Comprehensive molecular profiling of 718 Multiple Myelomas reveals significant differences in mutation frequencies between African and European descent cases

Zarko Manojlovic; Austin Christofferson; Winnie S. Liang; Jessica Aldrich; Megan Washington; Shukmei Wong; Daniel Rohrer; Scott Jewell; Rick A. Kittles; Mary Derome; Daniel Auclair; David Wesley Craig; Jonathan Keats; John D. Carpten

doi:10.1371/journal.pgen.1007087

Comprehensive molecular profiling of 718 Multiple Myelomas reveals significant differences in mutation frequencies between African and European descent cases

Zarko Manojlovic, Austin Christofferson, Winnie S. Liang, Jessica Aldrich, Megan Washington, Shukmei Wong, Daniel Rohrer, Scott Jewell, Rick A. Kittles, Mary Derome, Daniel Auclair, David Wesley Craig, Jonathan Keats, John D. Carpten

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Abstract

Multiple Myeloma (MM) is a plasma cell malignancy with significantly greater incidence and mortality rates among African Americans (AA) compared to Caucasians (CA). The overall goal of this study is to elucidate differences in molecular alterations in MM as a function of self-reported race and genetic ancestry. Our study utilized somatic whole exome, RNA-sequencing, and correlated clinical data from 718 MM patients from the Multiple Myeloma Research Foundation CoMMpass study Interim Analysis 9. Somatic mutational analyses based upon self-reported race corrected for ancestry revealed significant differences in mutation frequency between groups. Of interest, BCL7A, BRWD3, and AUTS2 demonstrate significantly higher mutation frequencies among AA cases. These genes are all involved in translocations in B-cell malignancies. Moreover, we detected a significant difference in mutation frequency of TP53 and IRF4 with frequencies higher among CA cases. Our study provides rationale for interrogating diverse tumor cohorts to best understand tumor genomics across populations.

Original language	English (US)
Article number	e1007087
Journal	PLoS genetics
Volume	13
Issue number	11
DOIs	https://doi.org/10.1371/journal.pgen.1007087
State	Published - Nov 2017

ASJC Scopus subject areas

Ecology, Evolution, Behavior and Systematics
Molecular Biology
Genetics
Genetics(clinical)
Cancer Research

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Manojlovic, Z., Christofferson, A., Liang, W. S., Aldrich, J., Washington, M., Wong, S., Rohrer, D., Jewell, S., Kittles, R. A., Derome, M., Auclair, D., Craig, D. W., Keats, J., & Carpten, J. D. (2017). Comprehensive molecular profiling of 718 Multiple Myelomas reveals significant differences in mutation frequencies between African and European descent cases. PLoS genetics, 13(11), Article e1007087. https://doi.org/10.1371/journal.pgen.1007087

Manojlovic, Z, Christofferson, A, Liang, WS, Aldrich, J, Washington, M, Wong, S, Rohrer, D, Jewell, S, Kittles, RA, Derome, M, Auclair, D, Craig, DW, Keats, J & Carpten, JD 2017, 'Comprehensive molecular profiling of 718 Multiple Myelomas reveals significant differences in mutation frequencies between African and European descent cases', PLoS genetics, vol. 13, no. 11, e1007087. https://doi.org/10.1371/journal.pgen.1007087

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title = "Comprehensive molecular profiling of 718 Multiple Myelomas reveals significant differences in mutation frequencies between African and European descent cases",

abstract = "Multiple Myeloma (MM) is a plasma cell malignancy with significantly greater incidence and mortality rates among African Americans (AA) compared to Caucasians (CA). The overall goal of this study is to elucidate differences in molecular alterations in MM as a function of self-reported race and genetic ancestry. Our study utilized somatic whole exome, RNA-sequencing, and correlated clinical data from 718 MM patients from the Multiple Myeloma Research Foundation CoMMpass study Interim Analysis 9. Somatic mutational analyses based upon self-reported race corrected for ancestry revealed significant differences in mutation frequency between groups. Of interest, BCL7A, BRWD3, and AUTS2 demonstrate significantly higher mutation frequencies among AA cases. These genes are all involved in translocations in B-cell malignancies. Moreover, we detected a significant difference in mutation frequency of TP53 and IRF4 with frequencies higher among CA cases. Our study provides rationale for interrogating diverse tumor cohorts to best understand tumor genomics across populations.",

author = "Zarko Manojlovic and Austin Christofferson and Liang, {Winnie S.} and Jessica Aldrich and Megan Washington and Shukmei Wong and Daniel Rohrer and Scott Jewell and Kittles, {Rick A.} and Mary Derome and Daniel Auclair and Craig, {David Wesley} and Jonathan Keats and Carpten, {John D.}",

note = "Funding Information: This work was supported from Multiple Myeloma Research Foundation (CoMMpass) MMRF-TGen Carpten and USC-Carpten and Start-up Fund, University of Southern California to JDC. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. The authors would like to thank MMRF CoMMpass Network (Abella, Eugenia; Anderson, Larry; Ascensao, Joao; Azaceta, Gemma; Bahlis, Nizar; Balaraman, Rama; Bar, Michael; Bargay, Joan; Belani, Rajesh; Berdeja, Jesus; Chinea, Anabelle; Conde, Miguel; Costello, Caitlin; Dakhil, Shaker; Fern{\'a}ndez de Larrea, Carlos; Gasparetto, Cristina; Giever, Thomas; Graham, Mark; Granell, Miquel; Grossbard, Michael; Guti{\'e}rrez, Norma; Harroff, Allyson; Hassoun, Hani; Hern{\'a}ndez, Miguel; Hofmeister, Craig; Hsu, Gerald; Jagannath, Sundar; Jakubowiak, Andrzej; Kambhampati, Suman; Kaya, Hakan; Klein, Leonard; Kolibaba, Kathryn; Krsnik, Isabel; Kumar, Shaji; Kuzma, Charles; Levy, Moshe; Lewis, DeQuincy; Liles, Darla; Lonial, Sagar; Lunning, Matthew; Martinez-Chamorro, Carmen; Masso Asensio, Pilar; Matkiwsky, May; Meehan, Kenneth; Menter, Alex; Mikhael, Joseph; Milner, Carter; Min, Frederick; Ngaiza, Justinian; Niesvizky, Ruben; Onitilo, Adedayo; Orloff, Gregory; Patel, Dilip; Posada, Juan; Richards, Donald; Rifkin, Robert; R{\'i}os, Pablo; Robles, Robert; Rodr{\'i}guez, Paula; Roy, Vivek; Sampol, Antonia; Scott, Emma; Sebag, Michael; Siegel, David; Solomon, William; Srinivas, Shanti; Trudel, Suzanne; Usmani, Saad; Venner, Christopher; Vij, Ravi; Volterra, Fabio; Wachsman, William; Whittenberger, Brock; Wolf, Jeffrey; Xia, Chunzhi; Yalamanchili, Madhuri; Yost, Kathleen; Zonder, Jeffrey) for their contributions to the CoMMpass patient and data collection. Publisher Copyright: {\textcopyright} 2017 Manojlovic et al.",

year = "2017",

month = nov,

doi = "10.1371/journal.pgen.1007087",

language = "English (US)",

volume = "13",

journal = "PLoS genetics",

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T1 - Comprehensive molecular profiling of 718 Multiple Myelomas reveals significant differences in mutation frequencies between African and European descent cases

AU - Manojlovic, Zarko

AU - Christofferson, Austin

AU - Liang, Winnie S.

AU - Aldrich, Jessica

AU - Washington, Megan

AU - Wong, Shukmei

AU - Rohrer, Daniel

AU - Jewell, Scott

AU - Kittles, Rick A.

AU - Derome, Mary

AU - Auclair, Daniel

AU - Craig, David Wesley

AU - Keats, Jonathan

AU - Carpten, John D.

N1 - Funding Information: This work was supported from Multiple Myeloma Research Foundation (CoMMpass) MMRF-TGen Carpten and USC-Carpten and Start-up Fund, University of Southern California to JDC. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. The authors would like to thank MMRF CoMMpass Network (Abella, Eugenia; Anderson, Larry; Ascensao, Joao; Azaceta, Gemma; Bahlis, Nizar; Balaraman, Rama; Bar, Michael; Bargay, Joan; Belani, Rajesh; Berdeja, Jesus; Chinea, Anabelle; Conde, Miguel; Costello, Caitlin; Dakhil, Shaker; Fernández de Larrea, Carlos; Gasparetto, Cristina; Giever, Thomas; Graham, Mark; Granell, Miquel; Grossbard, Michael; Gutiérrez, Norma; Harroff, Allyson; Hassoun, Hani; Hernández, Miguel; Hofmeister, Craig; Hsu, Gerald; Jagannath, Sundar; Jakubowiak, Andrzej; Kambhampati, Suman; Kaya, Hakan; Klein, Leonard; Kolibaba, Kathryn; Krsnik, Isabel; Kumar, Shaji; Kuzma, Charles; Levy, Moshe; Lewis, DeQuincy; Liles, Darla; Lonial, Sagar; Lunning, Matthew; Martinez-Chamorro, Carmen; Masso Asensio, Pilar; Matkiwsky, May; Meehan, Kenneth; Menter, Alex; Mikhael, Joseph; Milner, Carter; Min, Frederick; Ngaiza, Justinian; Niesvizky, Ruben; Onitilo, Adedayo; Orloff, Gregory; Patel, Dilip; Posada, Juan; Richards, Donald; Rifkin, Robert; Ríos, Pablo; Robles, Robert; Rodríguez, Paula; Roy, Vivek; Sampol, Antonia; Scott, Emma; Sebag, Michael; Siegel, David; Solomon, William; Srinivas, Shanti; Trudel, Suzanne; Usmani, Saad; Venner, Christopher; Vij, Ravi; Volterra, Fabio; Wachsman, William; Whittenberger, Brock; Wolf, Jeffrey; Xia, Chunzhi; Yalamanchili, Madhuri; Yost, Kathleen; Zonder, Jeffrey) for their contributions to the CoMMpass patient and data collection. Publisher Copyright: © 2017 Manojlovic et al.

PY - 2017/11

Y1 - 2017/11

N2 - Multiple Myeloma (MM) is a plasma cell malignancy with significantly greater incidence and mortality rates among African Americans (AA) compared to Caucasians (CA). The overall goal of this study is to elucidate differences in molecular alterations in MM as a function of self-reported race and genetic ancestry. Our study utilized somatic whole exome, RNA-sequencing, and correlated clinical data from 718 MM patients from the Multiple Myeloma Research Foundation CoMMpass study Interim Analysis 9. Somatic mutational analyses based upon self-reported race corrected for ancestry revealed significant differences in mutation frequency between groups. Of interest, BCL7A, BRWD3, and AUTS2 demonstrate significantly higher mutation frequencies among AA cases. These genes are all involved in translocations in B-cell malignancies. Moreover, we detected a significant difference in mutation frequency of TP53 and IRF4 with frequencies higher among CA cases. Our study provides rationale for interrogating diverse tumor cohorts to best understand tumor genomics across populations.

AB - Multiple Myeloma (MM) is a plasma cell malignancy with significantly greater incidence and mortality rates among African Americans (AA) compared to Caucasians (CA). The overall goal of this study is to elucidate differences in molecular alterations in MM as a function of self-reported race and genetic ancestry. Our study utilized somatic whole exome, RNA-sequencing, and correlated clinical data from 718 MM patients from the Multiple Myeloma Research Foundation CoMMpass study Interim Analysis 9. Somatic mutational analyses based upon self-reported race corrected for ancestry revealed significant differences in mutation frequency between groups. Of interest, BCL7A, BRWD3, and AUTS2 demonstrate significantly higher mutation frequencies among AA cases. These genes are all involved in translocations in B-cell malignancies. Moreover, we detected a significant difference in mutation frequency of TP53 and IRF4 with frequencies higher among CA cases. Our study provides rationale for interrogating diverse tumor cohorts to best understand tumor genomics across populations.

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DO - 10.1371/journal.pgen.1007087

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ER -

Comprehensive molecular profiling of 718 Multiple Myelomas reveals significant differences in mutation frequencies between African and European descent cases

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