Li, Mahesworo, Bharuno, Morrison, John L., Murphy, Neil, Nan, Hongmei, Nassir, Rami, Newcomb, Polly A., Obón-Santacana, Mireia, Ogino, Shuji, Ose, Jennifer, Pai, Rish K., Palmer, Julie R., Papadimitriou, Nikos, Pardamean, Bens, Peoples, Anita R., Pharoah, Paul D P, Platz, Elizabeth A., Rennert, Gad, Ruiz-Narvaez, Edward, Sakoda, Lori C., Scacheri, Peter C., Schmit, Stephanie L., Schoen, Robert E., Shcherbina, Anna, Slattery, Martha L., Stern, Mariana C., Su, Yu-Ru, Tangen, Catherine M., Thomas, Duncan C., Tian, Yu, Tsilidis, Konstantinos K., Ulrich, Cornelia M., van Duijnhoven, Fränzel J B, van Guelpen, Bethany, Visvanathan, Kala, Vodicka, Pavel, Cenggoro, Tjeng Wawan, Weinstein, Stephanie J., White, Emily, Wolk, Alicja, Woods, Michael O., Hsu, Li, Peters, Ulrike, Moreno, Victor, Gauderman, W. James, Carreras-Torres, Robert, Kim, Andre E., Lin, Yi, Díez-Obrero, Virginia, Bien, Stephanie A., Qu, Conghui, Wang, Jun, Dimou, Niki, Aglago, Elom K., Albanes, Demetrius, Arndt, Volker, Baurley, James W., Berndt, Sonja I., Bézieau, Stéphane, Bishop, D Timothy, Bouras, Emmanouil, Brenner, Hermann, Budiarto, Arif, Campbell, Peter T., Casey, Graham, Chan, Andrew T., Chang-Claude, Jenny, Chen, Xuechen, Conti, David V., Dampier, Christopher H., Devall, Matthew A M, Drew, David A., Figueiredo, Jane C., Gallinger, Steven, Giles, Graham G., Gruber, Stephen B., Gsur, Andrea, Gunter, Marc J., Harrison, Tabitha A., Hidaka, Akihisa, Hoffmeister, Michael, Huyghe, Jeroen R., Jenkins, Mark A., Jordahl, Kristina M., Kawaguchi, Eric, Keku, Temitope O., Kundaje, Anshul, Le Marchand, Loic, Lewinger, Juan Pablo, Li, Li, Mahesworo, Bharuno, Morrison, John L., Murphy, Neil, Nan, Hongmei, Nassir, Rami, Newcomb, Polly A., Obón-Santacana, Mireia, Ogino, Shuji, Ose, Jennifer, Pai, Rish K., Palmer, Julie R., Papadimitriou, Nikos, Pardamean, Bens, Peoples, Anita R., Pharoah, Paul D P, Platz, Elizabeth A., Rennert, Gad, Ruiz-Narvaez, Edward, Sakoda, Lori C., Scacheri, Peter C., Schmit, Stephanie L., Schoen, Robert E., Shcherbina, Anna, Slattery, Martha L., Stern, Mariana C., Su, Yu-Ru, Tangen, Catherine M., Thomas, Duncan C., Tian, Yu, Tsilidis, Konstantinos K., Ulrich, Cornelia M., van Duijnhoven, Fränzel J B, van Guelpen, Bethany, Visvanathan, Kala, Vodicka, Pavel, Cenggoro, Tjeng Wawan, Weinstein, Stephanie J., White, Emily, Wolk, Alicja, Woods, Michael O., Hsu, Li, Peters, Ulrike, Moreno, Victor, and Gauderman, W. James

Abstract

BACKGROUND: Tobacco smoking is an established risk factor for colorectal cancer. However, genetically defined population subgroups may have increased susceptibility to smoking-related effects on colorectal cancer. METHODS: A genome-wide interaction scan was performed including 33,756 colorectal cancer cases and 44,346 controls from three genetic consortia. RESULTS: Evidence of an interaction was observed between smoking status (ever vs. never smokers) and a locus on 3p12.1 (rs9880919, P = 4.58 × 10-8), with higher associated risk in subjects carrying the GG genotype [OR, 1.25; 95% confidence interval (CI), 1.20-1.30] compared with the other genotypes (OR <1.17 for GA and AA). Among ever smokers, we observed interactions between smoking intensity (increase in 10 cigarettes smoked per day) and two loci on 6p21.33 (rs4151657, P = 1.72 × 10-8) and 8q24.23 (rs7005722, P = 2.88 × 10-8). Subjects carrying the rs4151657 TT genotype showed higher risk (OR, 1.12; 95% CI, 1.09-1.16) compared with the other genotypes (OR <1.06 for TC and CC). Similarly, higher risk was observed among subjects carrying the rs7005722 AA genotype (OR, 1.17; 95% CI, 1.07-1.28) compared with the other genotypes (OR <1.13 for AC and CC). Functional annotation revealed that SNPs in 3p12.1 and 6p21.33 loci were located in regulatory regions, and were associated with expression levels of nearby genes. Genetic models predicting gene expression revealed that smoking parameters were associated with lower colorectal cancer risk with higher expression levels of CADM2 (3p12.1) and ATF6B (6p21.33). CONCLUSIONS: Our study identified novel genetic loci that may modulate the risk for colorectal cancer of smoking status and intensity, linked to tumor suppression and immune response. IMPACT: These findings can guide potential prevention treatments.

Published

2023

3. Large-scale Integrated Analysis of Genetics and Metabolomic Data Reveals Potential Links Between Lipids and Colorectal Cancer Risk

Author

Shu, Xiang, Chen, Zhishan, Long, Jirong, Guo, Xingyi, Yang, Yaohua, Qu, Conghui, Ahn, Yoon-Ok, Cai, Qiuyin, Casey, Graham, Gruber, Stephen B., Huyghe, Jeroen R., Jee, Sun Ha, Jenkins, Mark A., Jia, Wei-Hua, Jung, Keum Ji, Kamatani, Yoichiro, Kim, Dong-Hyun, Kim, Jeongseon, Kweon, Sun-Seog, Le Marchand, Loic, Matsuda, Koichi, Matsuo, Keitaro, Newcomb, Polly A., Oh, Jae Hwan, Ose, Jennifer, Oze, Isao, Pai, Rish K., Pan, Zhi-Zhong, Pharoah, Paul D.P., Playdon, Mary C., Ren, Ze-Fang, Schoen, Robert E., Shin, Aesun, Shin, Min-Ho, Shu, Xiao-Ou, Sun, Xiaohui, Tangen, Catherine M., Tanikawa, Chizu, Ulrich, Cornelia M., van Duijnhoven, Franzel J.B., van Guelpen, Bethany, Wolk, Alicja, Woods, Michael O., Wu, Anna H., Peters, Ulrike, Zheng, Wei, Shu, Xiang, Chen, Zhishan, Long, Jirong, Guo, Xingyi, Yang, Yaohua, Qu, Conghui, Ahn, Yoon-Ok, Cai, Qiuyin, Casey, Graham, Gruber, Stephen B., Huyghe, Jeroen R., Jee, Sun Ha, Jenkins, Mark A., Jia, Wei-Hua, Jung, Keum Ji, Kamatani, Yoichiro, Kim, Dong-Hyun, Kim, Jeongseon, Kweon, Sun-Seog, Le Marchand, Loic, Matsuda, Koichi, Matsuo, Keitaro, Newcomb, Polly A., Oh, Jae Hwan, Ose, Jennifer, Oze, Isao, Pai, Rish K., Pan, Zhi-Zhong, Pharoah, Paul D.P., Playdon, Mary C., Ren, Ze-Fang, Schoen, Robert E., Shin, Aesun, Shin, Min-Ho, Shu, Xiao-Ou, Sun, Xiaohui, Tangen, Catherine M., Tanikawa, Chizu, Ulrich, Cornelia M., van Duijnhoven, Franzel J.B., van Guelpen, Bethany, Wolk, Alicja, Woods, Michael O., Wu, Anna H., Peters, Ulrike, and Zheng, Wei

Abstract

Background: The etiology of colorectal cancer is not fully understood. Methods: Using genetic variants and metabolomics data including 217 metabolites from the Framingham Heart Study (n = 1,357), we built genetic prediction models for circulating metabolites. Models with prediction R2 > 0.01 (Nmetabolite = 58) were applied to predict levels of metabolites in two large consortia with a combined sample size of approximately 46,300 cases and 59,200 controls of European and approximately 21,700 cases and 47,400 controls of East Asian (EA) descent. Genetically predicted levels of metabolites were evaluated for their associations with colorectal cancer risk in logistic regressions within each racial group, after which the results were combined by meta-analysis. Results: Of the 58 metabolites tested, 24 metabolites were significantly associated with colorectal cancer risk [Benjamini-Hochberg FDR (BH-FDR) < 0.05] in the European population (ORs ranged from 0.91 to 1.06; P values ranged from 0.02 to 6.4 × 10-8). Twenty one of the 24 associations were replicated in the EA population (ORs ranged from 0.26 to 1.69, BH-FDR < 0.05). In addition, the genetically predicted levels of C16:0 cholesteryl ester was significantly associated with colorectal cancer risk in the EA population only (OREA: 1.94, 95% CI, 1.60−2.36, P = 2.6 × 10-11; OREUR: 1.01, 95% CI, 0.99−1.04, P = 0.3). Nineteen of the 25 metabolites were glycerophospholipids and triacylglycerols (TAG). Eighteen associations exhibited significant heterogeneity between the two racial groups (PEUR-EA-Het < 0.005), which were more strongly associated in the EA population. This integrative study suggested a potential role of lipids, especially certain glycerophospholipids and TAGs, in the etiology of colorectal cancer. Conclusions: This study identified potential novel risk biomarkers for colorectal cancer by integrating genetics and circulating metabolomics data. Impact: The identified metabolites could be developed

Published

2022

4. Genetic Predictors for Fecal Propionate and Butyrate-Producing Microbiome Pathway Are Not Associated with Colorectal Cancer Risk: A Mendelian Randomization Analysis.

Author

Yujia Lu, Yu Chen Zhao, Chang-Claude, Jenny, Gruber, Stephen B., Gsur, Andrea, Offit, Kenneth, Vodickova, Ludmila, Woods, Michael O., Nguyen, Long H., Wade, Kaitlin H., Carreras-Torres, Robert, Moreno, Victor, Buchanan, Daniel D., Cotterchio, Michelle, Chan, Andrew T., Phipps, Amanda I., Peters, Ulrike, and Mingyang Song

Abstract

Background: Mechanistic data indicate the benefit of short-chain fatty acids (SCFA) produced by gut microbial fermentation of fiber on colorectal cancer, but direct epidemiologic evidence is limited. A recent study identified SNPs for two SCFA traits (fecal propionate and butyrate-producing microbiome pathway PWY-5022) in Europeans and showed metabolic benefits. Methods: We conducted a two-sample Mendelian randomization analysis of the genetic instruments for the two SCFA traits (three SNPs for fecal propionate and nine for PWY-5022) in relation to colorectal cancer risk in three large European genetic consortia of 58,131 colorectal cancer cases and 67,347 controls. We estimated the risk of overall colorectal cancer and conducted subgroup analyses by sex, age, and anatomic subsites of colorectal cancer. Results: We did not observe strong evidence for an association of the genetic predictors for fecal propionate levels and the abundance of PWY-5022 with the risk of overall colorectal cancer, colorectal cancer by sex, or early-onset colorectal cancer (diagnosed at <50 years), with no evidence of heterogeneity or pleiotropy. When assessed by tumor subsites, we found weak evidence for an association between PWY-5022 and risk of rectal cancer (OR per 1-SD, 0.95; 95% confidence intervals, 0.91-0.99; P = 0.03) but it did not surpass multiple testing of subgroup analysis. Conclusions: Genetic instruments for fecal propionate levels and the abundance of PWY-5022 were not associated with colorectal cancer risk. Impact: Fecal propionate and PWY-5022 may not have a substantial influence on colorectal cancer risk. Future research is warranted to comprehensively investigate the effects of SCFA-producing bacteria and SCFAs on colorectal cancer risk. [ABSTRACT FROM AUTHOR]

Published

2023

5. Abstract 2737: Clinical and epidemiologic predictors of clonal immune responses in colorectal cancer

Author

Gruber, Stephen B., primary, Bonner, Joseph D., additional, Lindsey, Sidney S., additional, Tsai, Ya-Yu, additional, Sanz-Pamplona, Rebeca, additional, Alonso, M. Henar, additional, Melas, Marilena, additional, Rennert, Hedy S., additional, McDonnell, Kevin J., additional, Idos, Gregory E., additional, Walker, Christopher P., additional, Kast, W. Martin, additional, Da Silva, Diane, additional, Robins, Harlan S., additional, Greenson, Joel K., additional, Moreno, Victor, additional, Schmit, Stephanie L., additional, and Rennert, Gad, additional

Published

2021

6. Abstract 835: T-cell abundance, clonality and disease specific survival in colorectal cancer

Author

Bonner, Joseph, primary, Schmit, Sephanie L., additional, Lindsey, Sidney S., additional, Tsai, Ya-Yu, additional, Sanz-Pamplona, Rebeca, additional, Alonso, M. Henar, additional, Melas, Marilena, additional, Rennert, Hedy S., additional, McDonnell, Kevin J., additional, Idos, Gregory, additional, Walker, Christopher P., additional, Kast, W. Martin, additional, Da Silva, Diane, additional, Robins, Harlan S., additional, Greenson, Joel K., additional, Moreno, Victor, additional, Rennert, Gad, additional, and Gruber, Stephen B., additional

Published

2021

7. Abstract 881: Benchmarking genome-wide polygenic risk score development techniques in colorectal cancer risk prediction

Author

Thomas, Minta, primary, Sakoda, Lori C, additional, Lee, Jeffrey K, additional, Jenkins, Mark A, additional, Burnett-Hartman, Andrea, additional, Hampel, Heather, additional, Rosenthal, Elisabeth A, additional, Brenner, Hermann, additional, Chang-Claude, Jenny, additional, Gunter, Marc J, additional, Newcomb, Polly A, additional, Gallinger, Steven, additional, Harrison, Tabitha A, additional, Casey, Graham, additional, Moreno, Victor, additional, Jarvik, Gail P, additional, Gruber, Stephen B, additional, Schoen, Robert E, additional, Chan, Andrew T, additional, Hayes, Richard B, additional, Corley, Douglas A, additional, Peters, Ulrike, additional, and Hsu, Li, additional

Published

2021

8. Abstract 818: Association of polygenic risk score and menopausal hormone therapy for colorectal cancer risk

Author

Tian, Yu, primary, Lin, Yi, additional, Kim, Andre E., additional, Bien, Stephanie A., additional, Newcomb, Polly A., additional, Casey, Graham, additional, Platz, Elizabeth A., additional, Marchand, Loic Le, additional, Campbell, Peter T., additional, Brenner, Hermann, additional, Hoffmeister, Michael, additional, Guo, Feng, additional, Chen, Xuechen, additional, Gunter, Marc J., additional, Dimou, Niki, additional, Gruber, Stephen B., additional, Chan, Andrew T., additional, Joshi, Amit D., additional, Berndt, Sonja I., additional, White, Emily, additional, Moreno, Victor, additional, Prentice, Ross L., additional, Peters, Ulrike, additional, Gauderman, William, additional, Hsu, Li, additional, and Chang-Claude, Jenny, additional

Published

2021

9. Abstract 817: Probing the diabetes - colorectal cancer link using gene - environment interaction analyses

Author

Dimou, Niki, primary, Kim, Andre E., additional, Flanagan, Orlagh, additional, Murphy, Neil, additional, Bouras, Emmanouil, additional, Campbell, Peter T., additional, Casey, Graham, additional, Gallinger, Steven, additional, Gruber, Stephen B., additional, Hsu, Li, additional, Jenkins, Mark A., additional, Lin, Yi, additional, Moreno, Victor, additional, Qu, Conghui, additional, Ruiz-Narvaez, Edward, additional, Stern, Mariana C., additional, Tian, Yu, additional, Tsilidis, Kostas, additional, Gauderman, W. James, additional, Gunter, Marc J., additional, and Peters, Ulrike, additional

Published

2021

10. Abstract 824: Germline genetic regulation of the adaptive immune response in colorectal cancer

Author

Schmit, Stephanie L., primary, Tsai, Ya-Yu, additional, Bonner, Joseph, additional, Sanz-Pamplona, Rebeca, additional, Joshi, Amit D., additional, Lindsey, Sidney S., additional, Melas, Marilena, additional, McDonnell, Kevin J., additional, Idos, Gregory E., additional, Walker, Christopher P., additional, Kast, W. Martin, additional, Da Silva, Diane, additional, Ugai, Tomotaka, additional, Rennert, Hedy S., additional, Robins, Harlan S., additional, Greenson, Joel K., additional, Ogino, Shuji, additional, Moreno, Victor, additional, Rennert, Gad, additional, and Gruber, Stephen B., additional

Published

2021

11. Large-scale Integrated Analysis of Genetics and Metabolomic Data Reveals Potential Links Between Lipids and Colorectal Cancer Risk.

Author

Xiang Shu, Zhishan Chen, Jirong Long, Xingyi Guo, Yaohua Yang, Conghui Qu, Yoon-Ok Ahn, Qiuyin Cai, Casey, Graham, Gruber, Stephen B., Huyghe, Jeroen R., Sun Ha Jee, Jenkins, Mark A., Wei-Hua Jia, Keum Ji Jung, Yoichiro Kamatani, Dong-Hyun Kim, Jeongseon Kim, Sun-Seog Kweon, and Le Marchand, Loic

Abstract

Background: The etiology of colorectal cancer is not fully understood. Methods: Using genetic variants and metabolomics data including 217 metabolites from the Framingham Heart Study (n = 1,357), we built genetic prediction models for circulating metabolites. Models with prediction R2 > 0.01 (Nmetabolite = 58) were applied to predict levels of metabolites in two large consortia with a combined sample size of approximately 46,300 cases and 59,200 controls of European and approximately 21,700 cases and 47,400 controls of East Asian (EA) descent. Genetically predicted levels of metabolites were evaluated for their associations with colorectal cancer risk in logistic regressions within each racial group, after which the results were combined by meta-analysis. Results: Of the 58 metabolites tested, 24 metabolites were significantly associated with colorectal cancer risk [Benjamini-Hochberg FDR (BH-FDR) < 0.05] in the European population (ORs ranged from 0.91 to 1.06; P values ranged from 0.02 to 6.4 × 10-8). Twenty one of the 24 associations were replicated in the EA population (ORs ranged from 0.26 to 1.69, BH-FDR < 0.05). In addition, the genetically predicted levels of C16:0 cholesteryl ester was significantly associated with colorectal cancer risk in the EA population only (OREA: 1.94, 95% CI, 1.60-2.36, P = 2.6 × 10-11; OREUR: 1.01, 95% CI, 0.99-1.04, P = 0.3). Nineteen of the 25 metabolites were glycerophospholipids and triacylglycerols (TAG). Eighteen associations exhibited significant heterogeneity between the two racial groups (PEUR-EA-Het < 0.005), which were more strongly associated in the EA population. This integrative study suggested a potential role of lipids, especially certain glycerophospholipids and TAGs, in the etiology of colorectal cancer. Conclusions: This study identified potential novel risk biomarkers for colorectal cancer by integrating genetics and circulating metabolomics data. Impact: The identified metabolites could be developed into new tools for risk assessment of colorectal cancer in both European and EA populations. [ABSTRACT FROM AUTHOR]

Published

2022

12. Abstract 2332: Tumor infiltrating lymphocytes, immunoSeq, and CMS classification in the molecular epidemiology of colorectal cancer study

Author

Melas, Marilena, primary, Lazaris, Charalampos, additional, Schmit, Stephanie L., additional, Maoz, Asaf, additional, Pamplona, Rebeca Sanz, additional, Qu, Chenxu, additional, Greenson, Joel K., additional, Kuick, Rork, additional, Lejbkowicz, Flavio, additional, Rennert, Hedy S., additional, Walker, Christopher P., additional, Bowen, Chase M., additional, Silva, Diane M. Da, additional, Kast, W. Martin, additional, Idos, Gregory E., additional, McDonnell, Kevin J., additional, Moreno, Victor, additional, Rennert, Gad, additional, and Gruber, Stephen B., additional

Published

2019

13. Abstract 2685: Identification of circulating protein biomarkers for colorectal cancer risk: A genetic instrument analysis

Author

Shu, Xiang, primary, Shu, Xiao-ou, additional, Long, Jirong, additional, Cai, Qiuyin, additional, Qu, Conghui, additional, Schmit, Stephanie L., additional, Qu, Chenxu, additional, Berndt, Sonja I., additional, Campbell, Peter T., additional, Chan, Andrew T., additional, Giles, Graham G., additional, Gsur, Andrea, additional, Hoffmeister, Michael, additional, Jenkins, Mark A., additional, Markowitz, Sanford D., additional, Li, Li, additional, Rennert, Gad, additional, Offit, Kenneth, additional, Conti, David, additional, Lindblom, Annika, additional, Casey, Graham, additional, Gruber, Stephen B., additional, Peters, Ulrike, additional, and Zheng, Wei, additional

Published

2019

14. Association of Known Melanoma Risk Factors with Primary Melanoma of the Scalp and Neck.

Author

Wood, Renee P., Heyworth, Jane S., McCarthy, Nina S., Mauguen, Audrey, Berwick, Marianne, Thomas, Nancy E., Millward, Michael J., Anton-Culver, Hoda, Cust, Anne E., Dwyer, Terence, Gallagher, Richard P., Gruber, Stephen B., Kanetsky, Peter A., Orlow, Irene, Rosso, Stefano, Moses, Eric K., Begg, Colin B., and Ward, Sarah V.

Abstract

Background: Scalp and neck (SN) melanoma confers a worse prognosis than melanoma of other sites but little is known about its determinants. We aimed to identify associations between SN melanoma and known risk genes, phenotypic traits, and sun exposure patterns. Methods: Participants were cases from the Western Australian Melanoma Health Study (n = 1,200) and the Genes, Environment, and Melanoma Study (n = 3,280). Associations between risk factors and SN melanoma, compared with truncal and arm/leg melanoma, were investigated using binomial logistic regression. Facial melanoma was also compared with the trunk and extremities, to evaluate whether associations were subregion specific, or reflective of the whole head/neck region. Results: Compared with other sites, increased odds of SN and facial melanoma were observed in older individuals [SN: OR = 1.28, 95% confidence interval (CI) = 0.92-1.80, Ptrend = 0.016; Face: OR = 4.57, 95% CI = 3.34-6.35, Ptrend < 0.001] and those carrying IRF4-rs12203592*T (SN: OR = 1.35, 95% CI = 1.12-1.63, Ptrend = 0.002; Face: OR = 1.29, 95% CI = 1.10-1.50, Ptrend = 0.001). Decreased odds were observed for females (SN: OR = 0.49, 95% CI = 0.37-0.64, P < 0.001; Face: OR = 0.66, 95% CI = 0.53-0.82, P < 0.001) and the presence of nevi (SN: OR = 0.66, 95% CI = 0.49-0.89, P = 0.006; Face: OR = 0.65, 95% CI = 0.52-0.83, P < 0.001). Conclusions: Differences observed between SN melanoma and other sites were also observed for facial melanoma. Factors previously associated with the broader head and neck region, notably older age, may be driven by the facial subregion. A novel finding was the association of IRF4-rs12203592 with both SN and facial melanoma. [ABSTRACT FROM AUTHOR]

Published

2020

15. Exploratory Genome-Wide Interaction Analysis of Nonsteroidal Anti-inflammatory Drugs and Predicted Gene Expression on Colorectal Cancer Risk.

Author

Xiaoliang Wang, Yu-Ru Su, Petersen, Paneen S., Bien, Stephanie, Schmit, Stephanie L., Drew, David A., Albanes, Demetrius, Berndt, Sonja I., Brenner, Hermann, Campbell, Peter T., Casey, Graham, Chang-Claude, Jenny, Gallinger, Steven J., Gruber, Stephen B., Haile, Robert W., Harrison, Tabitha A., Hoffmeister, Michael, Jacobs, Eric J., Jenkins, Mark A., and Joshi, Amit D.

Abstract

Background: Regular use of nonsteroidal anti-inflammatory drugs (NSAID) is associated with lower risk of colorectal cancer. Genome-wide interaction analysis on single variants (G × E) has identified several SNPs that may interact with NSAIDs to confer colorectal cancer risk, but variations in gene expression levels may also modify the effect of NSAID use. Therefore, we tested interactions between NSAID use and predicted gene expression levels in relation to colorectal cancer risk. Methods: Genetically predicted gene expressions were tested for interaction with NSAID use on colorectal cancer risk among 19,258 colorectal cancer cases and 18,597 controls from 21 observational studies. A Mixed Score Test for Interactions (MiSTi) approach was used to jointly assess G × E effects which are modeled via fixed interaction effects of the weighted burden within each gene set (burden) and residual G × E effects (variance). A false discovery rate (FDR) at 0.2 was applied to correct for multiple testing. Results: Among the 4,840 genes tested, genetically predicted expression levels of four genes modified the effect of any NSAID use on colorectal cancer risk, including DPP10 (PG×E = 1.96 × 10-4), KRT16 (PG×E = 2.3 × 10-4), CD14 (PG×E = 9.38 × 10-4), and CYP27A1 (PG×E = 1.44 × 10-3). There was a significant interaction between expression level of RP11-89N17 and regular use of aspirin only on colorectal cancer risk (PG×E = 3.23 × 10-5). No interactions were observed between predicted gene expression and nonaspirin NSAID use at FDR < 0.2. Conclusions: By incorporating functional information, we discovered several novel genes that interacted with NSAID use. [ABSTRACT FROM AUTHOR]

Published

2020

16. Abstract 4746: Microbes in the tumor microenvironment: Bacterial influences on host immunity in colorectal cancer

Author

Pierce, Christine M., primary, Hong, Bo-young, additional, Hoehn, Hannah J., additional, Gomez, Maria F., additional, Melas, Marilena, additional, McDonnell, Kevin, additional, Kim, Youngchul, additional, Sodergren, Erica, additional, Weinstock, George, additional, Rennert, Hedy S., additional, Giordano, Thomas, additional, Greenson, Joel, additional, Rennert, Gad, additional, Gruber, Stephen B., additional, and Schmit, Stephanie L., additional

Published

2018

17. Abstract 1304: The contribution of rare and low-frequency variants to colorectal cancer heritability

Author

Huyghe, Jeroen R., primary, Chen, Sai, additional, Kang, Hyun M., additional, Harrison, Tabitha, additional, Berndt, Sonja I., additional, Bézieau, Stephane, additional, Brenner, Hermann, additional, Casey, Graham, additional, Chan, Andrew T., additional, Chang-Claude, Jenny, additional, Gallinger, Steven J., additional, Gruber, Stephen B., additional, Gsur, Andrea, additional, Hoffmeister, Michael, additional, Hudson, Thomas, additional, Jenkins, Mark A., additional, Marchand, Loic Le, additional, Newcomb, Polly A., additional, Potter, John D., additional, Qu, Conghui, additional, Slattery, Martha L., additional, Smith, Joshua D., additional, White, Emily, additional, Abecasis, Goncalo R., additional, Hsu, Li, additional, Nickerson, Deborah A., additional, and Peters, Ulrike, additional

Published

2017

18. Abstract LB-161: GAME-ON and OncoArray: Understanding the genetic architecture of cancer risk

Author

Nelson, Stefanie A., primary, Caga-Anan, Charlisse, additional, Daee, Danielle, additional, Costello, Maura Kate, additional, Seminara, Daniela, additional, Amos, Christopher I., additional, Gruber, Stephen B., additional, Haiman, Christopher, additional, Hunter, David, additional, Kraft, Peter, additional, Sellers, Thomas, additional, and Gillanders, Elizabeth M., additional

Published

2017

19. Abstract 491: Elucidatingde novoPATRR-mediated t(3;8) balanced translocation and clear cell renal cell carcinoma

Author

Melas, Marilena, primary, McDonnell, Kevin J., additional, Edlund, Christopher K., additional, Tash, Sarah J., additional, Sturgeon, Duveen Y., additional, Qu, Chenxu, additional, Lazaris, Charalampos, additional, Gruber, Peter J., additional, Glover, Thomas W., additional, Emanuel, Beverly S., additional, and Gruber, Stephen B., additional

Published

2017

20. Abstract 1300: Genetic predictors of gene expression associated with risk of colorectal cancer

Author

Bien, Stephanie A., primary, Guo, Xingyi, additional, Su, Yu-Ru, additional, Harrison, Tabitha A., additional, Qu, Conghui, additional, Lu, Yingchang, additional, Long, Jiron, additional, Chen, Sai, additional, Chan, Andrew T., additional, Conti, David V., additional, Kang, Hyun M., additional, Hoffmeister, Michael, additional, Hudson, Thomas J., additional, Jenkins, Mark A., additional, Marchand, Loic Le, additional, Newcomb, Polly A., additional, Slattery, Martha L., additional, White, Emily, additional, Abeçasis, Goncalo R., additional, Gruber, Stephen B., additional, Nickerson, Deborah A., additional, Schmit, Stephanie L., additional, Casey, Graham, additional, Hsu, Li, additional, Zheng, Wei, additional, and Peters, Ulrike, additional

Published

2017

21. Abstract PR17: Comprehensive colorectal cancer risk prediction to inform personalized screening and intervention

Author

Jeon, Jihyoun, primary, Berndt, Sonja I., additional, Brenner, Hermann, additional, Campbell, Peter T., additional, Chan, Andrew T., additional, Chang-Claude, Jenny, additional, Du, Mengmeng, additional, Giles, Graham, additional, Gong, Jian, additional, Gruber, Stephen B., additional, Harrison, Tabitha A., additional, Hoffmeister, Michael, additional, LeMarchand, Loic, additional, Li, Li, additional, Potter, John D., additional, Rennert, Gad, additional, Schoen, Robert E., additional, Slattery, Martha L., additional, White, Emily, additional, Woods, Michael O., additional, Peters, Ulrike, additional, and Hsu, Li, additional

Published

2017

22. Abstract B17: Comprehensive colorectal cancer risk prediction to inform personalized screening and intervention

Author

Jeon, Jihyoun, primary, Berndt, Sonja I., additional, Brenner, Hermann, additional, Campbell, Peter T., additional, Chan, Andrew T., additional, Chang-Claude, Jenny, additional, Du, Mengmeng, additional, Giles, Graham, additional, Gong, Jian, additional, Gruber, Stephen B., additional, Harrison, Tabitha A., additional, Hoffmeister, Michael, additional, LeMarchand, Loic, additional, Li, Li, additional, Potter, John D., additional, Rennert, Gad, additional, Schoen, Robert E., additional, Slattery, Martha L., additional, White, Emily, additional, Woods, Michael O., additional, Peters, Ulrike, additional, and Hsu, Li, additional

Published

2017

23. Abstract 5230: Large scale whole genome sequencing with imputation into GWAS improves our understanding of the genetic architecture of colorectal cancer

Author

Huyghe, Jeroen, primary, Chen, Sai, additional, Kang, Hyun M., additional, Harrison, Tabitha A., additional, Berndt, Sonja I., additional, Bézieau, Stephane, additional, Brenner, Hermann, additional, Casey, Graham, additional, Chan, Andrew T., additional, Chang-Claude, Jenny, additional, Steven, Gallinger J., additional, Gruber, Stephen B., additional, Gsur, Andrea, additional, Hoffmeister, Michael, additional, Hudson, Thomas J., additional, Le Marchand, Loic, additional, Newcomb, Polly A., additional, Potter, John D., additional, Qu, Conghui, additional, Slattery, Martha L., additional, Smith, Joshua D., additional, White, Emily, additional, Hsu, Li, additional, Abecasis, Goncalo R., additional, Nickerson, Deborah A., additional, and Peters, Ulrike, additional

Published

2016

24. Abstract 1622: Assessment of candidate host “progression genes” in the development of advanced colorectal cancer

Author

Cohen, Stacey A., primary, Qu, Conghui, additional, Harrison, Tabitha A., additional, Hsu, Li, additional, Newcomb, Polly A., additional, Gruber, Stephen B., additional, Bezieau, Stephane, additional, Casey, Graham, additional, Chan, Andrew T., additional, Chang-Claude, Jenny, additional, Slattery, Martha L., additional, White, Emily, additional, Vargas, Ashley J., additional, Nassir, Rami, additional, Peters, Ulrike, additional, and Grady, William M., additional

Published

2016

25. Abstract 2587: Comprehensive colorectal cancer risk prediction to inform personalized screening and intervention

Author

Jeon, Jihyoun, primary, Berndt, Sonja I., additional, Brenner, Hermann, additional, Campbell, Peter T., additional, Chan, Andrew T., additional, Chang-Claude, Jenny, additional, Du, Mengmeng, additional, Giles, Graham, additional, Gong, Jian, additional, Gruber, Stephen B., additional, Harrison, Tabitha A., additional, Hoffmeister, Michael, additional, LeMarchand, Loic, additional, Li, Li, additional, Potter, John D., additional, Rennert, Gad, additional, Schoen, Robert E., additional, Slattery, Martha L., additional, White, Emily, additional, Woods, Michael O., additional, Peters, Ulrike, additional, and Hsu, Li, additional

Published

2016

26. Abstract 4489: Using functional data from Roadmap Epigenomics to inform analysis of rare variants linked to gene expression in a large colorectal cancer study

Author

Bien, Stephanie A., primary, Harrison, Tabitha A., additional, Auer, Paul L., additional, Qu, Flora, additional, Huyghe, Jeroen, additional, Banbury, Barbara, additional, Greenside, Peyton, additional, Abecasis, Goncalo R., additional, Berndt, Sonja I., additional, Bézieau, Stephane, additional, Brenner, Hermann, additional, Casey, Graham, additional, Chan, Andrew T., additional, Chang-Claude, Jenny, additional, Chen, Sai, additional, Smith, Joshua D., additional, Le Marchand, Loic, additional, Carlson, Christopher, additional, Newcomb, Polly A., additional, Fuchsberger, Christian, additional, Slattery, Marty L., additional, Kang, Hyun M., additional, White, Emily, additional, Potter, John, additional, Gallinger, Steven J., additional, Hoffmeister, Michael, additional, Gruber, Stephen B., additional, Nickerson, Deborah A., additional, Peters, Ulrike, additional, Kundaje, Anshul, additional, and Hsu, Li, additional

Published

2016

27. Abstract LB-372: Robust targeted sequencing strategy identifies highly penetrant mutations in hereditary colorectal cancer cases from Colon Cancer Family Registry

Author

Raskin, Leon, primary, Guo, Yan, additional, Gruber, Stephen B., additional, and Buchanan, Daniel D., additional

Published

2016

28. Abstract 2745: Exome sequencing analysis of 41 patients with Familial Colorectal Cancer Type X (FCCTX)

Author

Melas, Marilena, primary, Luu, Hung N., additional, Rennert, Gad, additional, Lejbkowicz, Flavio, additional, Gruber, Stephen B., additional, Wiesner, Georgia L., additional, and Raskin, Leon, additional

Published

2015

29. Quantifying the Genetic Correlation between Multiple Cancer Types.

Author

Lindström, Sara, Finucane, Hilary, Bulik-Sullivan, Brendan, Schumacher, Fredrick R., Amos, Christopher I., Hung, Rayjean J., Rand, Kristin, Gruber, Stephen B., Conti, David, Permuth, Jennifer B., Hui-Yi Lin, Goode, Ellen L., Sellers, Thomas A., Amundadottir, Laufey T., Stolzenberg-Solomon, Rachael, Klein, Alison, Petersen, Gloria, Risch, Harvey, Wolpin, Brian, and Li Hsu

Abstract

Background: Many cancers share specific genetic risk factors, including both rare high-penetrance mutations and common SNPs identified through genome-wide association studies (GWAS). However, little is known about the overall shared heritability across cancers. Quantifying the extent to which two distinct cancers share genetic origin will give insights to shared biological mechanisms underlying cancer and inform design for future genetic association studies. Methods: In this study, we estimated the pair-wise genetic correlation between six cancer types (breast, colorectal, lung, ovarian, pancreatic, and prostate) using cancer-specific GWAS summary statistics data based on 66,958 case and 70,665 control subjects of European ancestry. We also estimated genetic correlations between cancers and 14 noncancer diseases and traits. Results: After adjusting for 15 pair-wise genetic correlation tests between cancers, we found significant (P < 0.003) genetic correlations between pancreatic and colorectal cancer (rg = 0.55, P = 0.003), lung and colorectal cancer (rg = 0.31, P = 0.001). We also found suggestive genetic correlations between lung and breast cancer (rg = 0.27, P = 0.009), and colorectal and breast cancer (rg = 0.22, P = 0.01). In contrast, we found no evidence that prostate cancer shared an appreciable proportion of heritability with other cancers. After adjusting for 84 tests studying genetic correlations between cancer types and other traits (Bonferroni-corrected P value: 0.0006), only the genetic correlation between lung cancer and smoking remained significant (rg = 0.41, P = 1.03 × 10-6). We also observed nominally significant genetic correlations between body mass index and all cancers except ovarian cancer. Conclusions: Our results highlight novel genetic correlations and lend support to previous observational studies that have observed links between cancers and risk factors. Impact: This study demonstrates modest genetic correlations between cancers; in particular, breast, colorectal, and lung cancer share some degree of genetic basis. [ABSTRACT FROM AUTHOR]

Published

2017

30. The OncoArray Consortium: A Network for Understanding the Genetic Architecture of Common Cancers.

Author

Amos, Christopher I., Dennis, Joe, Zhaoming Wang, Jinyoung Byun, Schumacher, Fredrick R., Gayther, Simon A., Casey, Graham, Hunter, David J., Sellers, Thomas A., Gruber, Stephen B., Dunning, Alison M., Michailidou, Kyriaki, Fachal, Laura, Doheny, Kimberly, Spurdle, Amanda B., Yafang Li, Xiangjun Xiao, Romm, Jane, Pugh, Elizabeth, and Coetzee, Gerhard A.

Abstract

Background: Common cancers develop through a multistep process often including inherited susceptibility. Collaboration among multiple institutions, and funding from multiple sources, has allowed the development of an inexpensive genotyping microarray, the OncoArray. The array includes a genome-wide backbone, comprising 230,000 SNPs tagging most common genetic variants, together with dense mapping of known susceptibility regions, rare variants from sequencing experiments, pharmacogenetic markers, and cancer-related traits. Methods: The OncoArray can be genotyped using a novel technology developed by Illumina to facilitate efficient genotyping. The consortium developed standard approaches for selecting SNPs for study, for quality control of markers, and for ancestry analysis. The array was genotyped at selected sites and with prespecified replicate samples to permit evaluation of genotyping accuracy among centers and by ethnic background. Results: The OncoArray consortium genotyped 447,705 samples. A total of 494,763 SNPs passed quality control steps with a sample success rate of 97% of the samples. Participating sites performed ancestry analysis using a common set of markers and a scoring algorithm based on principal components analysis. Conclusions: Results from these analyses will enable researchers to identify new susceptibility loci, perform fine-mapping of new or known loci associated with either single or multiple cancers, assess the degree of overlap in cancer causation and pleiotropic effects of loci that have been identified for disease-specific risk, and jointly model genetic, environmental, and lifestyle-related exposures. Impact: Ongoing analyses will shed light on etiology and risk assessment for many types of cancer. [ABSTRACT FROM AUTHOR]

Published

2017

31. Coffee Consumption and the Risk of Colorectal Cancer.

Author

Schmit, Stephanie L., Rennert, Hedy S., Rennert, Gad, and Gruber, Stephen B.

Abstract

Background: Coffee contains several bioactive compounds relevant to colon physiology. Although coffee intake is a proposed protective factor for colorectal cancer, current evidence remains inconclusive. Methods: We investigated the association between coffee consumption and risk of colorectal cancer in 5,145 cases and 4,097 controls from the Molecular Epidemiology of Colorectal Cancer (MECC) study, a population-based case-control study in northern Israel. We also examined this association by type of coffee, by cancer site (colon and rectum), and by ethnic subgroup (Ashkenazi Jews, Sephardi Jews, and Arabs). Coffee data were collected by interview using a validated, semi-quantitative food frequency questionnaire. Results: Coffee consumption was associated with 26% lower odds of developing colorectal cancer [OR (drinkers vs. non-drinkers), 0.74; 95% confidence interval (CI), 0.64-0.86; P < 0.001]. The inverse association was also observed for decaffeinated coffee consumption alone (OR, 0.82; 95% CI, 0.68-0.99; P = 0.04) and for boiled coffee (OR, 0.82; 95% CI, 0.71-0.94; P = 0.004). Increasing consumption of coffee was associated with lower odds of developing colorectal cancer. Compared with <1 serving/day, intake of 1 to <2 servings/day (OR, 0.78; 95% CI, 0.68-0.90; P < 0.001), 2 to 2.5 servings/day (OR, 0.59; 95% CI, 0.51-0.68; P < 0.001), and >2.5 servings/day (OR, 0.46; 95% CI, 0.39-0.54; P < 0.001) were associated with significantly lower odds of colorectal cancer (Ptrend < 0.001), and the dose-response trend was statistically significant for both colon and rectal cancers. Conclusions: Coffee consumption may be inversely associated with risk of colorectal cancer in a dose-response manner. Impact: Global coffee consumption patterns suggest potential health benefits of the beverage for reducing the risk of colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2016

32. A Cross-Cancer Genetic Association Analysis of the DNA Repair and DNA Damage Signaling Pathways for Lung, Ovary, Prostate, Breast, and Colorectal Cancer.

Author

Scarbrough, Peter M., Weber, Rachel Palmieri, Iversen, Edwin S., Brhane, Yonathan, Amos, Christopher I., Kraft, Peter, Hung, Rayjean J., Sellers, Thomas A., Witte, John S., Pharoah, Paul, Henderson, Brian E., Gruber, Stephen B., Hunter, David J., Garber, Judy E., Joshi, Amit D., McDonnell, Kevin, Easton, Doug F., Eeles, Ros, Kote-Jarai, Zsofia, and Muir, Kenneth

Abstract

Background: DNA damage is an established mediator of carcinogenesis, although genome-wide association studies (GWAS) have identified few significant loci. This cross-cancer site, pooled analysis was performed to increase the power to detect common variants of DNA repair genes associated with cancer susceptibility. Methods: We conducted a cross-cancer analysis of 60,297 single nucleotide polymorphisms, at 229 DNA repair gene regions, using data from the NCI Genetic Associations and Mechanisms in Oncology (GAME-ON) Network. Our analysis included data from 32 GWAS and 48,734 controls and 51,537 cases across five cancer sites (breast, colon, lung, ovary, and prostate). Because of the unavailability of individual data, data were analyzed at the aggregate level. Meta-analysis was performed using the Association analysis for SubSETs (ASSET) software. To test for genetic associations that might escape individual variant testing due to small effect sizes, pathway analysis of eight DNA repair pathways was performed using hierarchical modeling. Results: We identified three susceptibility DNA repair genes, RAD51B (P < 5.09 × 10-6), MSH5 (P < 5.09 × 10-6), and BRCA2 (P = 5.70 × 10-6). Hierarchical modeling identified several pleiotropic associations with cancer risk in the base excision repair, nucleotide excision repair, mismatch repair, and homologous recombination pathways. Conclusions: Only three susceptibility loci were identified, which had all been previously reported. In contrast, hierarchical modeling identified several pleiotropic cancer risk associations in key DNA repair pathways. Impact: Results suggest that many common variants in DNA repair genes are likely associated with cancer susceptibility through small effect sizes that do not meet stringent significance testing criteria [ABSTRACT FROM AUTHOR]

Published

2016

33. Inherited Genetic Variants Associated with Occurrence of Multiple Primary Melanoma.

Author

Gibbs, David C., Orlow, Irene, Kanetsky, Peter A., Li Luo, Kricker, Anne, Armstrong, Bruce K., Anton-Culver, Hoda, Gruber, Stephen B., Marrett, Loraine D., Gallagher, Richard P., Zanetti, Roberto, Rosso, Stefano, Dwyer, Terence, Sharma, Ajay, La Pilla, Emily, From, Lynn, Busam, Klaus J., Cust, Anne E., Ollila, David W., and Begg, Colin B.

Abstract

The article discusses research on inherited genetic variants such as TYRP1 (Tyrosinase-related protein 1 gene) associated with multiple primary melanoma. Topics discussed include determining genetic predisposition for multiple primary melanoma in the Genes, Environment, and Melanoma Study. Topics discussed include assessment of effects of single nucleotide proteins, evidences for relevance of genetic regions to melanoma risk, and magnitude of genetic effect on development of primary melanoma.

Published

2015

34. MicroRNA Polymorphisms and Risk of Colorectal Cancer.

Author

Schmit, Stephanie L., Gollub, Jeremy, Shapero, Michael H., Shu-Chen Huang, Rennert, Hedy S., Finn, Andrea, Rennert, Gad, and Gruber, Stephen B.

Abstract

The article presents study on the contribution of micro ribonucleic acid (miRNA)-related polymorphisms to the etiology of colorectal cancer across the genome, using the Axiom miRNA Target Site Genotyping Array. It mentions that miRNAs act in post-transcriptional regulation of gene expression and genetic variation in miRNA-encoding sequences may affect the fidelity of the miRNA-mRNA interaction. It adds association of marker and colorectal cancer was examined using logistic regression.

Published

2015

35. Sun Exposure and Melanoma Survival: A GEM Study.

Author

Berwick, Marianne, Reiner, Anne S., Paine, Susan, Armstrong, Bruce K., Kricker, Anne, Goumas, Chris, Cust, Anne E., Thomas, Nancy E., Groben, Pamela A., From, Lynn, Busam, Klaus, Orlow, Irene, Marrett, Loraine D., Gallagher, Richard P., Gruber, Stephen B., Anton-Culver, Hoda, Rosso, Stefano, Zanetti, Roberto, Kanetsky, Peter A., and Dwyer, Terry

Abstract

The article discusses a study which aims to evaluate the hypothesis of association of sun exposure with greater survival in a larger, international population. Topics discussed include evidence for less effect on survival with melanoma with sun exposure before melanoma diagnosis, role of ultra violet radiation exposure in the development of melanoma, and better effects of sunny vacations before diagnosis which causes melanoma-specific survival.

Published

2014

36. Disclosing Individual CDKN2A Research Results to Melanoma Survivors: Interest, Impact, and Demands on Researchers.

Author

Christensen, Kurt D., Roberts, J. Scott, Shalowitz, David I., Everett, Jessica N., Kim, Scott Y. H., Raskin, Leon, and Gruber, Stephen B.

Abstract

The article discusses the impact of disclosing research results to participants of the 2008 Genetics, Environment and Melanoma (GEM) Study. Results of cyclin-dependent kinase inhibitor type 2A (CDKN2A) gene test and melanoma susceptibility were disclosed by telephone and followed for three months. That participation in future research is likely with disclosure despite potential challenges for investigators is emphasized. Participants reportedly did not exhibit evidence of psychological harm from disclosure and responded positively to the information.

Published

2011

37. Smoking, Gender, and Ethnicity Predict Somatic BRAF Mutations in Colorectal Cancer.

Author

Rozek, Laura S., Herron, Casey M., Greenson, Joel K., Moreno, Victor, Capella, Gabriel, Rennert, Gad, and Gruber, Stephen B.

Abstract

The article discusses a study that measured the prevalence and epidemiologic correlates of the B-Raf proto-oncogene serine/threonine-protein kinase (BRAF) V600E somatic mutation in cases collected as part of a population-based case-control study of colorectal cancer (CRC) in northern Israel. It examined whether gender, smoking and ethnicity predict somatic BRAF mutations in colorectal cancer. The study found that Israel has lower prevalence of BRAF V600E mutation than other Western populations.

Published

2010

38. Recreational Physical Activity Modifies the Association Between a Common GH1 Polymorphism and Colorectal Cancer Risk.

Author

Khoury-Shakour, Sana, Gruber, Stephen B., Lejbkowicz, Flavio, Rennert, Hedy S., Raskin, Leon, Pinchev, Mila, and Rennert, Gad

Abstract

The article investigates the association of the GH1 gene polymorphism with colorectal cancer risk in a case-control study. According to the authors, they found that the A allele of the polymorphism is associated with reduced risk of colorectal cancer only among physically inactive individuals, indicating an interaction between physical activity and the growth hormone/insulin-like growth factor-I system.

Published

2008

39. PTPRJ Haplotypes and Colorectal Cancer Risk.

Author

Toland, Amanda E., Rozek, Laura S., Presswala, Shafaq, Rennert, Gad, and Gruber, Stephen B.

Abstract

The article presents a study which examined PTPRJ, a candidate gene for mouse locus sustainability to colorectal cancer (CRC). It genotyped a variant, rs1566734 and six additional PTPRJ haplotype tagging single nucleotide polymorphisms (SNP) in CRC cases and case controls study of the Molecular Epidemiology of Colorectal Cancer, to examine if variants or haplotype in PTPRJ confer protective or risk effect for CRC. It concludes that variant or haplotypes in PTPRJ has no significant effect on CRC.

Published

2008

40. FGFR2 Is a Breast Cancer Susceptibility Gene in Jewish and Arab Israeli Populations.

Author

Raskin, Leon, Pinchev, Mila, Arad, Chana, Lejbkowicz, Flavio, Tamir, Ada, Rennert, Hedy S., Rennert, Gad, and Gruber, Stephen B.

Abstract

The article reports on the study which investigates the relative risk and contribution of fibroblast growth factor receptor 2 (FGFR2) to breast cancer risk in ethnic groups within Jewish and Arab Israeli populations. The study revealed a significant associations between breast cancer risk and single nucleotide polymorphisms. It is indicated that the genetic variation in FGFR2 may account for a substantial fraction of breast cancer in Arab, Ashkenazi and Sephardi Jewish populations.

Published

2008

41. Large-Scale Alternative Polyadenylation-Wide Association Studies to Identify Putative Cancer Susceptibility Genes.

Author

Guo X, Ping J, Yang Y, Su X, Shu XO, Wen W, Chen Z, Zhang Y, Tao R, Jia G, He J, Cai Q, Zhang Q, Giles GG, Pearlman R, Rennert G, Vodicka P, Phipps A, Gruber SB, Casey G, Peters U, Long J, Lin W, and Zheng W

Subjects

Humans, Quantitative Trait Loci, Polymorphism, Single Nucleotide, Female, Male, Gene Expression Regulation, Neoplastic, RNA, Messenger genetics, RNA, Messenger metabolism, Cell Line, Tumor, Genetic Predisposition to Disease, Polyadenylation, Genome-Wide Association Study, Neoplasms genetics, 3' Untranslated Regions genetics

Abstract

Alternative polyadenylation (APA) modulates mRNA processing in the 3'-untranslated regions (3' UTR), affecting mRNA stability and translation efficiency. Research into genetically regulated APA has the potential to provide insights into cancer risk. In this study, we conducted large APA-wide association studies to investigate associations between APA levels and cancer risk. Genetic models were built to predict APA levels in multiple tissues using genotype and RNA sequencing data from 1,337 samples from the Genotype-Tissue Expression project. Associations of genetically predicted APA levels with cancer risk were assessed by applying the prediction models to data from large genome-wide association studies of six common cancers among European ancestry populations: breast, ovarian, prostate, colorectal, lung, and pancreatic cancers. A total of 58 risk genes (corresponding to 76 APA sites) were associated with at least one type of cancer, including 25 genes previously not linked to cancer susceptibility. Of the identified risk APAs, 97.4% and 26.3% were supported by 3'-UTR APA quantitative trait loci and colocalization analyses, respectively. Luciferase reporter assays for four selected putative regulatory 3'-UTR variants demonstrated that the risk alleles of 3'-UTR variants, rs324015 (STAT6), rs2280503 (DIP2B), rs1128450 (FBXO38), and rs145220637 (LDHA), significantly increased the posttranscriptional activities of their target genes compared with reference alleles. Furthermore, knockdown of the target genes confirmed their ability to promote proliferation and migration. Overall, this study provides insights into the role of APA in the genetic susceptibility to common cancers. Significance: Systematic evaluation of associations of alternative polyadenylation with cancer risk reveals 58 putative susceptibility genes, highlighting the contribution of genetically regulated alternative polyadenylation of 3'UTRs to genetic susceptibility to cancer., (©2024 American Association for Cancer Research.)

Published

2024

42. Epidemiologic Factors in Relation to Colorectal Cancer Risk and Survival by Genotoxic Colibactin Mutational Signature.

Author

Thomas CE, Georgeson P, Qu C, Steinfelder RS, Buchanan DD, Song M, Harrison TA, Um CY, Hullar MA, Jenkins MA, Van Guelpen B, Lynch BM, Melaku YA, Huyghe JR, Aglago EK, Berndt SI, Boardman LA, Campbell PT, Cao Y, Chan AT, Drew DA, Figueiredo JC, French AJ, Giannakis M, Goode EL, Gruber SB, Gsur A, Gunter MJ, Hoffmeister M, Hsu L, Huang WY, Moreno V, Murphy N, Newcomb PA, Newton CC, Nowak JA, Obón-Santacana M, Ogino S, Sun W, Toland AE, Trinh QM, Ugai T, Zaidi SH, Peters U, and Phipps AI

Subjects

Humans, DNA Damage, Epidemiologic Factors, Risk Factors, Microsatellite Instability, Colorectal Neoplasms epidemiology, Colorectal Neoplasms genetics, Peptides, Polyketides

Abstract

Background: The genotoxin colibactin causes a tumor single-base substitution (SBS) mutational signature, SBS88. It is unknown whether epidemiologic factors' association with colorectal cancer risk and survival differs by SBS88., Methods: Within the Genetic Epidemiology of Colorectal Cancer Consortium and Colon Cancer Family Registry, we measured SBS88 in 4,308 microsatellite stable/microsatellite instability low tumors. Associations of epidemiologic factors with colorectal cancer risk by SBS88 were assessed using multinomial regression (N = 4,308 cases, 14,192 controls; cohort-only cases N = 1,911), and with colorectal cancer-specific survival using Cox proportional hazards regression (N = 3,465 cases)., Results: 392 (9%) tumors were SBS88 positive. Among all cases, the highest quartile of fruit intake was associated with lower risk of SBS88-positive colorectal cancer than SBS88-negative colorectal cancer [odds ratio (OR) = 0.53, 95% confidence interval (CI) 0.37-0.76; OR = 0.75, 95% CI 0.66-0.85, respectively, Pheterogeneity = 0.047]. Among cohort studies, associations of body mass index (BMI), alcohol, and fruit intake with colorectal cancer risk differed by SBS88. BMI ≥30 kg/m2 was associated with worse colorectal cancer-specific survival among those SBS88-positive [hazard ratio (HR) = 3.40, 95% CI 1.47-7.84], but not among those SBS88-negative (HR = 0.97, 95% CI 0.78-1.21, Pheterogeneity = 0.066)., Conclusions: Most epidemiologic factors did not differ by SBS88 for colorectal cancer risk or survival. Higher BMI may be associated with worse colorectal cancer-specific survival among those SBS88-positive; however, validation is needed in samples with whole-genome or whole-exome sequencing available., Impact: This study highlights the importance of identification of tumor phenotypes related to colorectal cancer and understanding potential heterogeneity for risk and survival., (©2024 American Association for Cancer Research.)

Published

2024

43. Genome-Wide Gene-Environment Interaction Analyses to Understand the Relationship between Red Meat and Processed Meat Intake and Colorectal Cancer Risk.

Author

Stern MC, Sanchez Mendez J, Kim AE, Obón-Santacana M, Moratalla-Navarro F, Martín V, Moreno V, Lin Y, Bien SA, Qu C, Su YR, White E, Harrison TA, Huyghe JR, Tangen CM, Newcomb PA, Phipps AI, Thomas CE, Kawaguchi ES, Lewinger JP, Morrison JL, Conti DV, Wang J, Thomas DC, Platz EA, Visvanathan K, Keku TO, Newton CC, Um CY, Kundaje A, Shcherbina A, Murphy N, Gunter MJ, Dimou N, Papadimitriou N, Bézieau S, van Duijnhoven FJB, Männistö S, Rennert G, Wolk A, Hoffmeister M, Brenner H, Chang-Claude J, Tian Y, Le Marchand L, Cotterchio M, Tsilidis KK, Bishop DT, Melaku YA, Lynch BM, Buchanan DD, Ulrich CM, Ose J, Peoples AR, Pellatt AJ, Li L, Devall MAM, Campbell PT, Albanes D, Weinstein SJ, Berndt SI, Gruber SB, Ruiz-Narvaez E, Song M, Joshi AD, Drew DA, Petrick JL, Chan AT, Giannakis M, Peters U, Hsu L, and Gauderman WJ

Subjects

Humans, Gene-Environment Interaction, Meat adverse effects, Risk Factors, Red Meat adverse effects, Colorectal Neoplasms genetics

Abstract

Background: High red meat and/or processed meat consumption are established colorectal cancer risk factors. We conducted a genome-wide gene-environment (GxE) interaction analysis to identify genetic variants that may modify these associations., Methods: A pooled sample of 29,842 colorectal cancer cases and 39,635 controls of European ancestry from 27 studies were included. Quantiles for red meat and processed meat intake were constructed from harmonized questionnaire data. Genotyping arrays were imputed to the Haplotype Reference Consortium. Two-step EDGE and joint tests of GxE interaction were utilized in our genome-wide scan., Results: Meta-analyses confirmed positive associations between increased consumption of red meat and processed meat with colorectal cancer risk [per quartile red meat OR = 1.30; 95% confidence interval (CI) = 1.21-1.41; processed meat OR = 1.40; 95% CI = 1.20-1.63]. Two significant genome-wide GxE interactions for red meat consumption were found. Joint GxE tests revealed the rs4871179 SNP in chromosome 8 (downstream of HAS2); greater than median of consumption ORs = 1.38 (95% CI = 1.29-1.46), 1.20 (95% CI = 1.12-1.27), and 1.07 (95% CI = 0.95-1.19) for CC, CG, and GG, respectively. The two-step EDGE method identified the rs35352860 SNP in chromosome 18 (SMAD7 intron); greater than median of consumption ORs = 1.18 (95% CI = 1.11-1.24), 1.35 (95% CI = 1.26-1.44), and 1.46 (95% CI = 1.26-1.69) for CC, CT, and TT, respectively., Conclusions: We propose two novel biomarkers that support the role of meat consumption with an increased risk of colorectal cancer., Impact: The reported GxE interactions may explain the increased risk of colorectal cancer in certain population subgroups., (©2023 American Association for Cancer Research.)

Published

2024

44. A Genetic Locus within the FMN1/GREM1 Gene Region Interacts with Body Mass Index in Colorectal Cancer Risk.

Author

Aglago EK, Kim A, Lin Y, Qu C, Evangelou M, Ren Y, Morrison J, Albanes D, Arndt V, Barry EL, Baurley JW, Berndt SI, Bien SA, Bishop DT, Bouras E, Brenner H, Buchanan DD, Budiarto A, Carreras-Torres R, Casey G, Cenggoro TW, Chan AT, Chang-Claude J, Chen X, Conti DV, Devall M, Diez-Obrero V, Dimou N, Drew D, Figueiredo JC, Gallinger S, Giles GG, Gruber SB, Gsur A, Gunter MJ, Hampel H, Harlid S, Hidaka A, Harrison TA, Hoffmeister M, Huyghe JR, Jenkins MA, Jordahl K, Joshi AD, Kawaguchi ES, Keku TO, Kundaje A, Larsson SC, Marchand LL, Lewinger JP, Li L, Lynch BM, Mahesworo B, Mandic M, Obón-Santacana M, Moreno V, Murphy N, Nan H, Nassir R, Newcomb PA, Ogino S, Ose J, Pai RK, Palmer JR, Papadimitriou N, Pardamean B, Peoples AR, Platz EA, Potter JD, Prentice RL, Rennert G, Ruiz-Narvaez E, Sakoda LC, Scacheri PC, Schmit SL, Schoen RE, Shcherbina A, Slattery ML, Stern MC, Su YR, Tangen CM, Thibodeau SN, Thomas DC, Tian Y, Ulrich CM, van Duijnhoven FJ, Van Guelpen B, Visvanathan K, Vodicka P, Wang J, White E, Wolk A, Woods MO, Wu AH, Zemlianskaia N, Hsu L, Gauderman WJ, Peters U, Tsilidis KK, and Campbell PT

Subjects

Humans, Body Mass Index, Risk Factors, Genetic Loci, Polymorphism, Single Nucleotide, Genetic Predisposition to Disease, Genome-Wide Association Study, Intercellular Signaling Peptides and Proteins genetics, Obesity complications, Obesity genetics, Colorectal Neoplasms genetics

Abstract

Colorectal cancer risk can be impacted by genetic, environmental, and lifestyle factors, including diet and obesity. Gene-environment interactions (G × E) can provide biological insights into the effects of obesity on colorectal cancer risk. Here, we assessed potential genome-wide G × E interactions between body mass index (BMI) and common SNPs for colorectal cancer risk using data from 36,415 colorectal cancer cases and 48,451 controls from three international colorectal cancer consortia (CCFR, CORECT, and GECCO). The G × E tests included the conventional logistic regression using multiplicative terms (one degree of freedom, 1DF test), the two-step EDGE method, and the joint 3DF test, each of which is powerful for detecting G × E interactions under specific conditions. BMI was associated with higher colorectal cancer risk. The two-step approach revealed a statistically significant G×BMI interaction located within the Formin 1/Gremlin 1 (FMN1/GREM1) gene region (rs58349661). This SNP was also identified by the 3DF test, with a suggestive statistical significance in the 1DF test. Among participants with the CC genotype of rs58349661, overweight and obesity categories were associated with higher colorectal cancer risk, whereas null associations were observed across BMI categories in those with the TT genotype. Using data from three large international consortia, this study discovered a locus in the FMN1/GREM1 gene region that interacts with BMI on the association with colorectal cancer risk. Further studies should examine the potential mechanisms through which this locus modifies the etiologic link between obesity and colorectal cancer., Significance: This gene-environment interaction analysis revealed a genetic locus in FMN1/GREM1 that interacts with body mass index in colorectal cancer risk, suggesting potential implications for precision prevention strategies., (©2023 The Authors; Published by the American Association for Cancer Research.)

Published

2023

45. Genome-wide Interaction Study with Smoking for Colorectal Cancer Risk Identifies Novel Genetic Loci Related to Tumor Suppression, Inflammation, and Immune Response.

Author

Carreras-Torres R, Kim AE, Lin Y, Díez-Obrero V, Bien SA, Qu C, Wang J, Dimou N, Aglago EK, Albanes D, Arndt V, Baurley JW, Berndt SI, Bézieau S, Bishop DT, Bouras E, Brenner H, Budiarto A, Campbell PT, Casey G, Chan AT, Chang-Claude J, Chen X, Conti DV, Dampier CH, Devall MAM, Drew DA, Figueiredo JC, Gallinger S, Giles GG, Gruber SB, Gsur A, Gunter MJ, Harrison TA, Hidaka A, Hoffmeister M, Huyghe JR, Jenkins MA, Jordahl KM, Kawaguchi E, Keku TO, Kundaje A, Le Marchand L, Lewinger JP, Li L, Mahesworo B, Morrison JL, Murphy N, Nan H, Nassir R, Newcomb PA, Obón-Santacana M, Ogino S, Ose J, Pai RK, Palmer JR, Papadimitriou N, Pardamean B, Peoples AR, Pharoah PDP, Platz EA, Rennert G, Ruiz-Narvaez E, Sakoda LC, Scacheri PC, Schmit SL, Schoen RE, Shcherbina A, Slattery ML, Stern MC, Su YR, Tangen CM, Thomas DC, Tian Y, Tsilidis KK, Ulrich CM, van Duijnhoven FJB, Van Guelpen B, Visvanathan K, Vodicka P, Cenggoro TW, Weinstein SJ, White E, Wolk A, Woods MO, Hsu L, Peters U, Moreno V, and Gauderman WJ

Subjects

Humans, Smoking genetics, Risk Factors, Genotype, Inflammation, Tobacco Smoking, Genetic Loci, Polymorphism, Single Nucleotide, Case-Control Studies, Genetic Predisposition to Disease, Colorectal Neoplasms epidemiology

Abstract

Background: Tobacco smoking is an established risk factor for colorectal cancer. However, genetically defined population subgroups may have increased susceptibility to smoking-related effects on colorectal cancer., Methods: A genome-wide interaction scan was performed including 33,756 colorectal cancer cases and 44,346 controls from three genetic consortia., Results: Evidence of an interaction was observed between smoking status (ever vs. never smokers) and a locus on 3p12.1 (rs9880919, P = 4.58 × 10-8), with higher associated risk in subjects carrying the GG genotype [OR, 1.25; 95% confidence interval (CI), 1.20-1.30] compared with the other genotypes (OR <1.17 for GA and AA). Among ever smokers, we observed interactions between smoking intensity (increase in 10 cigarettes smoked per day) and two loci on 6p21.33 (rs4151657, P = 1.72 × 10-8) and 8q24.23 (rs7005722, P = 2.88 × 10-8). Subjects carrying the rs4151657 TT genotype showed higher risk (OR, 1.12; 95% CI, 1.09-1.16) compared with the other genotypes (OR <1.06 for TC and CC). Similarly, higher risk was observed among subjects carrying the rs7005722 AA genotype (OR, 1.17; 95% CI, 1.07-1.28) compared with the other genotypes (OR <1.13 for AC and CC). Functional annotation revealed that SNPs in 3p12.1 and 6p21.33 loci were located in regulatory regions, and were associated with expression levels of nearby genes. Genetic models predicting gene expression revealed that smoking parameters were associated with lower colorectal cancer risk with higher expression levels of CADM2 (3p12.1) and ATF6B (6p21.33)., Conclusions: Our study identified novel genetic loci that may modulate the risk for colorectal cancer of smoking status and intensity, linked to tumor suppression and immune response., Impact: These findings can guide potential prevention treatments., (©2022 American Association for Cancer Research.)

Published

2023

46. Validation of a Genetic-Enhanced Risk Prediction Model for Colorectal Cancer in a Large Community-Based Cohort.

Author

Su YR, Sakoda LC, Jeon J, Thomas M, Lin Y, Schneider JL, Udaltsova N, Lee JK, Lansdorp-Vogelaar I, Peterse EFP, Zauber AG, Zheng J, Zheng Y, Hauser E, Baron JA, Barry EL, Bishop DT, Brenner H, Buchanan DD, Burnett-Hartman A, Campbell PT, Casey G, Castellví-Bel S, Chan AT, Chang-Claude J, Figueiredo JC, Gallinger SJ, Giles GG, Gruber SB, Gsur A, Gunter MJ, Hampe J, Hampel H, Harrison TA, Hoffmeister M, Hua X, Huyghe JR, Jenkins MA, Keku TO, Marchand LL, Li L, Lindblom A, Moreno V, Newcomb PA, Pharoah PDP, Platz EA, Potter JD, Qu C, Rennert G, Schoen RE, Slattery ML, Song M, van Duijnhoven FJB, Van Guelpen B, Vodicka P, Wolk A, Woods MO, Wu AH, Hayes RB, Peters U, Corley DA, and Hsu L

Subjects

Humans, Middle Aged, Aged, Risk Factors, Risk Assessment, Colorectal Neoplasms epidemiology

Abstract

Background: Polygenic risk scores (PRS) which summarize individuals' genetic risk profile may enhance targeted colorectal cancer screening. A critical step towards clinical implementation is rigorous external validations in large community-based cohorts. This study externally validated a PRS-enhanced colorectal cancer risk model comprising 140 known colorectal cancer loci to provide a comprehensive assessment on prediction performance., Methods: The model was developed using 20,338 individuals and externally validated in a community-based cohort (n = 85,221). We validated predicted 5-year absolute colorectal cancer risk, including calibration using expected-to-observed case ratios (E/O) and calibration plots, and discriminatory accuracy using time-dependent AUC. The PRS-related improvement in AUC, sensitivity and specificity were assessed in individuals of age 45 to 74 years (screening-eligible age group) and 40 to 49 years with no endoscopy history (younger-age group)., Results: In European-ancestral individuals, the predicted 5-year risk calibrated well [E/O = 1.01; 95% confidence interval (CI), 0.91-1.13] and had high discriminatory accuracy (AUC = 0.73; 95% CI, 0.71-0.76). Adding the PRS to a model with age, sex, family and endoscopy history improved the 5-year AUC by 0.06 (P < 0.001) and 0.14 (P = 0.05) in the screening-eligible age and younger-age groups, respectively. Using a risk-threshold of 5-year SEER colorectal cancer incidence rate at age 50 years, adding the PRS had a similar sensitivity but improved the specificity by 11% (P < 0.001) in the screening-eligible age group. In the younger-age group it improved the sensitivity by 27% (P = 0.04) with similar specificity., Conclusions: The proposed PRS-enhanced model provides a well-calibrated 5-year colorectal cancer risk prediction and improves discriminatory accuracy in the external cohort., Impact: The proposed model has potential utility in risk-stratified colorectal cancer prevention., (©2023 American Association for Cancer Research.)

Published

2023

47. Genetic Predictors for Fecal Propionate and Butyrate-Producing Microbiome Pathway Are Not Associated with Colorectal Cancer Risk: A Mendelian Randomization Analysis.

Author

Lu Y, Zhao YC, Chang-Claude J, Gruber SB, Gsur A, Offit K, Vodickova L, Woods MO, Nguyen LH, Wade KH, Carreras-Torres R, Moreno V, Buchanan DD, Cotterchio M, Chan AT, Phipps AI, Peters U, and Song M

Subjects

Humans, Fatty Acids, Volatile analysis, Fatty Acids, Volatile genetics, Fatty Acids, Volatile metabolism, Mendelian Randomization Analysis, Risk, Europe epidemiology, Butyrates analysis, Butyrates metabolism, Colorectal Neoplasms epidemiology, Colorectal Neoplasms genetics, Colorectal Neoplasms metabolism, Feces chemistry, Feces microbiology, Gastrointestinal Microbiome genetics, Gastrointestinal Microbiome physiology, Propionates analysis, Propionates metabolism

Abstract

Background: Mechanistic data indicate the benefit of short-chain fatty acids (SCFA) produced by gut microbial fermentation of fiber on colorectal cancer, but direct epidemiologic evidence is limited. A recent study identified SNPs for two SCFA traits (fecal propionate and butyrate-producing microbiome pathway PWY-5022) in Europeans and showed metabolic benefits., Methods: We conducted a two-sample Mendelian randomization analysis of the genetic instruments for the two SCFA traits (three SNPs for fecal propionate and nine for PWY-5022) in relation to colorectal cancer risk in three large European genetic consortia of 58,131 colorectal cancer cases and 67,347 controls. We estimated the risk of overall colorectal cancer and conducted subgroup analyses by sex, age, and anatomic subsites of colorectal cancer., Results: We did not observe strong evidence for an association of the genetic predictors for fecal propionate levels and the abundance of PWY-5022 with the risk of overall colorectal cancer, colorectal cancer by sex, or early-onset colorectal cancer (diagnosed at <50 years), with no evidence of heterogeneity or pleiotropy. When assessed by tumor subsites, we found weak evidence for an association between PWY-5022 and risk of rectal cancer (OR per 1-SD, 0.95; 95% confidence intervals, 0.91-0.99; P = 0.03) but it did not surpass multiple testing of subgroup analysis., Conclusions: Genetic instruments for fecal propionate levels and the abundance of PWY-5022 were not associated with colorectal cancer risk., Impact: Fecal propionate and PWY-5022 may not have a substantial influence on colorectal cancer risk. Future research is warranted to comprehensively investigate the effects of SCFA-producing bacteria and SCFAs on colorectal cancer risk., (©2022 American Association for Cancer Research.)

Published

2023

48. Large-scale Integrated Analysis of Genetics and Metabolomic Data Reveals Potential Links Between Lipids and Colorectal Cancer Risk.

Author

Shu X, Chen Z, Long J, Guo X, Yang Y, Qu C, Ahn YO, Cai Q, Casey G, Gruber SB, Huyghe JR, Jee SH, Jenkins MA, Jia WH, Jung KJ, Kamatani Y, Kim DH, Kim J, Kweon SS, Le Marchand L, Matsuda K, Matsuo K, Newcomb PA, Oh JH, Ose J, Oze I, Pai RK, Pan ZZ, Pharoah PDP, Playdon MC, Ren ZF, Schoen RE, Shin A, Shin MH, Shu XO, Sun X, Tangen CM, Tanikawa C, Ulrich CM, van Duijnhoven FJB, Van Guelpen B, Wolk A, Woods MO, Wu AH, Peters U, and Zheng W

Subjects

Asian People, Case-Control Studies, Glycerophospholipids, Humans, Lipids, Metabolomics methods, Colorectal Neoplasms epidemiology, Colorectal Neoplasms genetics, Colorectal Neoplasms metabolism

Abstract

Background: The etiology of colorectal cancer is not fully understood., Methods: Using genetic variants and metabolomics data including 217 metabolites from the Framingham Heart Study (n = 1,357), we built genetic prediction models for circulating metabolites. Models with prediction R2 > 0.01 (Nmetabolite = 58) were applied to predict levels of metabolites in two large consortia with a combined sample size of approximately 46,300 cases and 59,200 controls of European and approximately 21,700 cases and 47,400 controls of East Asian (EA) descent. Genetically predicted levels of metabolites were evaluated for their associations with colorectal cancer risk in logistic regressions within each racial group, after which the results were combined by meta-analysis., Results: Of the 58 metabolites tested, 24 metabolites were significantly associated with colorectal cancer risk [Benjamini-Hochberg FDR (BH-FDR) < 0.05] in the European population (ORs ranged from 0.91 to 1.06; P values ranged from 0.02 to 6.4 × 10-8). Twenty one of the 24 associations were replicated in the EA population (ORs ranged from 0.26 to 1.69, BH-FDR < 0.05). In addition, the genetically predicted levels of C16:0 cholesteryl ester was significantly associated with colorectal cancer risk in the EA population only (OREA: 1.94, 95% CI, 1.60-2.36, P = 2.6 × 10-11; OREUR: 1.01, 95% CI, 0.99-1.04, P = 0.3). Nineteen of the 25 metabolites were glycerophospholipids and triacylglycerols (TAG). Eighteen associations exhibited significant heterogeneity between the two racial groups (PEUR-EA-Het < 0.005), which were more strongly associated in the EA population. This integrative study suggested a potential role of lipids, especially certain glycerophospholipids and TAGs, in the etiology of colorectal cancer., Conclusions: This study identified potential novel risk biomarkers for colorectal cancer by integrating genetics and circulating metabolomics data., Impact: The identified metabolites could be developed into new tools for risk assessment of colorectal cancer in both European and EA populations., (©2022 American Association for Cancer Research.)

Published

2022

49. Beyond GWAS of Colorectal Cancer: Evidence of Interaction with Alcohol Consumption and Putative Causal Variant for the 10q24.2 Region.

Author

Jordahl KM, Shcherbina A, Kim AE, Su YR, Lin Y, Wang J, Qu C, Albanes D, Arndt V, Baurley JW, Berndt SI, Bien SA, Bishop DT, Bouras E, Brenner H, Buchanan DD, Budiarto A, Campbell PT, Carreras-Torres R, Casey G, Cenggoro TW, Chan AT, Conti DV, Dampier CH, Devall MA, Díez-Obrero V, Dimou N, Drew DA, Figueiredo JC, Gallinger S, Giles GG, Gruber SB, Gsur A, Gunter MJ, Hampel H, Harlid S, Harrison TA, Hidaka A, Hoffmeister M, Huyghe JR, Jenkins MA, Joshi AD, Keku TO, Larsson SC, Le Marchand L, Lewinger JP, Li L, Mahesworo B, Moreno V, Morrison JL, Murphy N, Nan H, Nassir R, Newcomb PA, Obón-Santacana M, Ogino S, Ose J, Pai RK, Palmer JR, Papadimitriou N, Pardamean B, Peoples AR, Pharoah PDP, Platz EA, Potter JD, Prentice RL, Rennert G, Ruiz-Narvaez E, Sakoda LC, Scacheri PC, Schmit SL, Schoen RE, Slattery ML, Stern MC, Tangen CM, Thibodeau SN, Thomas DC, Tian Y, Tsilidis KK, Ulrich CM, van Duijnhoven FJB, Van Guelpen B, Visvanathan K, Vodicka P, White E, Wolk A, Woods MO, Wu AH, Zemlianskaia N, Chang-Claude J, Gauderman WJ, Hsu L, Kundaje A, and Peters U

Subjects

Alcohol Drinking adverse effects, Alcohol Drinking epidemiology, Alcohol Drinking genetics, Electron Transport Complex IV genetics, Humans, Polymorphism, Single Nucleotide, Risk Factors, Colorectal Neoplasms etiology, Colorectal Neoplasms genetics, Genome-Wide Association Study

Abstract

Background: Currently known associations between common genetic variants and colorectal cancer explain less than half of its heritability of 25%. As alcohol consumption has a J-shape association with colorectal cancer risk, nondrinking and heavy drinking are both risk factors for colorectal cancer., Methods: Individual-level data was pooled from the Colon Cancer Family Registry, Colorectal Transdisciplinary Study, and Genetics and Epidemiology of Colorectal Cancer Consortium to compare nondrinkers (≤1 g/day) and heavy drinkers (>28 g/day) with light-to-moderate drinkers (1-28 g/day) in GxE analyses. To improve power, we implemented joint 2df and 3df tests and a novel two-step method that modifies the weighted hypothesis testing framework. We prioritized putative causal variants by predicting allelic effects using support vector machine models., Results: For nondrinking as compared with light-to-moderate drinking, the hybrid two-step approach identified 13 significant SNPs with pairwise r2 > 0.9 in the 10q24.2/COX15 region. When stratified by alcohol intake, the A allele of lead SNP rs2300985 has a dose-response increase in risk of colorectal cancer as compared with the G allele in light-to-moderate drinkers [OR for GA genotype = 1.11; 95% confidence interval (CI), 1.06-1.17; OR for AA genotype = 1.22; 95% CI, 1.14-1.31], but not in nondrinkers or heavy drinkers. Among the correlated candidate SNPs in the 10q24.2/COX15 region, rs1318920 was predicted to disrupt an HNF4 transcription factor binding motif., Conclusions: Our study suggests that the association with colorectal cancer in 10q24.2/COX15 observed in genome-wide association study is strongest in nondrinkers. We also identified rs1318920 as the putative causal regulatory variant for the region., Impact: The study identifies multifaceted evidence of a possible functional effect for rs1318920., (©2022 American Association for Cancer Research.)

Published

2022

50. Disease-Associated Risk Variants in ANRIL Are Associated with Tumor-Infiltrating Lymphocyte Presence in Primary Melanomas in the Population-Based GEM Study.

Author

Davari DR, Orlow I, Kanetsky PA, Luo L, Edmiston SN, Conway K, Parrish EA, Hao H, Busam KJ, Sharma A, Kricker A, Cust AE, Anton-Culver H, Gruber SB, Gallagher RP, Zanetti R, Rosso S, Sacchetto L, Dwyer T, Ollila DW, Begg CB, Berwick M, and Thomas NE

Subjects

Aged, Female, GTP Phosphohydrolases, Genome-Wide Association Study, Humans, Male, Melanoma pathology, Membrane Proteins, Middle Aged, Mutation, Proto-Oncogene Proteins B-raf, Skin Neoplasms pathology, Melanoma, Cutaneous Malignant, Cyclin-Dependent Kinase Inhibitor p15, Lymphocytes, Tumor-Infiltrating pathology, Melanoma genetics, Skin Neoplasms genetics

Abstract

Background: Genome-wide association studies have reported that genetic variation at ANRIL ( CDKN2B-AS1 ) is associated with risk of several chronic diseases including coronary artery disease, coronary artery calcification, myocardial infarction, and type 2 diabetes mellitus. ANRIL is located at the CDKN2A/B locus, which encodes multiple melanoma tumor suppressors. We investigated the association of these variants with melanoma prognostic characteristics., Methods: The Genes, Environment, and Melanoma Study enrolled 3,285 European origin participants with incident invasive primary melanoma. For each of ten disease-associated SNPs at or near ANRIL , we used linear and logistic regression modeling to estimate, respectively, the per allele mean changes in log of Breslow thickness and ORs for presence of ulceration and tumor-infiltrating lymphocytes (TIL). We also assessed effect modification by tumor NRAS/BRAF mutational status., Results: Rs518394, rs10965215, and rs564398 passed false discovery and were each associated ( P ≤ 0.005) with TILs, although only rs564398 was independently associated ( P = 0.0005) with TILs. Stratified by NRAS/BRAF mutational status, rs564398*A was significantly positively associated with TILs among NRAS/BRAF mutant, but not wild-type, cases. We did not find SNP associations with Breslow thickness or ulceration., Conclusions: ANRIL rs564398 was associated with TIL presence in primary melanomas, and this association may be limited to NRAS/BRAF -mutant cases., Impact: Pathways related to ANRIL variants warrant exploration in relationship to TILs in melanoma, especially given the impact of TILs on immunotherapy and survival., (©2021 The Authors; Published by the American Association for Cancer Research.)

Published

2021