Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway

A. Hunter Shain; Maria Garrido; Thomas Botton; Eric Talevich; Iwei Yeh; J. Zachary Sanborn; Jongsuk Chung; Nicholas J. Wang; Hojabr Kakavand; Graham J. Mann; John F. Thompson; Thomas Wiesner; Ritu Roy; Adam B. Olshen; Alexander Gagnon; Joe W. Gray; Nam Huh; Joe S. Hur; Klaus J. Busam; Richard A. Scolyer; Raymond J. Cho; Rajmohan Murali; Boris C. Bastian

doi:10.1038/ng.3382

Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway

A. Hunter Shain, Maria Garrido, Thomas Botton, Eric Talevich, Iwei Yeh, J. Zachary Sanborn, Jongsuk Chung, Nicholas J. Wang, Hojabr Kakavand, Graham J. Mann, John F. Thompson, Thomas Wiesner, Ritu Roy, Adam B. Olshen, Alexander Gagnon, Joe W. Gray, Nam Huh, Joe S. Hur, Klaus J. Busam, Richard A. ScolyerRaymond J. Cho, Rajmohan Murali, Boris C. Bastian

Center for Spatial Systems Biomedicine

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Abstract

Desmoplastic melanoma is an uncommon variant of melanoma with sarcomatous histology, distinct clinical behavior and unknown pathogenesis. We performed low-coverage genome and high-coverage exome sequencing of 20 desmoplastic melanomas, followed by targeted sequencing of 293 genes in a validation cohort of 42 cases. A high mutation burden (median of 62 mutations/Mb) ranked desmoplastic melanoma among the most highly mutated cancers. Mutation patterns strongly implicate ultraviolet radiation as the dominant mutagen, indicating a superficially located cell of origin. Newly identified alterations included recurrent promoter mutations of NFKBIE, encoding NF-κB inhibitor ε (IκBε), in 14.5% of samples. Common oncogenic mutations in melanomas, in particular in BRAF (encoding p.Val600Glu) and NRAS (encoding p.Gln61Lys or p.Gln61Arg), were absent. Instead, other genetic alterations known to activate the MAPK and PI3K signaling cascades were identified in 73% of samples, affecting NF1, CBL, ERBB2, MAP2K1, MAP3K1, BRAF, EGFR, PTPN11, MET, RAC1, SOS2, NRAS and PIK3CA, some of which are candidates for targeted therapies.

Original language	English (US)
Pages (from-to)	1194-1199
Number of pages	6
Journal	Nature genetics
Volume	47
Issue number	10
DOIs	https://doi.org/10.1038/ng.3382
State	Published - Sep 29 2015

ASJC Scopus subject areas

Genetics

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Shain, A. H., Garrido, M., Botton, T., Talevich, E., Yeh, I., Sanborn, J. Z., Chung, J., Wang, N. J., Kakavand, H., Mann, G. J., Thompson, J. F., Wiesner, T., Roy, R., Olshen, A. B., Gagnon, A., Gray, J. W., Huh, N., Hur, J. S., Busam, K. J., ... Bastian, B. C. (2015). Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway. Nature genetics, 47(10), 1194-1199. https://doi.org/10.1038/ng.3382

Shain, AH, Garrido, M, Botton, T, Talevich, E, Yeh, I, Sanborn, JZ, Chung, J, Wang, NJ, Kakavand, H, Mann, GJ, Thompson, JF, Wiesner, T, Roy, R, Olshen, AB, Gagnon, A, Gray, JW, Huh, N, Hur, JS, Busam, KJ, Scolyer, RA, Cho, RJ, Murali, R & Bastian, BC 2015, 'Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway', Nature genetics, vol. 47, no. 10, pp. 1194-1199. https://doi.org/10.1038/ng.3382

@article{a86ee685302a4eb789035d711aa722fa,

title = "Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway",

abstract = "Desmoplastic melanoma is an uncommon variant of melanoma with sarcomatous histology, distinct clinical behavior and unknown pathogenesis. We performed low-coverage genome and high-coverage exome sequencing of 20 desmoplastic melanomas, followed by targeted sequencing of 293 genes in a validation cohort of 42 cases. A high mutation burden (median of 62 mutations/Mb) ranked desmoplastic melanoma among the most highly mutated cancers. Mutation patterns strongly implicate ultraviolet radiation as the dominant mutagen, indicating a superficially located cell of origin. Newly identified alterations included recurrent promoter mutations of NFKBIE, encoding NF-κB inhibitor ε (IκBε), in 14.5% of samples. Common oncogenic mutations in melanomas, in particular in BRAF (encoding p.Val600Glu) and NRAS (encoding p.Gln61Lys or p.Gln61Arg), were absent. Instead, other genetic alterations known to activate the MAPK and PI3K signaling cascades were identified in 73% of samples, affecting NF1, CBL, ERBB2, MAP2K1, MAP3K1, BRAF, EGFR, PTPN11, MET, RAC1, SOS2, NRAS and PIK3CA, some of which are candidates for targeted therapies.",

author = "Shain, {A. Hunter} and Maria Garrido and Thomas Botton and Eric Talevich and Iwei Yeh and Sanborn, {J. Zachary} and Jongsuk Chung and Wang, {Nicholas J.} and Hojabr Kakavand and Mann, {Graham J.} and Thompson, {John F.} and Thomas Wiesner and Ritu Roy and Olshen, {Adam B.} and Alexander Gagnon and Gray, {Joe W.} and Nam Huh and Hur, {Joe S.} and Busam, {Klaus J.} and Scolyer, {Richard A.} and Cho, {Raymond J.} and Rajmohan Murali and Bastian, {Boris C.}",

note = "Funding Information: This work was supported by US National Institutes of Health grants R01 CA131524 (B.C.B.), P01 CA025874 (B.C.B.), P30 CA82103 (A.B.O.) and 5T32 CA177555-02 (A.H.S.), the American Skin Association (B.C.B.), the Gerson and Barbara Bakar Distinguished Chair in Cancer Biology (B.C.B.), the Well Aging Research Center at the Samsung Advanced Institute of Technology under the auspices of S.C. Park, the Dermatology Foundation and US National Institutes of Health grants K08 CA169865 (R.J.C.), U54 CA112970 (J.W.G.) and the Oregon Health and Sciences University Knight Cancer Institute 5P30 CA069533 (J.W.G.). The authors acknowledge support from the Australian National Health and Medical Research Council, Cancer Institute New South Wales, the Melanoma Foundation of the University of Sydney and the staff of Melanoma Institute Australia and Royal Prince Alfred Hospital. Finally, we would like to thank A. Ribas (UCLA Jonsson Comprehensive Cancer Center) and G. Long (Melanoma Institute Australia) for providing samples used in this study. Publisher Copyright: {\textcopyright} 2015 Nature America, Inc.",

year = "2015",

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doi = "10.1038/ng.3382",

language = "English (US)",

volume = "47",

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T1 - Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway

AU - Shain, A. Hunter

AU - Garrido, Maria

AU - Botton, Thomas

AU - Talevich, Eric

AU - Yeh, Iwei

AU - Sanborn, J. Zachary

AU - Chung, Jongsuk

AU - Wang, Nicholas J.

AU - Kakavand, Hojabr

AU - Mann, Graham J.

AU - Thompson, John F.

AU - Wiesner, Thomas

AU - Roy, Ritu

AU - Olshen, Adam B.

AU - Gagnon, Alexander

AU - Gray, Joe W.

AU - Huh, Nam

AU - Hur, Joe S.

AU - Busam, Klaus J.

AU - Scolyer, Richard A.

AU - Cho, Raymond J.

AU - Murali, Rajmohan

AU - Bastian, Boris C.

N1 - Funding Information: This work was supported by US National Institutes of Health grants R01 CA131524 (B.C.B.), P01 CA025874 (B.C.B.), P30 CA82103 (A.B.O.) and 5T32 CA177555-02 (A.H.S.), the American Skin Association (B.C.B.), the Gerson and Barbara Bakar Distinguished Chair in Cancer Biology (B.C.B.), the Well Aging Research Center at the Samsung Advanced Institute of Technology under the auspices of S.C. Park, the Dermatology Foundation and US National Institutes of Health grants K08 CA169865 (R.J.C.), U54 CA112970 (J.W.G.) and the Oregon Health and Sciences University Knight Cancer Institute 5P30 CA069533 (J.W.G.). The authors acknowledge support from the Australian National Health and Medical Research Council, Cancer Institute New South Wales, the Melanoma Foundation of the University of Sydney and the staff of Melanoma Institute Australia and Royal Prince Alfred Hospital. Finally, we would like to thank A. Ribas (UCLA Jonsson Comprehensive Cancer Center) and G. Long (Melanoma Institute Australia) for providing samples used in this study. Publisher Copyright: © 2015 Nature America, Inc.

PY - 2015/9/29

Y1 - 2015/9/29

N2 - Desmoplastic melanoma is an uncommon variant of melanoma with sarcomatous histology, distinct clinical behavior and unknown pathogenesis. We performed low-coverage genome and high-coverage exome sequencing of 20 desmoplastic melanomas, followed by targeted sequencing of 293 genes in a validation cohort of 42 cases. A high mutation burden (median of 62 mutations/Mb) ranked desmoplastic melanoma among the most highly mutated cancers. Mutation patterns strongly implicate ultraviolet radiation as the dominant mutagen, indicating a superficially located cell of origin. Newly identified alterations included recurrent promoter mutations of NFKBIE, encoding NF-κB inhibitor ε (IκBε), in 14.5% of samples. Common oncogenic mutations in melanomas, in particular in BRAF (encoding p.Val600Glu) and NRAS (encoding p.Gln61Lys or p.Gln61Arg), were absent. Instead, other genetic alterations known to activate the MAPK and PI3K signaling cascades were identified in 73% of samples, affecting NF1, CBL, ERBB2, MAP2K1, MAP3K1, BRAF, EGFR, PTPN11, MET, RAC1, SOS2, NRAS and PIK3CA, some of which are candidates for targeted therapies.

AB - Desmoplastic melanoma is an uncommon variant of melanoma with sarcomatous histology, distinct clinical behavior and unknown pathogenesis. We performed low-coverage genome and high-coverage exome sequencing of 20 desmoplastic melanomas, followed by targeted sequencing of 293 genes in a validation cohort of 42 cases. A high mutation burden (median of 62 mutations/Mb) ranked desmoplastic melanoma among the most highly mutated cancers. Mutation patterns strongly implicate ultraviolet radiation as the dominant mutagen, indicating a superficially located cell of origin. Newly identified alterations included recurrent promoter mutations of NFKBIE, encoding NF-κB inhibitor ε (IκBε), in 14.5% of samples. Common oncogenic mutations in melanomas, in particular in BRAF (encoding p.Val600Glu) and NRAS (encoding p.Gln61Lys or p.Gln61Arg), were absent. Instead, other genetic alterations known to activate the MAPK and PI3K signaling cascades were identified in 73% of samples, affecting NF1, CBL, ERBB2, MAP2K1, MAP3K1, BRAF, EGFR, PTPN11, MET, RAC1, SOS2, NRAS and PIK3CA, some of which are candidates for targeted therapies.

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Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway

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