Your search keyword '"Burdett, Laurie"' showing total 18 results

1. Distinct germline genetic susceptibility profiles identified for common non-Hodgkin lymphoma subtypes

Author

Berndt, Sonja I., Vijai, Joseph, Benavente, Yolanda, Camp, Nicola J., Nieters, Alexandra, Wang, Zhaoming, Smedby, Karin E., Kleinstern, Geffen, Hjalgrim, Henrik, Besson, Caroline, Skibola, Christine F., Morton, Lindsay M., Brooks-Wilson, Angela R., Teras, Lauren R., Breeze, Charles, Arias, Joshua, Adami, Hans-Olov, Albanes, Demetrius, Anderson, Kenneth C., Ansell, Stephen M., Bassig, Bryan, Becker, Nikolaus, Bhatti, Parveen, Birmann, Brenda M., Boffetta, Paolo, Bracci, Paige M., Brennan, Paul, Brown, Elizabeth E., Burdett, Laurie, Cannon-Albright, Lisa A., Chang, Ellen T., Chiu, Brian C. H., Chung, Charles C., Clavel, Jacqueline, Cocco, Pierluigi, Colditz, Graham, Conde, Lucia, Conti, David V., Cox, David G., Curtin, Karen, Casabonne, Delphine, De Vivo, Immaculata, Diver, W. Ryan, Dogan, Ahmet, Edlund, Christopher K., Foretova, Lenka, Fraumeni, Joseph F., Gabbas, Attilio, Ghesquières, Hervé, Giles, Graham G., Glaser, Sally, Glenn, Martha, Glimelius, Bengt, Gu, Jian, Habermann, Thomas M., Haiman, Christopher A., Haioun, Corinne, Hofmann, Jonathan N., Holford, Theodore R., Holly, Elizabeth A., Hutchinson, Amy, Izhar, Aalin, Jackson, Rebecca D., Jarrett, Ruth F., Kaaks, Rudolph, Kane, Eleanor, Kolonel, Laurence N., Kong, Yinfei, Kraft, Peter, Kricker, Anne, Lake, Annette, Lan, Qing, Lawrence, Charles, Li, Dalin, Liebow, Mark, Link, Brian K., Magnani, Corrado, Maynadie, Marc, McKay, James, Melbye, Mads, Miligi, Lucia, Milne, Roger L., Molina, Thierry J., Monnereau, Alain, Montalvan, Rebecca, North, Kari E., Novak, Anne J., Onel, Kenan, Purdue, Mark P., Rand, Kristin A., Riboli, Elio, Riby, Jacques, Roman, Eve, Salles, Gilles, Sborov, Douglas W., Severson, Richard K., Shanafelt, Tait D., Smith, Martyn T., Smith, Alexandra, Song, Kevin W., Song, Lei, Southey, Melissa C., Spinelli, John J., Staines, Anthony, Stephens, Deborah, Sutherland, Heather J., Tkachuk, Kaitlyn, Thompson, Carrie A., Tilly, Hervé, Tinker, Lesley F., Travis, Ruth C., Turner, Jenny, Vachon, Celine M., Vajdic, Claire M., Van Den Berg, Anke, Van Den Berg, David J., Vermeulen, Roel C. H., Vineis, Paolo, Wang, Sophia S., Weiderpass, Elisabete, Weiner, George J., Weinstein, Stephanie, Doo, Nicole Wong, Ye, Yuanqing, Yeager, Meredith, Yu, Kai, Zeleniuch-Jacquotte, Anne, Zhang, Yawei, Zheng, Tongzhang, Ziv, Elad, Sampson, Joshua, Chatterjee, Nilanjan, Offit, Kenneth, Cozen, Wendy, Wu, Xifeng, Cerhan, James R., Chanock, Stephen J., Slager, Susan L., and Rothman, Nathaniel

Abstract

Lymphoma risk is elevated for relatives with common non-Hodgkin lymphoma (NHL) subtypes, suggesting shared genetic susceptibility across subtypes. To evaluate the extent of mutual heritability among NHL subtypes and discover novel loci shared among subtypes, we analyzed data from eight genome-wide association studies within the InterLymph Consortium, including 10,629 cases and 9505 controls. We utilized Association analysis based on SubSETs (ASSET) to discover loci for subsets of NHL subtypes and evaluated shared heritability across the genome using Genome-wide Complex Trait Analysis (GCTA) and polygenic risk scores. We discovered 17 genome-wide significant loci (P< 5 × 10−8) for subsets of NHL subtypes, including a novel locus at 10q23.33 (HHEX) (P= 3.27 × 10−9). Most subset associations were driven primarily by only one subtype. Genome-wide genetic correlations between pairs of subtypes varied broadly from 0.20 to 0.86, suggesting substantial heterogeneity in the extent of shared heritability among subtypes. Polygenic risk score analyses of established loci for different lymphoid malignancies identified strong associations with some NHL subtypes (P< 5 × 10−8), but weak or null associations with others. Although our analyses suggest partially shared heritability and biological pathways, they reveal substantial heterogeneity among NHL subtypes with each having its own distinct germline genetic architecture.

Published

2022

2. Sex specific associations in genome wide association analysis of renal cell carcinoma

Author

Laskar, Ruhina, Muller, David, Li, Peng, Machiela, Mitchell, Ye, Yuanqing, Gaborieau, Valerie, Foll, Matthieu, Hofmann, Jonathan, Colli, Leandro, Sampson, Joshua, Wang, Zhaoming, Bacq-Daian, Delphine, Boland, Anne, Abedi-Ardekani, Behnoush, Durand, Geoffroy, Calvez-Kelm, Florence, Robinot, Nivonirina, Blanche, Helene, Prokhortchouk, Egor, Skryabin, Konstantin, Burdett, Laurie, Yeager, Meredith, Radojevic-Skodric, Sanja, Savic, Slavisa, Foretova, Lenka, Holcatova, Ivana, Janout, Vladimir, Mates, Dana, Rascu, Stefan, Mukeria, Anush, Zaridze, David, Bencko, Vladimir, Cybulski, Cezary, Fabianova, Eleonora, Jinga, Viorel, Lissowska, Jolanta, Lubinski, Jan, Navratilova, Marie, Rudnai, Peter, Świątkowska, Beata, Benhamou, Simone, Cancel-Tassin, Geraldine, Cussenot, Olivier, Trichopoulou, Antonia, Riboli, Elio, Overvad, Kim, Panico, Salvatore, Ljungberg, Borje, Sitaram, Raviprakash, Giles, Graham, Milne, Roger, Severi, Gianluca, Bruinsma, Fiona, Fletcher, Tony, Koppova, Kvetoslava, Larsson, Susanna, Wolk, Alicja, Banks, Rosamonde, Selby, Peter, Easton, Douglas, Pharoah, Paul, Andreotti, Gabriella, Beane Freeman, Laura, Koutros, Stella, Albanes, Demetrius, Männistö, Satu, Weinstein, Stephanie, Clark, Peter, Edwards, Todd, Lipworth, Loren, Carol, Hallie, Freedman, Matthew, Pomerantz, Mark, Cho, Eunyoung, Kraft, Peter, Preston, Mark, Wilson, Kathryn, Michael Gaziano, J., Sesso, Howard, Black, Amanda, Freedman, Neal, Huang, Wen-Yi, Anema, John, Kahnoski, Richard, Lane, Brian, Noyes, Sabrina, Petillo, David, Teh, Bin, Peters, Ulrike, White, Emily, Anderson, Garnet, Johnson, Lisa, Luo, Juhua, Chow, Wong-Ho, Moore, Lee, Choueiri, Toni, Wood, Christopher, Johansson, Mattias, McKay, James, Brown, Kevin, Rothman, Nathaniel, Lathrop, Mark, Deleuze, Jean-Francois, Wu, Xifeng, Brennan, Paul, Chanock, Stephen, Purdue, Mark, and Scelo, Ghislaine

Abstract

Renal cell carcinoma (RCC) has an undisputed genetic component and a stable 2:1 male to female sex ratio in its incidence across populations, suggesting possible sexual dimorphism in its genetic susceptibility. We conducted the first sex-specific genome-wide association analysis of RCC for men (3227 cases, 4916 controls) and women (1992 cases, 3095 controls) of European ancestry from two RCC genome-wide scans and replicated the top findings using an additional series of men (2261 cases, 5852 controls) and women (1399 cases, 1575 controls) from two independent cohorts of European origin. Our study confirmed sex-specific associations for two known RCC risk loci at 14q24.2 (DPF3) and 2p21(EPAS1). We also identified two additional suggestive male-specific loci at 6q24.3 (SAMD5, male odds ratio (ORmale) = 0.83 [95% CI = 0.78-0.89], Pmale= 1.71 × 10−8compared with female odds ratio (ORfemale) = 0.98 [95% CI = 0.90–1.07], Pfemale= 0.68) and 12q23.3 (intergenic, ORmale= 0.75 [95% CI = 0.68-0.83], Pmale= 1.59 × 10−8compared with ORfemale= 0.93 [95% CI = 0.82–1.06], Pfemale= 0.21) that attained genome-wide significance in the joint meta-analysis. Herein, we provide evidence of sex-specific associations in RCC genetic susceptibility and advocate the necessity of larger genetic and genomic studies to unravel the endogenous causes of sex bias in sexually dimorphic traits and diseases like RCC.

Published

2019

3. Correction: Distinct germline genetic susceptibility profiles identified for common non-Hodgkin lymphoma subtypes

Author

Berndt, Sonja I., Vijai, Joseph, Benavente, Yolanda, Camp, Nicola J., Nieters, Alexandra, Wang, Zhaoming, Smedby, Karin E., Kleinstern, Geffen, Hjalgrim, Henrik, Besson, Caroline, Skibola, Christine F., Morton, Lindsay M., Brooks-Wilson, Angela R., Teras, Lauren R., Breeze, Charles, Arias, Joshua, Adami, Hans-Olov, Albanes, Demetrius, Anderson, Kenneth C., Ansell, Stephen M., Bassig, Bryan, Becker, Nikolaus, Bhatti, Parveen, Birmann, Brenda M., Boffetta, Paolo, Bracci, Paige M., Brennan, Paul, Brown, Elizabeth E., Burdett, Laurie, Cannon-Albright, Lisa A., Chang, Ellen T., Chiu, Brian C. H., Chung, Charles C., Clavel, Jacqueline, Cocco, Pierluigi, Colditz, Graham, Conde, Lucia, Conti, David V., Cox, David G., Curtin, Karen, Casabonne, Delphine, De Vivo, Immaculata, Diepstra, Arjan, Diver, W. Ryan, Dogan, Ahmet, Edlund, Christopher K., Foretova, Lenka, Fraumeni, Joseph F., Gabbas, Attilio, Ghesquières, Hervé, Giles, Graham G., Glaser, Sally, Glenn, Martha, Glimelius, Bengt, Gu, Jian, Habermann, Thomas M., Haiman, Christopher A., Haioun, Corinne, Hofmann, Jonathan N., Holford, Theodore R., Holly, Elizabeth A., Hutchinson, Amy, Izhar, Aalin, Jackson, Rebecca D., Jarrett, Ruth F., Kaaks, Rudolph, Kane, Eleanor, Kolonel, Laurence N., Kong, Yinfei, Kraft, Peter, Kricker, Anne, Lake, Annette, Lan, Qing, Lawrence, Charles, Li, Dalin, Liebow, Mark, Link, Brian K., Magnani, Corrado, Maynadie, Marc, McKay, James, Melbye, Mads, Miligi, Lucia, Milne, Roger L., Molina, Thierry J., Monnereau, Alain, Montalvan, Rebecca, North, Kari E., Novak, Anne J., Onel, Kenan, Purdue, Mark P., Rand, Kristin A., Riboli, Elio, Riby, Jacques, Roman, Eve, Salles, Gilles, Sborov, Douglas W., Severson, Richard K., Shanafelt, Tait D., Smith, Martyn T., Smith, Alexandra, Song, Kevin W., Song, Lei, Southey, Melissa C., Spinelli, John J., Staines, Anthony, Stephens, Deborah, Sutherland, Heather J., Tkachuk, Kaitlyn, Thompson, Carrie A., Tilly, Hervé, Tinker, Lesley F., Travis, Ruth C., Turner, Jenny, Vachon, Celine M., Vajdic, Claire M., Van Den Berg, Anke, Van Den Berg, David J., Vermeulen, Roel C. H., Vineis, Paolo, Wang, Sophia S., Weiderpass, Elisabete, Weiner, George J., Weinstein, Stephanie, Doo, Nicole Wong, Ye, Yuanqing, Yeager, Meredith, Yu, Kai, Zeleniuch-Jacquotte, Anne, Zhang, Yawei, Zheng, Tongzhang, Ziv, Elad, Sampson, Joshua, Chatterjee, Nilanjan, Offit, Kenneth, Cozen, Wendy, Wu, Xifeng, Cerhan, James R., Chanock, Stephen J., Slager, Susan L., and Rothman, Nathaniel

Published

2023

4. Whole-exome sequencing and functional studies identify RPS29 as a novel gene mutated in multicase Diamond-Blackfan anemia families

Author

Mirabello, Lisa, Macari, Elizabeth R., Jessop, Lea, Ellis, Steven R., Myers, Timothy, Giri, Neelam, Taylor, Alison M., McGrath, Katherine E., Humphries, Jessica M., Ballew, Bari J., Yeager, Meredith, Boland, Joseph F., He, Ji, Hicks, Belynda D., Burdett, Laurie, Alter, Blanche P., Zon, Leonard, and Savage, Sharon A.

Abstract

Diamond-Blackfan anemia (DBA) is a cancer-prone inherited bone marrow failure syndrome. Approximately half of DBA patients have a germ-line mutation in a ribosomal protein gene. We used whole-exome sequencing to identify disease-causing genes in 2 large DBA families. After filtering, 1 nonsynonymous mutation (p.I31F) in the ribosomal protein S29 (RPS29[AUQ1]) gene was present in all 5 DBA-affected individuals and the obligate carrier, and absent from the unaffected noncarrier parent in 1 DBA family. A second DBA family was found to have a different nonsynonymous mutation (p.I50T) in RPS29. Both mutations are amino acid substitutions in exon 2 predicted to be deleterious and resulted in haploinsufficiency of RPS29 expression compared with wild-type RPS29 expression from an unaffected control. The DBA proband with the p.I31F RPS29 mutation had a pre–ribosomal RNA (rRNA) processing defect compared with the healthy control. We demonstrated that both RPS29 mutations failed to rescue the defective erythropoiesis in the rps29−/− mutant zebra fish DBA model. RPS29 is a component of the small 40S ribosomal subunit and essential for rRNA processing and ribosome biogenesis. We uncovered a novel DBA causative gene, RPS29, and showed that germ-line mutations in RPS29 can cause a defective erythropoiesis phenotype using a zebra fish model.

Published

2014

5. Whole-exome sequencing and functional studies identify RPS29as a novel gene mutated in multicase Diamond-Blackfan anemia families

Author

Mirabello, Lisa, Macari, Elizabeth R., Jessop, Lea, Ellis, Steven R., Myers, Timothy, Giri, Neelam, Taylor, Alison M., McGrath, Katherine E., Humphries, Jessica M., Ballew, Bari J., Yeager, Meredith, Boland, Joseph F., He, Ji, Hicks, Belynda D., Burdett, Laurie, Alter, Blanche P., Zon, Leonard, and Savage, Sharon A.

Abstract

Diamond-Blackfan anemia (DBA) is a cancer-prone inherited bone marrow failure syndrome. Approximately half of DBA patients have a germ-line mutation in a ribosomal protein gene. We used whole-exome sequencing to identify disease-causing genes in 2 large DBA families. After filtering, 1 nonsynonymous mutation (p.I31F) in the ribosomal protein S29 (RPS29[AUQ1]) gene was present in all 5 DBA-affected individuals and the obligate carrier, and absent from the unaffected noncarrier parent in 1 DBA family. A second DBA family was found to have a different nonsynonymous mutation (p.I50T) in RPS29. Both mutations are amino acid substitutions in exon 2 predicted to be deleterious and resulted in haploinsufficiency of RPS29expression compared with wild-type RPS29expression from an unaffected control. The DBA proband with the p.I31F RPS29mutation had a pre–ribosomal RNA (rRNA) processing defect compared with the healthy control. We demonstrated that both RPS29mutations failed to rescue the defective erythropoiesis in the rps29−/−mutant zebra fish DBA model. RPS29is a component of the small 40S ribosomal subunit and essential for rRNA processing and ribosome biogenesis. We uncovered a novel DBA causative gene, RPS29, and showed that germ-line mutations in RPS29can cause a defective erythropoiesis phenotype using a zebra fish model.

Published

2014

6. Whole exome sequencing in families with CLL detects a variant in Integrin β 2 associated with disease susceptibility

Author

Goldin, Lynn R., McMaster, Mary L., Rotunno, Melissa, Herman, Sarah E. M., Jones, Kristine, Zhu, Bin, Boland, Joseph, Burdett, Laurie, Hicks, Belynda, Ravichandran, Sarangan, Luke, Brian T., Yeager, Meredith, Fontaine, Laura, Goldstein, Alisa M., Chanock, Stephen J., Tucker, Margaret A., Wiestner, Adrian, Marti, Gerald, and Caporaso, Neil E.

Published

2016

7. Whole exome sequencing in families with CLL detects a variant in Integrin β 2associated with disease susceptibility

Author

Goldin, Lynn R., McMaster, Mary L., Rotunno, Melissa, Herman, Sarah E.M., Jones, Kristine, Zhu, Bin, Boland, Joseph, Burdett, Laurie, Hicks, Belynda, Ravichandran, Sarangan, Luke, Brian T., Yeager, Meredith, Fontaine, Laura, Goldstein, Alisa M., Chanock, Stephen J., Tucker, Margaret A., Wiestner, Adrian, Marti, Gerald, and Caporaso, Neil E.

Published

2016

8. Somatic sequence alterations in twenty-one genes selected by expression profile analysis of breast carcinomas

Author

Chanock, Stephen, Burdett, Laurie, Yeager, Meredith, Llaca, Victor, Langerød, Anita, Presswalla, Shafaq, Kaaresen, Rolf, Strausberg, Robert, Gerhard, Daniela, Kristensen, Vessela, Perou, Charles, and Børresen-Dale, Anne-Lise

Abstract

Genomic alterations have been observed in breast carcinomas that affect the capacity of cells to regulate proliferation, signaling, and metastasis. Re-sequence studies have investigated candidate genes based on prior genetic observations (changes in copy number or regions of genetic instability) or other laboratory observations and have defined critical somatic mutations in genes such as TP53and PIK3CA. We have extended the paradigm and analyzed 21 genes primarily identified by expression profiling studies, which are useful for breast cancer subtyping and prognosis. This study conducted a bidirectional re-sequence analysis of all exons and 5', 3', and evolutionarily conserved regions (spanning more than 16 megabases) in 91 breast tumor samples. Eighty-seven unique somatic alterations were identified in 16 genes. Seventy-eight were single base pair alterations, of which 23 were missense mutations; 55 were distributed across conserved intronic regions or the 5' and 3' regions. There were nine insertion/deletions. Because there is no a prioriway to predict whether any one of the identified synonymous and noncoding somatic alterations disrupt function, analysis unique to each gene will be required to establish whether it is a tumor suppressor gene or whether there is no effect. In five genes, no somatic alterations were observed. The study confirms the value of re-sequence analysis in cancer gene discovery and underscores the importance of characterizing somatic alterations across genes that are related not only by function, or functional pathways, but also based upon expression patterns.

Published

2007

9. Genome-Wide Association Study Identifies an Immune-Related Etiology for Severe Aplastic Anemia

Author

Savage, Sharon A., Viard, Mathias, Zhou, Weiyin, Yeager, Meredith, Li, Shengchao, Wang, Tao, Vogt, Aurelie, Hicks, Belynda, Burdett, Laurie, Chung, Charles, O'hUigin, Colm, Dean, Michael, de Andrade, Kelvin, Freedman, Neal D, Berndt, Sonja I, Rothman, Nathaniel, Lan, Qing, Cerhan, James R., Slager, Susan L, Zhang, Yawei, Teras, Lauren R, Haagenson, Michael, Chanock, Stephen J, Spellman, Stephen R., Wang, Youjin, Willis, Amanda, Askar, Medhat, Lee, Stephanie J., Mary, Carrington, and Gadalla, Shahinaz M

Abstract

Cerhan: Janssen: Membership on an entity's Board of Directors or advisory committees; NanoString: Research Funding; Celgene: Research Funding. Lee:Incyte: Research Funding; Syndax: Research Funding; Amgen: Research Funding; Novartis: Research Funding; Takeda: Research Funding; Kadmon: Consultancy, Research Funding; Pfizer: Consultancy, Research Funding; AstraZeneca: Research Funding.

Published

2019

10. Genome-Wide Association Study Identifies an Immune-Related Etiology for Severe Aplastic Anemia

Author

Savage, Sharon A., Viard, Mathias, Zhou, Weiyin, Yeager, Meredith, Li, Shengchao, Wang, Tao, Vogt, Aurelie, Hicks, Belynda, Burdett, Laurie, Chung, Charles, O'hUigin, Colm, Dean, Michael, de Andrade, Kelvin, Freedman, Neal D, Berndt, Sonja I, Rothman, Nathaniel, Lan, Qing, Cerhan, James R., Slager, Susan L, Zhang, Yawei, Teras, Lauren R, Haagenson, Michael, Chanock, Stephen J, Spellman, Stephen R., Wang, Youjin, Willis, Amanda, Askar, Medhat, Lee, Stephanie J., Mary, Carrington, and Gadalla, Shahinaz M

Abstract

Introduction.Acquired severe aplastic anemia (SAA) is a life-threatening disorder characterized by severe progressive pancytopenia and hypocellular bone marrow. The etiology of acquired SAA is not understood but believed to be related to abnormal immune responses to environmental exposures. We conducted a genome-wide association study (GWAS) to identify common germline variants associated with SAA.

Published

2019

11. Functional Consequences Of RPS29 Germline Mutations In Diamond-Blackfan Anemia

Author

Mirabello, Lisa, Macari, Elizabeth R, Jessop, Lea, Myers, Timothy, Giri, Neelam, Taylor, Alison M., McGrath, Katherine E., Humphries, Jessica M., Ballew, Bari J, Yeager, Meredith, Boland, Joseph F, He, Ji, Hicks, Belynda D, Burdett, Laurie, Alter, Blanche P, Zon, Leonard I., and Savage, Sharon A

Abstract

Zon: FATE Therapeutics, Inc: Consultancy, Equity Ownership, Founder Other, Membership on an entity’s Board of Directors or advisory committees, Patents & Royalties; Stemgent, Inc: Consultancy, Membership on an entity’s Board of Directors or advisory committees, Stocks, Stocks Other; Scholar Rock: Consultancy, Equity Ownership, Founder, Founder Other, Membership on an entity’s Board of Directors or advisory committees, Patents & Royalties.

Published

2013

12. Functional Consequences Of RPS29Germline Mutations In Diamond-Blackfan Anemia

Author

Mirabello, Lisa, Macari, Elizabeth R, Jessop, Lea, Myers, Timothy, Giri, Neelam, Taylor, Alison M., McGrath, Katherine E., Humphries, Jessica M., Ballew, Bari J, Yeager, Meredith, Boland, Joseph F, He, Ji, Hicks, Belynda D, Burdett, Laurie, Alter, Blanche P, Zon, Leonard I., and Savage, Sharon A

Abstract

Diamond-Blackfan anemia (DBA) is an inherited bone marrow failure syndrome (IBMFS) characterized by red blood cell aplasia, variable physical anomalies, and increased risks of cancer. Approximately half of DBA cases have a germline mutation or deletion in a ribosomal protein gene (i.e., RPS19, RPS24, RPS17, RPL35A, RPL5, RPL11, RPS7, RPS10, or RPS26), or in GATA1,an X-linked hematopoietic transcription factor. The inheritance of mutated ribosomal protein genes is autosomal dominant (AD), but de novogermline mutations may also occur. We previously reported a novel nonsynonymous ribosomal protein S29 (RPS29) mutation, I31F, which segregated with DBA in a large multi-case family (NCI-193). We now present functional data that link this RPS29mutation to the DBA phenotype and report an additional large multi-case DBA family (NCI-38) with another novel RPS29mutation.

Published

2013

13. Germline Mutations in RTEL1 cause Dyskeratosis Congenita

Author

Ballew, Bari J., Jacobs, Kevin B., Yeager, Meredith, Giri, Neelam, Boland, Joseph F., Hicks, Belynda D., Burdett, Laurie, Hutchinson, Amy A., Alter, Blanche P., and Savage, Sharon A.

Abstract

No relevant conflicts of interest to declare.

Published

2012

14. RPS29 is Mutated in a Multi-Case Diamond Blackfan Anemia Family

Author

Mirabello, Lisa, Ballew, Bari J., Giri, Neelam, Jacobs, Kevin B., Yeager, Meredith, Boland, Joseph F., Hicks, Belynda D., Burdett, Laurie, Hutchinson, Amy A., Alter, Blanche P., and Savage, Sharon A.

Abstract

No relevant conflicts of interest to declare.

Published

2012

15. Germline Mutations in RTEL1cause Dyskeratosis Congenita

Author

Ballew, Bari J., Jacobs, Kevin B., Yeager, Meredith, Giri, Neelam, Boland, Joseph F., Hicks, Belynda D., Burdett, Laurie, Hutchinson, Amy A., Alter, Blanche P., and Savage, Sharon A.

Abstract

Abstract 515This icon denotes a clinically relevant abstract

Published

2012

16. RPS29is Mutated in a Multi-Case Diamond Blackfan Anemia Family

Author

Mirabello, Lisa, Ballew, Bari J., Giri, Neelam, Jacobs, Kevin B., Yeager, Meredith, Boland, Joseph F., Hicks, Belynda D., Burdett, Laurie, Hutchinson, Amy A., Alter, Blanche P., and Savage, Sharon A.

Abstract

Abstract 511This icon denotes a clinically relevant abstract

Published

2012

17. An unusual suspect: an uncommon human-specific synonymous coding variant within the UGT1A6gene explains a GWAS signal and protects against bladder cancer

Author

Tang, Wei, Fu, Yi-Ping, Figueroa, Jonine D, Malats, Núria, Garcia-Closas, Montserrat, Chatterjee, Nilanjan, Kogevinas, Manolis, Baris, Dalsu, Thun, Michael, Hall, Jennifer L, De Vivo, Immaculata, Albanes, Demetrius, Porter-Gill, Patricia, Purdue, Mark P, Burdett, Laurie, Liu, Luyang, Hutchinson, Amy, Myers, Timothy, Tardón, Adonina, Serra, Consol, Carrato, Alfredo, Garcia-Closas, Reina, Lloreta, Josep, Johnson, Alison, Schwenn, Molly, Karagas, Margaret R, Schned, Alan, Black, Amanda, Jacobs, Eric J, Diver, W Ryan, Gapstur, Susan M, Virtamo, Jarmo, Hunter, David J, Fraumeni, Joseph F, Chanock, Stephen J, Silverman, Debra T, Rothman, Nathaniel, and Prokunina-Olsson, Ludmila

Published

2011

18. An unusual suspect: an uncommon human-specific synonymous coding variant within the UGT1A6gene explains a GWAS signal and protects against bladder cancer

Author

Tang, Wei, Fu, Yi-Ping, Figueroa, Jonine D, Malats, Núria, Garcia-Closas, Montserrat, Chatterjee, Nilanjan, Kogevinas, Manolis, Baris, Dalsu, Thun, Michael, Hall, Jennifer L, De Vivo, Immaculata, Albanes, Demetrius, Porter-Gill, Patricia, Purdue, Mark P, Burdett, Laurie, Liu, Luyang, Hutchinson, Amy, Myers, Timothy, Tardón, Adonina, Serra, Consol, Carrato, Alfredo, Garcia-Closas, Reina, Lloreta, Josep, Johnson, Alison, Schwenn, Molly, Karagas, Margaret R, Schned, Alan, Black, Amanda, Jacobs, Eric J, Diver, W Ryan, Gapstur, Susan M, Virtamo, Jarmo, Hunter, David J, Fraumeni, Joseph F, Chanock, Stephen J, Silverman, Debra T, Rothman, Nathaniel, and Prokunina-Olsson, Ludmila

Published

2011