Whole-exome sequencing identifies recurrent SF3B1 R625 mutation and comutation of NF1 and KIT in mucosal melanoma

Jennifer D. Hintzsche; Nicholas T. Gorden; Carol M. Amato; Jihye Kim; Kelsey E. Wuensch; Steven E. Robinson; Allison J. Applegate; Kasey L. Couts; Theresa M. Medina; Keith R. Wells; Joshua A. Wisell; Martin D. McCarter; Neil F. Box; Yiqun G. Shellman; Rene C. Gonzalez; Karl D. Lewis; John J. Tentler; Aik Choon Tan; William A. Robinson

doi:10.1097/CMR.0000000000000345

Whole-exome sequencing identifies recurrent SF3B1 R625 mutation and comutation of NF1 and KIT in mucosal melanoma

Jennifer D. Hintzsche, Nicholas T. Gorden, Carol M. Amato, Jihye Kim, Kelsey E. Wuensch, Steven E. Robinson, Allison J. Applegate, Kasey L. Couts, Theresa M. Medina, Keith R. Wells, Joshua A. Wisell, Martin D. McCarter, Neil F. Box, Yiqun G. Shellman, Rene C. Gonzalez, Karl D. Lewis, John J. Tentler, Aik Choon Tan, William A. Robinson

Department of Computer Science and Engineering

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

83 Citations (Scopus)

Abstract

Mucosal melanomas are a rare subtype of melanoma, arising in mucosal tissues, which have a very poor prognosis due to the lack of effective targeted therapies. This study aimed to better understand the molecular landscape of these cancers and find potential new therapeutic targets. Whole-exome sequencing was performed on mucosal melanomas from 19 patients and 135 sun-exposed cutaneous melanomas, with matched peripheral blood samples when available. Mutational profiles were compared between mucosal subgroups and sun-exposed cutaneous melanomas. Comparisons of molecular profiles identified 161 genes enriched in mucosal melanoma (P<0.05). KIT and NF1 were frequently comutated (32%) in the mucosal subgroup, with a significantly higher incidence than that in cutaneous melanoma (4%). Recurrent SF3B1 R625H/S/C mutations were identified and validated in 7 of 19 (37%) mucosal melanoma patients. Mutations in the spliceosome pathway were found to be enriched in mucosal melanomas when compared with cutaneous melanomas. Alternative splicing in four genes were observed in SF3B1-mutant samples compared with the wild-type samples. This study identified potential new therapeutic targets for mucosal melanoma, including comutation of NF1 and KIT, and recurrent R625 mutations in SF3B1. This is the first report of SF3B1 R625 mutations in vulvovaginal mucosal melanoma, with the largest whole-exome sequencing project of mucosal melanomas to date. The results here also indicated that the mutations in SF3B1 lead to alternative splicing in multiple genes. These findings expand our knowledge of this rare disease.

Original language	English
Pages (from-to)	189-199
Number of pages	11
Journal	Melanoma Research
Volume	27
Issue number	3
DOIs	https://doi.org/10.1097/CMR.0000000000000345
Publication status	Published - 2017

Keywords

SF3B1 mutation
genomic landscape
mucosal melanoma
spliceosome
whole-exome sequencing

ASJC Scopus subject areas

Oncology
Dermatology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1097/CMR.0000000000000345

Cite this

Hintzsche, J. D., Gorden, N. T., Amato, C. M., Kim, J., Wuensch, K. E., Robinson, S. E., Applegate, A. J., Couts, K. L., Medina, T. M., Wells, K. R., Wisell, J. A., McCarter, M. D., Box, N. F., Shellman, Y. G., Gonzalez, R. C., Lewis, K. D., Tentler, J. J., Tan, A. C., & Robinson, W. A. (2017). Whole-exome sequencing identifies recurrent SF3B1 R625 mutation and comutation of NF1 and KIT in mucosal melanoma. Melanoma Research, 27(3), 189-199. https://doi.org/10.1097/CMR.0000000000000345

Hintzsche, JD, Gorden, NT, Amato, CM, Kim, J, Wuensch, KE, Robinson, SE, Applegate, AJ, Couts, KL, Medina, TM, Wells, KR, Wisell, JA, McCarter, MD, Box, NF, Shellman, YG, Gonzalez, RC, Lewis, KD, Tentler, JJ, Tan, AC & Robinson, WA 2017, 'Whole-exome sequencing identifies recurrent SF3B1 R625 mutation and comutation of NF1 and KIT in mucosal melanoma', Melanoma Research, vol. 27, no. 3, pp. 189-199. https://doi.org/10.1097/CMR.0000000000000345

@article{69c67ee6ad94441585571c5c029fd4e1,

title = "Whole-exome sequencing identifies recurrent SF3B1 R625 mutation and comutation of NF1 and KIT in mucosal melanoma",

abstract = "Mucosal melanomas are a rare subtype of melanoma, arising in mucosal tissues, which have a very poor prognosis due to the lack of effective targeted therapies. This study aimed to better understand the molecular landscape of these cancers and find potential new therapeutic targets. Whole-exome sequencing was performed on mucosal melanomas from 19 patients and 135 sun-exposed cutaneous melanomas, with matched peripheral blood samples when available. Mutational profiles were compared between mucosal subgroups and sun-exposed cutaneous melanomas. Comparisons of molecular profiles identified 161 genes enriched in mucosal melanoma (P<0.05). KIT and NF1 were frequently comutated (32%) in the mucosal subgroup, with a significantly higher incidence than that in cutaneous melanoma (4%). Recurrent SF3B1 R625H/S/C mutations were identified and validated in 7 of 19 (37%) mucosal melanoma patients. Mutations in the spliceosome pathway were found to be enriched in mucosal melanomas when compared with cutaneous melanomas. Alternative splicing in four genes were observed in SF3B1-mutant samples compared with the wild-type samples. This study identified potential new therapeutic targets for mucosal melanoma, including comutation of NF1 and KIT, and recurrent R625 mutations in SF3B1. This is the first report of SF3B1 R625 mutations in vulvovaginal mucosal melanoma, with the largest whole-exome sequencing project of mucosal melanomas to date. The results here also indicated that the mutations in SF3B1 lead to alternative splicing in multiple genes. These findings expand our knowledge of this rare disease.",

keywords = "SF3B1 mutation, genomic landscape, mucosal melanoma, spliceosome, whole-exome sequencing",

author = "Hintzsche, {Jennifer D.} and Gorden, {Nicholas T.} and Amato, {Carol M.} and Jihye Kim and Wuensch, {Kelsey E.} and Robinson, {Steven E.} and Applegate, {Allison J.} and Couts, {Kasey L.} and Medina, {Theresa M.} and Wells, {Keith R.} and Wisell, {Joshua A.} and McCarter, {Martin D.} and Box, {Neil F.} and Shellman, {Yiqun G.} and Gonzalez, {Rene C.} and Lewis, {Karl D.} and Tentler, {John J.} and Tan, {Aik Choon} and Robinson, {William A.}",

note = "Funding Information: This work is partly supported by the National Institutes of Health P30CA046934, Cancer League of Colorado, the David F. and Margaret T. Grohne Family Foundation, the Rifkin Endowed Chair (WAR), the Amy Davis Foundation and the Moore Family Foundation Publisher Copyright: {\textcopyright} 2017 The Author(s). Published by Wolters Kluwer Health, Inc.",

year = "2017",

doi = "10.1097/CMR.0000000000000345",

language = "English",

volume = "27",

pages = "189--199",

journal = "Melanoma Research",

issn = "0960-8931",

publisher = "Lippincott Williams and Wilkins",

number = "3",

}

TY - JOUR

T1 - Whole-exome sequencing identifies recurrent SF3B1 R625 mutation and comutation of NF1 and KIT in mucosal melanoma

AU - Hintzsche, Jennifer D.

AU - Gorden, Nicholas T.

AU - Amato, Carol M.

AU - Kim, Jihye

AU - Wuensch, Kelsey E.

AU - Robinson, Steven E.

AU - Applegate, Allison J.

AU - Couts, Kasey L.

AU - Medina, Theresa M.

AU - Wells, Keith R.

AU - Wisell, Joshua A.

AU - McCarter, Martin D.

AU - Box, Neil F.

AU - Shellman, Yiqun G.

AU - Gonzalez, Rene C.

AU - Lewis, Karl D.

AU - Tentler, John J.

AU - Tan, Aik Choon

AU - Robinson, William A.

N1 - Funding Information: This work is partly supported by the National Institutes of Health P30CA046934, Cancer League of Colorado, the David F. and Margaret T. Grohne Family Foundation, the Rifkin Endowed Chair (WAR), the Amy Davis Foundation and the Moore Family Foundation Publisher Copyright: © 2017 The Author(s). Published by Wolters Kluwer Health, Inc.

PY - 2017

Y1 - 2017

N2 - Mucosal melanomas are a rare subtype of melanoma, arising in mucosal tissues, which have a very poor prognosis due to the lack of effective targeted therapies. This study aimed to better understand the molecular landscape of these cancers and find potential new therapeutic targets. Whole-exome sequencing was performed on mucosal melanomas from 19 patients and 135 sun-exposed cutaneous melanomas, with matched peripheral blood samples when available. Mutational profiles were compared between mucosal subgroups and sun-exposed cutaneous melanomas. Comparisons of molecular profiles identified 161 genes enriched in mucosal melanoma (P<0.05). KIT and NF1 were frequently comutated (32%) in the mucosal subgroup, with a significantly higher incidence than that in cutaneous melanoma (4%). Recurrent SF3B1 R625H/S/C mutations were identified and validated in 7 of 19 (37%) mucosal melanoma patients. Mutations in the spliceosome pathway were found to be enriched in mucosal melanomas when compared with cutaneous melanomas. Alternative splicing in four genes were observed in SF3B1-mutant samples compared with the wild-type samples. This study identified potential new therapeutic targets for mucosal melanoma, including comutation of NF1 and KIT, and recurrent R625 mutations in SF3B1. This is the first report of SF3B1 R625 mutations in vulvovaginal mucosal melanoma, with the largest whole-exome sequencing project of mucosal melanomas to date. The results here also indicated that the mutations in SF3B1 lead to alternative splicing in multiple genes. These findings expand our knowledge of this rare disease.

AB - Mucosal melanomas are a rare subtype of melanoma, arising in mucosal tissues, which have a very poor prognosis due to the lack of effective targeted therapies. This study aimed to better understand the molecular landscape of these cancers and find potential new therapeutic targets. Whole-exome sequencing was performed on mucosal melanomas from 19 patients and 135 sun-exposed cutaneous melanomas, with matched peripheral blood samples when available. Mutational profiles were compared between mucosal subgroups and sun-exposed cutaneous melanomas. Comparisons of molecular profiles identified 161 genes enriched in mucosal melanoma (P<0.05). KIT and NF1 were frequently comutated (32%) in the mucosal subgroup, with a significantly higher incidence than that in cutaneous melanoma (4%). Recurrent SF3B1 R625H/S/C mutations were identified and validated in 7 of 19 (37%) mucosal melanoma patients. Mutations in the spliceosome pathway were found to be enriched in mucosal melanomas when compared with cutaneous melanomas. Alternative splicing in four genes were observed in SF3B1-mutant samples compared with the wild-type samples. This study identified potential new therapeutic targets for mucosal melanoma, including comutation of NF1 and KIT, and recurrent R625 mutations in SF3B1. This is the first report of SF3B1 R625 mutations in vulvovaginal mucosal melanoma, with the largest whole-exome sequencing project of mucosal melanomas to date. The results here also indicated that the mutations in SF3B1 lead to alternative splicing in multiple genes. These findings expand our knowledge of this rare disease.

KW - SF3B1 mutation

KW - genomic landscape

KW - mucosal melanoma

KW - spliceosome

KW - whole-exome sequencing

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M3 - Article

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SN - 0960-8931

VL - 27

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EP - 199

JO - Melanoma Research

JF - Melanoma Research

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ER -

Whole-exome sequencing identifies recurrent SF3B1 R625 mutation and comutation of NF1 and KIT in mucosal melanoma

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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