Association of germline variants in the APOBEC3 region with cancer risk and enrichment with APOBEC-signature mutations in tumors

Candace D Middlebrooks; A Rouf Banday; Konichi Matsuda; Krizia-Ivana Udquim; Olusegun O Onabajo; Ashley Paquin; Jonine D Figueroa; Bin Zhu; Stella Koutros; Michiaki Kubo; Taro Shuin; Neal D Freedman; Manolis Kogevinas; Nuria Malats; Stephen J Chanock; Montserrat Garcia-Closas; Debra T Silverman; Nathaniel Rothman; Ludmila Prokunina-Olsson

doi:10.1038/ng.3670

Association of germline variants in the APOBEC3 region with cancer risk and enrichment with APOBEC-signature mutations in tumors

Candace D Middlebrooks, A Rouf Banday, Konichi Matsuda, Krizia-Ivana Udquim, Olusegun O Onabajo, Ashley Paquin, Jonine D Figueroa, Bin Zhu, Stella Koutros, Michiaki Kubo, Taro Shuin, Neal D Freedman, Manolis Kogevinas, Nuria Malats, Stephen J Chanock, Montserrat Garcia-Closas, Debra T Silverman, Nathaniel Rothman, Ludmila Prokunina-Olsson

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

Abstract

High rates of APOBEC-signature mutations are found in many tumors, but factors affecting this mutation pattern are not well understood. Here we explored the contribution of two common germline variants in the APOBEC3 region. SNP rs1014971 was associated with bladder cancer risk, increased APOBEC3B expression, and enrichment with APOBEC-signature mutations in bladder tumors. In contrast, a 30-kb deletion that eliminates APOBEC3B and creates an APOBEC3A–APOBEC3B chimera was not important in bladder cancer, whereas it was associated with breast cancer risk and enrichment with APOBEC-signature mutations in breast tumors. In vitro, APOBEC3B expression was predominantly induced by treatment with a DNA-damaging drug in bladder cancer cell lines, and APOBEC3A expression was induced as part of the antiviral interferon-stimulated response in breast cancer cell lines. These findings suggest a tissue-specific role of environmental oncogenic triggers, particularly in individuals with germline APOBEC3 risk variants.

Original language	English
Pages (from-to)	1330–1338
Number of pages	9
Journal	Nature Genetics
Volume	48
Issue number	11
Early online date	19 Sep 2016
DOIs	https://doi.org/10.1038/ng.3670
Publication status	Published - Nov 2016

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Jonine Figueroa
- Deanery of Molecular, Genetic and Population Health Sciences - UoE Honorary staff
Person: Affiliated Independent Researcher

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Middlebrooks, C. D., Banday, A. R., Matsuda, K., Udquim, K-I., Onabajo, O. O., Paquin, A., Figueroa, J. D., Zhu, B., Koutros, S., Kubo, M., Shuin, T., Freedman, N. D., Kogevinas, M., Malats, N., Chanock, S. J., Garcia-Closas, M., Silverman, D. T., Rothman, N., & Prokunina-Olsson, L. (2016). Association of germline variants in the APOBEC3 region with cancer risk and enrichment with APOBEC-signature mutations in tumors. Nature Genetics, 48(11), 1330–1338. https://doi.org/10.1038/ng.3670

@article{fa78b05ee2f641098bc3a0b3249c3aba,

title = "Association of germline variants in the APOBEC3 region with cancer risk and enrichment with APOBEC-signature mutations in tumors",

abstract = "High rates of APOBEC-signature mutations are found in many tumors, but factors affecting this mutation pattern are not well understood. Here we explored the contribution of two common germline variants in the APOBEC3 region. SNP rs1014971 was associated with bladder cancer risk, increased APOBEC3B expression, and enrichment with APOBEC-signature mutations in bladder tumors. In contrast, a 30-kb deletion that eliminates APOBEC3B and creates an APOBEC3A–APOBEC3B chimera was not important in bladder cancer, whereas it was associated with breast cancer risk and enrichment with APOBEC-signature mutations in breast tumors. In vitro, APOBEC3B expression was predominantly induced by treatment with a DNA-damaging drug in bladder cancer cell lines, and APOBEC3A expression was induced as part of the antiviral interferon-stimulated response in breast cancer cell lines. These findings suggest a tissue-specific role of environmental oncogenic triggers, particularly in individuals with germline APOBEC3 risk variants.",

author = "Middlebrooks, {Candace D} and Banday, {A Rouf} and Konichi Matsuda and Krizia-Ivana Udquim and Onabajo, {Olusegun O} and Ashley Paquin and Figueroa, {Jonine D} and Bin Zhu and Stella Koutros and Michiaki Kubo and Taro Shuin and Freedman, {Neal D} and Manolis Kogevinas and Nuria Malats and Chanock, {Stephen J} and Montserrat Garcia-Closas and Silverman, {Debra T} and Nathaniel Rothman and Ludmila Prokunina-Olsson",

year = "2016",

month = nov,

doi = "10.1038/ng.3670",

language = "English",

volume = "48",

pages = "1330–1338",

journal = "Nature Genetics",

issn = "1061-4036",

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Middlebrooks, CD, Banday, AR, Matsuda, K, Udquim, K-I, Onabajo, OO, Paquin, A, Figueroa, JD, Zhu, B, Koutros, S, Kubo, M, Shuin, T, Freedman, ND, Kogevinas, M, Malats, N, Chanock, SJ, Garcia-Closas, M, Silverman, DT, Rothman, N & Prokunina-Olsson, L 2016, 'Association of germline variants in the APOBEC3 region with cancer risk and enrichment with APOBEC-signature mutations in tumors', Nature Genetics, vol. 48, no. 11, pp. 1330–1338. https://doi.org/10.1038/ng.3670

TY - JOUR

T1 - Association of germline variants in the APOBEC3 region with cancer risk and enrichment with APOBEC-signature mutations in tumors

AU - Middlebrooks, Candace D

AU - Banday, A Rouf

AU - Matsuda, Konichi

AU - Udquim, Krizia-Ivana

AU - Onabajo, Olusegun O

AU - Paquin, Ashley

AU - Figueroa, Jonine D

AU - Zhu, Bin

AU - Koutros, Stella

AU - Kubo, Michiaki

AU - Shuin, Taro

AU - Freedman, Neal D

AU - Kogevinas, Manolis

AU - Malats, Nuria

AU - Chanock, Stephen J

AU - Garcia-Closas, Montserrat

AU - Silverman, Debra T

AU - Rothman, Nathaniel

AU - Prokunina-Olsson, Ludmila

PY - 2016/11

Y1 - 2016/11

N2 - High rates of APOBEC-signature mutations are found in many tumors, but factors affecting this mutation pattern are not well understood. Here we explored the contribution of two common germline variants in the APOBEC3 region. SNP rs1014971 was associated with bladder cancer risk, increased APOBEC3B expression, and enrichment with APOBEC-signature mutations in bladder tumors. In contrast, a 30-kb deletion that eliminates APOBEC3B and creates an APOBEC3A–APOBEC3B chimera was not important in bladder cancer, whereas it was associated with breast cancer risk and enrichment with APOBEC-signature mutations in breast tumors. In vitro, APOBEC3B expression was predominantly induced by treatment with a DNA-damaging drug in bladder cancer cell lines, and APOBEC3A expression was induced as part of the antiviral interferon-stimulated response in breast cancer cell lines. These findings suggest a tissue-specific role of environmental oncogenic triggers, particularly in individuals with germline APOBEC3 risk variants.

AB - High rates of APOBEC-signature mutations are found in many tumors, but factors affecting this mutation pattern are not well understood. Here we explored the contribution of two common germline variants in the APOBEC3 region. SNP rs1014971 was associated with bladder cancer risk, increased APOBEC3B expression, and enrichment with APOBEC-signature mutations in bladder tumors. In contrast, a 30-kb deletion that eliminates APOBEC3B and creates an APOBEC3A–APOBEC3B chimera was not important in bladder cancer, whereas it was associated with breast cancer risk and enrichment with APOBEC-signature mutations in breast tumors. In vitro, APOBEC3B expression was predominantly induced by treatment with a DNA-damaging drug in bladder cancer cell lines, and APOBEC3A expression was induced as part of the antiviral interferon-stimulated response in breast cancer cell lines. These findings suggest a tissue-specific role of environmental oncogenic triggers, particularly in individuals with germline APOBEC3 risk variants.

U2 - 10.1038/ng.3670

DO - 10.1038/ng.3670

M3 - Article

VL - 48

SP - 1330

EP - 1338

JO - Nature Genetics

JF - Nature Genetics

SN - 1061-4036

IS - 11

ER -

Association of germline variants in the APOBEC3 region with cancer risk and enrichment with APOBEC-signature mutations in tumors

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