Heterogeneous genetic architectures of prostate cancer susceptibility in sub-Saharan Africa

Rohini Janivara; Wenlong C. Chen; Ujani Hazra; Shakuntala Baichoo; Ilir Agalliu; Paidamoyo Kachambwa; Corrine N. Simonti; Lyda M. Brown; Saanika P. Tambe; Michelle S. Kim; Maxine Harlemon; Mohamed Jalloh; Dillon Muzondiwa; Daphne Naidoo; Olabode O. Ajayi; Nana Yaa Snyper; Lamine Niang; Halimatou Diop; Medina Ndoye; James E. Mensah; Afua O.D. Abrahams; Richard Biritwum; Andrew A. Adjei; Akindele O. Adebiyi; Olayiwola Shittu; Olufemi Ogunbiyi; Sikiru Adebayo; Maxwell M. Nwegbu; Hafees O. Ajibola; Olabode P. Oluwole; Mustapha A. Jamda; Audrey Pentz; Christopher A. Haiman; Petrus V. Spies; André van der Merwe; Michael B. Cook; Stephen J. Chanock; Sonja I. Berndt; Stephen Watya; Alexander Lubwama; Mazvita Muchengeti; Sean Doherty; Natalie Smyth; David Lounsbury; Brian Fortier; Thomas E. Rohan; Judith S. Jacobson; Alfred I. Neugut; Ann W. Hsing; Alexander Gusev; Oseremen I. Aisuodionoe-Shadrach; Maureen Joffe; Ben Adusei; Serigne M. Gueye; Pedro W. Fernandez; Jo McBride; Caroline Andrews; Lindsay N. Petersen; Joseph Lachance; Timothy R. Rebbeck

doi:10.1038/s41588-024-01931-3

Heterogeneous genetic architectures of prostate cancer susceptibility in sub-Saharan Africa

Rohini Janivara
, Wenlong C. Chen
, Ujani Hazra
, Shakuntala Baichoo
, Ilir Agalliu
, Paidamoyo Kachambwa
, Corrine N. Simonti
, Lyda M. Brown
, Saanika P. Tambe
, Michelle S. Kim
, Maxine Harlemon
, Mohamed Jalloh
, Dillon Muzondiwa
, Daphne Naidoo
, Olabode O. Ajayi
, Nana Yaa Snyper
, Lamine Niang
, Halimatou Diop
, Medina Ndoye
, James E. Mensah

Afua O.D. Abrahams, Richard Biritwum, Andrew A. Adjei, Akindele O. Adebiyi, Olayiwola Shittu, Olufemi Ogunbiyi, Sikiru Adebayo, Maxwell M. Nwegbu, Hafees O. Ajibola, Olabode P. Oluwole, Mustapha A. Jamda, Audrey Pentz, Christopher A. Haiman, Petrus V. Spies, André van der Merwe, Michael B. Cook, Stephen J. Chanock, Sonja I. Berndt, Stephen Watya, Alexander Lubwama, Mazvita Muchengeti, Sean Doherty, Natalie Smyth, David Lounsbury, Brian Fortier, Thomas E. Rohan, Judith S. Jacobson, Alfred I. Neugut, Ann W. Hsing, Alexander Gusev, Oseremen I. Aisuodionoe-Shadrach, Maureen Joffe, Ben Adusei, Serigne M. Gueye, Pedro W. Fernandez, Jo McBride, Caroline Andrews, Lindsay N. Petersen, Joseph Lachance, Timothy R. Rebbeck

Georgia Institute of Technology
University of the Witwatersrand
National Health Laboratory Services
University of Mauritius
Albert Einstein College of Medicine of Yeshiva University
Center for Proteomic and Genomic Research
Mediclinic Precise Southern Africa
Université Cheikh Anta Diop de Dakar
Université Iba Der Thiam de Thiès
37 Military Hospital
University of Ghana
College of Medicine, University of Ibadan
University of Abuja
Keck School of Medicine of USC
Stellenbosch University
National Institutes of Health
Uro Care
Dana-Farber Cancer Institute
International Center for AIDS Care and Treatment Programs-Columbia University
Stanford Cancer Institute
Harvard T.H. Chan School of Public Health

Research output: Contribution to journal › Article › peer-review

10 Citations (Scopus)

Abstract

Men of African descent have the highest prostate cancer incidence and mortality rates, yet the genetic basis of prostate cancer in African men has been understudied. We used genomic data from 3,963 cases and 3,509 controls from Ghana, Nigeria, Senegal, South Africa and Uganda to infer ancestry-specific genetic architectures and fine-map disease associations. Fifteen independent associations at 8q24.21, 6q22.1 and 11q13.3 reached genome-wide significance, including four new associations. Intriguingly, multiple lead associations are private alleles, a pattern arising from recent mutations and the out-of-Africa bottleneck. These African-specific alleles contribute to haplotypes with odds ratios above 2.4. We found that the genetic architecture of prostate cancer differs across Africa, with effect size differences contributing more to this heterogeneity than allele frequency differences. Population genetic analyses reveal that African prostate cancer associations are largely governed by neutral evolution. Collectively, our findings emphasize the utility of conducting genetic studies that use diverse populations.

Original language	English
Pages (from-to)	2093-2103
Number of pages	11
Journal	Nature Genetics
Volume	56
Issue number	10
DOIs	https://doi.org/10.1038/s41588-024-01931-3
Publication status	Published - Oct 2024

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SDG 3 Good Health and Well-being

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10.1038/s41588-024-01931-3

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Janivara, R., Chen, W. C., Hazra, U., Baichoo, S., Agalliu, I., Kachambwa, P., Simonti, C. N., Brown, L. M., Tambe, S. P., Kim, M. S., Harlemon, M., Jalloh, M., Muzondiwa, D., Naidoo, D., Ajayi, O. O., Snyper, N. Y., Niang, L., Diop, H., Ndoye, M., ... Rebbeck, T. R. (2024). Heterogeneous genetic architectures of prostate cancer susceptibility in sub-Saharan Africa. Nature Genetics, 56(10), 2093-2103. https://doi.org/10.1038/s41588-024-01931-3

@article{579a5a55368e49128e6ec4852cf87962,

title = "Heterogeneous genetic architectures of prostate cancer susceptibility in sub-Saharan Africa",

abstract = "Men of African descent have the highest prostate cancer incidence and mortality rates, yet the genetic basis of prostate cancer in African men has been understudied. We used genomic data from 3,963 cases and 3,509 controls from Ghana, Nigeria, Senegal, South Africa and Uganda to infer ancestry-specific genetic architectures and fine-map disease associations. Fifteen independent associations at 8q24.21, 6q22.1 and 11q13.3 reached genome-wide significance, including four new associations. Intriguingly, multiple lead associations are private alleles, a pattern arising from recent mutations and the out-of-Africa bottleneck. These African-specific alleles contribute to haplotypes with odds ratios above 2.4. We found that the genetic architecture of prostate cancer differs across Africa, with effect size differences contributing more to this heterogeneity than allele frequency differences. Population genetic analyses reveal that African prostate cancer associations are largely governed by neutral evolution. Collectively, our findings emphasize the utility of conducting genetic studies that use diverse populations.",

author = "Rohini Janivara and Chen, \{Wenlong C.\} and Ujani Hazra and Shakuntala Baichoo and Ilir Agalliu and Paidamoyo Kachambwa and Simonti, \{Corrine N.\} and Brown, \{Lyda M.\} and Tambe, \{Saanika P.\} and Kim, \{Michelle S.\} and Maxine Harlemon and Mohamed Jalloh and Dillon Muzondiwa and Daphne Naidoo and Ajayi, \{Olabode O.\} and Snyper, \{Nana Yaa\} and Lamine Niang and Halimatou Diop and Medina Ndoye and Mensah, \{James E.\} and Abrahams, \{Afua O.D.\} and Richard Biritwum and Adjei, \{Andrew A.\} and Adebiyi, \{Akindele O.\} and Olayiwola Shittu and Olufemi Ogunbiyi and Sikiru Adebayo and Nwegbu, \{Maxwell M.\} and Ajibola, \{Hafees O.\} and Oluwole, \{Olabode P.\} and Jamda, \{Mustapha A.\} and Audrey Pentz and Haiman, \{Christopher A.\} and Spies, \{Petrus V.\} and \{van der Merwe\}, Andr{\'e} and Cook, \{Michael B.\} and Chanock, \{Stephen J.\} and Berndt, \{Sonja I.\} and Stephen Watya and Alexander Lubwama and Mazvita Muchengeti and Sean Doherty and Natalie Smyth and David Lounsbury and Brian Fortier and Rohan, \{Thomas E.\} and Jacobson, \{Judith S.\} and Neugut, \{Alfred I.\} and Hsing, \{Ann W.\} and Alexander Gusev and Aisuodionoe-Shadrach, \{Oseremen I.\} and Maureen Joffe and Ben Adusei and Gueye, \{Serigne M.\} and Fernandez, \{Pedro W.\} and Jo McBride and Caroline Andrews and Petersen, \{Lindsay N.\} and Joseph Lachance and Rebbeck, \{Timothy R.\}",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature America, Inc. 2024.",

year = "2024",

month = oct,

doi = "10.1038/s41588-024-01931-3",

language = "English",

volume = "56",

pages = "2093--2103",

journal = "Nature Genetics",

issn = "1061-4036",

publisher = "Nature Research",

number = "10",

}

Janivara, R, Chen, WC, Hazra, U, Baichoo, S, Agalliu, I, Kachambwa, P, Simonti, CN, Brown, LM, Tambe, SP, Kim, MS, Harlemon, M, Jalloh, M, Muzondiwa, D, Naidoo, D, Ajayi, OO, Snyper, NY, Niang, L, Diop, H, Ndoye, M, Mensah, JE , Abrahams, AOD, Biritwum, R, Adjei, AA, Adebiyi, AO, Shittu, O, Ogunbiyi, O, Adebayo, S, Nwegbu, MM, Ajibola, HO, Oluwole, OP, Jamda, MA, Pentz, A, Haiman, CA, Spies, PV, van der Merwe, A, Cook, MB, Chanock, SJ, Berndt, SI, Watya, S, Lubwama, A, Muchengeti, M, Doherty, S, Smyth, N, Lounsbury, D, Fortier, B, Rohan, TE, Jacobson, JS, Neugut, AI, Hsing, AW, Gusev, A, Aisuodionoe-Shadrach, OI, Joffe, M, Adusei, B, Gueye, SM, Fernandez, PW, McBride, J, Andrews, C, Petersen, LN, Lachance, J & Rebbeck, TR 2024, 'Heterogeneous genetic architectures of prostate cancer susceptibility in sub-Saharan Africa', Nature Genetics, vol. 56, no. 10, pp. 2093-2103. https://doi.org/10.1038/s41588-024-01931-3

TY - JOUR

T1 - Heterogeneous genetic architectures of prostate cancer susceptibility in sub-Saharan Africa

AU - Janivara, Rohini

AU - Chen, Wenlong C.

AU - Hazra, Ujani

AU - Baichoo, Shakuntala

AU - Agalliu, Ilir

AU - Kachambwa, Paidamoyo

AU - Simonti, Corrine N.

AU - Brown, Lyda M.

AU - Tambe, Saanika P.

AU - Kim, Michelle S.

AU - Harlemon, Maxine

AU - Jalloh, Mohamed

AU - Muzondiwa, Dillon

AU - Naidoo, Daphne

AU - Ajayi, Olabode O.

AU - Snyper, Nana Yaa

AU - Niang, Lamine

AU - Diop, Halimatou

AU - Ndoye, Medina

AU - Mensah, James E.

AU - Abrahams, Afua O.D.

AU - Biritwum, Richard

AU - Adjei, Andrew A.

AU - Adebiyi, Akindele O.

AU - Shittu, Olayiwola

AU - Ogunbiyi, Olufemi

AU - Adebayo, Sikiru

AU - Nwegbu, Maxwell M.

AU - Ajibola, Hafees O.

AU - Oluwole, Olabode P.

AU - Jamda, Mustapha A.

AU - Pentz, Audrey

AU - Haiman, Christopher A.

AU - Spies, Petrus V.

AU - van der Merwe, André

AU - Cook, Michael B.

AU - Chanock, Stephen J.

AU - Berndt, Sonja I.

AU - Watya, Stephen

AU - Lubwama, Alexander

AU - Muchengeti, Mazvita

AU - Doherty, Sean

AU - Smyth, Natalie

AU - Lounsbury, David

AU - Fortier, Brian

AU - Rohan, Thomas E.

AU - Jacobson, Judith S.

AU - Neugut, Alfred I.

AU - Hsing, Ann W.

AU - Gusev, Alexander

AU - Aisuodionoe-Shadrach, Oseremen I.

AU - Joffe, Maureen

AU - Adusei, Ben

AU - Gueye, Serigne M.

AU - Fernandez, Pedro W.

AU - McBride, Jo

AU - Andrews, Caroline

AU - Petersen, Lindsay N.

AU - Lachance, Joseph

AU - Rebbeck, Timothy R.

PY - 2024/10

Y1 - 2024/10

N2 - Men of African descent have the highest prostate cancer incidence and mortality rates, yet the genetic basis of prostate cancer in African men has been understudied. We used genomic data from 3,963 cases and 3,509 controls from Ghana, Nigeria, Senegal, South Africa and Uganda to infer ancestry-specific genetic architectures and fine-map disease associations. Fifteen independent associations at 8q24.21, 6q22.1 and 11q13.3 reached genome-wide significance, including four new associations. Intriguingly, multiple lead associations are private alleles, a pattern arising from recent mutations and the out-of-Africa bottleneck. These African-specific alleles contribute to haplotypes with odds ratios above 2.4. We found that the genetic architecture of prostate cancer differs across Africa, with effect size differences contributing more to this heterogeneity than allele frequency differences. Population genetic analyses reveal that African prostate cancer associations are largely governed by neutral evolution. Collectively, our findings emphasize the utility of conducting genetic studies that use diverse populations.

AB - Men of African descent have the highest prostate cancer incidence and mortality rates, yet the genetic basis of prostate cancer in African men has been understudied. We used genomic data from 3,963 cases and 3,509 controls from Ghana, Nigeria, Senegal, South Africa and Uganda to infer ancestry-specific genetic architectures and fine-map disease associations. Fifteen independent associations at 8q24.21, 6q22.1 and 11q13.3 reached genome-wide significance, including four new associations. Intriguingly, multiple lead associations are private alleles, a pattern arising from recent mutations and the out-of-Africa bottleneck. These African-specific alleles contribute to haplotypes with odds ratios above 2.4. We found that the genetic architecture of prostate cancer differs across Africa, with effect size differences contributing more to this heterogeneity than allele frequency differences. Population genetic analyses reveal that African prostate cancer associations are largely governed by neutral evolution. Collectively, our findings emphasize the utility of conducting genetic studies that use diverse populations.

UR - https://www.scopus.com/pages/publications/85205442439

U2 - 10.1038/s41588-024-01931-3

DO - 10.1038/s41588-024-01931-3

M3 - Article

AN - SCOPUS:85205442439

SN - 1061-4036

VL - 56

SP - 2093

EP - 2103

JO - Nature Genetics

JF - Nature Genetics

IS - 10

ER -

Heterogeneous genetic architectures of prostate cancer susceptibility in sub-Saharan Africa

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