A novel recurrent mutation in MITF predisposes to familial and sporadic melanoma

Satoru Yokoyama; Susan L. Woods; Glen M. Boyle; Lauren G. Aoude; Stuart MacGregor; Victoria Zismann; Michael Gartside; Anne E. Cust; Rizwan Haq; Mark Harland; John C. Taylor; David L. Duffy; Kelly Holohan; Ken Dutton-Regester; Jane M. Palmer; Vanessa Bonazzi; Mitchell S. Stark; Judith Symmons; Matthew H. Law; Christopher Schmidt; Cathy Lanagan; Linda O'Connor; Elizabeth A. Holland; Helen Schmid; Judith A. Maskiell; Jodie Jetann; Megan Ferguson; Mark A. Jenkins; Richard F. Kefford; Graham G. Giles; Bruce K. Armstrong; Joanne F. Aitken; John L. Hopper; David C. Whiteman; Paul D. Pharoah; Douglas F. Easton; Alison M. Dunning; Julia A. Newton-Bishop; Grant W. Montgomery; Nicholas G. Martin; Graham J. Mann; D. Timothy Bishop; Hensin Tsao; Jeffrey M. Trent; David E. Fisher; Nicholas K. Hayward; Kevin M. Brown

doi:10.1038/nature10630

A novel recurrent mutation in MITF predisposes to familial and sporadic melanoma

Satoru Yokoyama, Susan L. Woods, Glen M. Boyle, Lauren G. Aoude, Stuart MacGregor, Victoria Zismann, Michael Gartside, Anne E. Cust, Rizwan Haq, Mark Harland, John C. Taylor, David L. Duffy, Kelly Holohan, Ken Dutton-Regester, Jane M. Palmer, Vanessa Bonazzi, Mitchell S. Stark, Judith Symmons, Matthew H. Law, Christopher SchmidtCathy Lanagan, Linda O'Connor, Elizabeth A. Holland, Helen Schmid, Judith A. Maskiell, Jodie Jetann, Megan Ferguson, Mark A. Jenkins, Richard F. Kefford, Graham G. Giles, Bruce K. Armstrong, Joanne F. Aitken, John L. Hopper, David C. Whiteman, Paul D. Pharoah, Douglas F. Easton, Alison M. Dunning, Julia A. Newton-Bishop, Grant W. Montgomery, Nicholas G. Martin, Graham J. Mann, D. Timothy Bishop, Hensin Tsao, Jeffrey M. Trent, David E. Fisher, Nicholas K. Hayward, Kevin M. Brown^*

^*Corresponding author for this work

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

402 Citations (Scopus)

Abstract

So far, two genes associated with familial melanoma have been identified, accounting for a minority of genetic risk in families. Mutations in CDKN2A account for approximately 40% of familial cases, and predisposing mutations in CDK4 have been reported in a very small number of melanoma kindreds. Here we report the whole-genome sequencing of probands from several melanoma families, which we performed in order to identify other genes associated with familial melanoma. We identify one individual carrying a novel germline variant (coding DNA sequence c.G1075A; protein sequence p.E318K; rs149617956) in the melanoma-lineage-specific oncogene microphthalmia-associated transcription factor (MITF). Although the variant co-segregated with melanoma in some but not all cases in the family, linkage analysis of 31 families subsequently identified to carry the variant generated a log of odds (lod) score of 2.7 under a dominant model, indicating E318K as a possible intermediate risk variant. Consistent with this, the E318K variant was significantly associated with melanoma in a large Australian case-control sample. Likewise, it was similarly associated in an independent case-control sample from the United Kingdom. In the Australian sample, the variant allele was significantly over-represented in cases with a family history of melanoma, multiple primary melanomas, or both. The variant allele was also associated with increased naevus count and non-blue eye colour. Functional analysis of E318K showed that MITF encoded by the variant allele had impaired sumoylation and differentially regulated several MITF targets. These data indicate that MITF is a melanoma-predisposition gene and highlight the utility of whole-genome sequencing to identify novel rare variants associated with disease susceptibility.

Original language	English
Pages (from-to)	99-103
Number of pages	5
Journal	Nature
Volume	480
Issue number	7375
DOIs	https://doi.org/10.1038/nature10630
Publication status	Published - 1 Dec 2011
Externally published	Yes

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Yokoyama, S., Woods, S. L., Boyle, G. M., Aoude, L. G., MacGregor, S., Zismann, V., Gartside, M., Cust, A. E., Haq, R., Harland, M., Taylor, J. C., Duffy, D. L., Holohan, K., Dutton-Regester, K., Palmer, J. M., Bonazzi, V., Stark, M. S., Symmons, J., Law, M. H., ... Brown, K. M. (2011). A novel recurrent mutation in MITF predisposes to familial and sporadic melanoma. Nature, 480(7375), 99-103. https://doi.org/10.1038/nature10630

@article{f44dbc017c474bf2822eae0ae1602c40,

title = "A novel recurrent mutation in MITF predisposes to familial and sporadic melanoma",

abstract = "So far, two genes associated with familial melanoma have been identified, accounting for a minority of genetic risk in families. Mutations in CDKN2A account for approximately 40\% of familial cases, and predisposing mutations in CDK4 have been reported in a very small number of melanoma kindreds. Here we report the whole-genome sequencing of probands from several melanoma families, which we performed in order to identify other genes associated with familial melanoma. We identify one individual carrying a novel germline variant (coding DNA sequence c.G1075A; protein sequence p.E318K; rs149617956) in the melanoma-lineage-specific oncogene microphthalmia-associated transcription factor (MITF). Although the variant co-segregated with melanoma in some but not all cases in the family, linkage analysis of 31 families subsequently identified to carry the variant generated a log of odds (lod) score of 2.7 under a dominant model, indicating E318K as a possible intermediate risk variant. Consistent with this, the E318K variant was significantly associated with melanoma in a large Australian case-control sample. Likewise, it was similarly associated in an independent case-control sample from the United Kingdom. In the Australian sample, the variant allele was significantly over-represented in cases with a family history of melanoma, multiple primary melanomas, or both. The variant allele was also associated with increased naevus count and non-blue eye colour. Functional analysis of E318K showed that MITF encoded by the variant allele had impaired sumoylation and differentially regulated several MITF targets. These data indicate that MITF is a melanoma-predisposition gene and highlight the utility of whole-genome sequencing to identify novel rare variants associated with disease susceptibility.",

author = "Satoru Yokoyama and Woods, \{Susan L.\} and Boyle, \{Glen M.\} and Aoude, \{Lauren G.\} and Stuart MacGregor and Victoria Zismann and Michael Gartside and Cust, \{Anne E.\} and Rizwan Haq and Mark Harland and Taylor, \{John C.\} and Duffy, \{David L.\} and Kelly Holohan and Ken Dutton-Regester and Palmer, \{Jane M.\} and Vanessa Bonazzi and Stark, \{Mitchell S.\} and Judith Symmons and Law, \{Matthew H.\} and Christopher Schmidt and Cathy Lanagan and Linda O'Connor and Holland, \{Elizabeth A.\} and Helen Schmid and Maskiell, \{Judith A.\} and Jodie Jetann and Megan Ferguson and Jenkins, \{Mark A.\} and Kefford, \{Richard F.\} and Giles, \{Graham G.\} and Armstrong, \{Bruce K.\} and Aitken, \{Joanne F.\} and Hopper, \{John L.\} and Whiteman, \{David C.\} and Pharoah, \{Paul D.\} and Easton, \{Douglas F.\} and Dunning, \{Alison M.\} and Newton-Bishop, \{Julia A.\} and Montgomery, \{Grant W.\} and Martin, \{Nicholas G.\} and Mann, \{Graham J.\} and Bishop, \{D. Timothy\} and Hensin Tsao and Trent, \{Jeffrey M.\} and Fisher, \{David E.\} and Hayward, \{Nicholas K.\} and Brown, \{Kevin M.\}",

year = "2011",

month = dec,

day = "1",

doi = "10.1038/nature10630",

language = "English",

volume = "480",

pages = "99--103",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Research",

number = "7375",

}

Yokoyama, S, Woods, SL, Boyle, GM, Aoude, LG, MacGregor, S, Zismann, V, Gartside, M, Cust, AE, Haq, R, Harland, M, Taylor, JC, Duffy, DL, Holohan, K, Dutton-Regester, K, Palmer, JM, Bonazzi, V, Stark, MS, Symmons, J, Law, MH, Schmidt, C, Lanagan, C, O'Connor, L, Holland, EA, Schmid, H, Maskiell, JA, Jetann, J, Ferguson, M, Jenkins, MA, Kefford, RF, Giles, GG, Armstrong, BK, Aitken, JF, Hopper, JL, Whiteman, DC, Pharoah, PD, Easton, DF, Dunning, AM, Newton-Bishop, JA, Montgomery, GW, Martin, NG, Mann, GJ, Bishop, DT, Tsao, H, Trent, JM, Fisher, DE, Hayward, NK & Brown, KM 2011, 'A novel recurrent mutation in MITF predisposes to familial and sporadic melanoma', Nature, vol. 480, no. 7375, pp. 99-103. https://doi.org/10.1038/nature10630

TY - JOUR

T1 - A novel recurrent mutation in MITF predisposes to familial and sporadic melanoma

AU - Yokoyama, Satoru

AU - Woods, Susan L.

AU - Boyle, Glen M.

AU - Aoude, Lauren G.

AU - MacGregor, Stuart

AU - Zismann, Victoria

AU - Gartside, Michael

AU - Cust, Anne E.

AU - Haq, Rizwan

AU - Harland, Mark

AU - Taylor, John C.

AU - Duffy, David L.

AU - Holohan, Kelly

AU - Dutton-Regester, Ken

AU - Palmer, Jane M.

AU - Bonazzi, Vanessa

AU - Stark, Mitchell S.

AU - Symmons, Judith

AU - Law, Matthew H.

AU - Schmidt, Christopher

AU - Lanagan, Cathy

AU - O'Connor, Linda

AU - Holland, Elizabeth A.

AU - Schmid, Helen

AU - Maskiell, Judith A.

AU - Jetann, Jodie

AU - Ferguson, Megan

AU - Jenkins, Mark A.

AU - Kefford, Richard F.

AU - Giles, Graham G.

AU - Armstrong, Bruce K.

AU - Aitken, Joanne F.

AU - Hopper, John L.

AU - Whiteman, David C.

AU - Pharoah, Paul D.

AU - Easton, Douglas F.

AU - Dunning, Alison M.

AU - Newton-Bishop, Julia A.

AU - Montgomery, Grant W.

AU - Martin, Nicholas G.

AU - Mann, Graham J.

AU - Bishop, D. Timothy

AU - Tsao, Hensin

AU - Trent, Jeffrey M.

AU - Fisher, David E.

AU - Hayward, Nicholas K.

AU - Brown, Kevin M.

PY - 2011/12/1

Y1 - 2011/12/1

N2 - So far, two genes associated with familial melanoma have been identified, accounting for a minority of genetic risk in families. Mutations in CDKN2A account for approximately 40% of familial cases, and predisposing mutations in CDK4 have been reported in a very small number of melanoma kindreds. Here we report the whole-genome sequencing of probands from several melanoma families, which we performed in order to identify other genes associated with familial melanoma. We identify one individual carrying a novel germline variant (coding DNA sequence c.G1075A; protein sequence p.E318K; rs149617956) in the melanoma-lineage-specific oncogene microphthalmia-associated transcription factor (MITF). Although the variant co-segregated with melanoma in some but not all cases in the family, linkage analysis of 31 families subsequently identified to carry the variant generated a log of odds (lod) score of 2.7 under a dominant model, indicating E318K as a possible intermediate risk variant. Consistent with this, the E318K variant was significantly associated with melanoma in a large Australian case-control sample. Likewise, it was similarly associated in an independent case-control sample from the United Kingdom. In the Australian sample, the variant allele was significantly over-represented in cases with a family history of melanoma, multiple primary melanomas, or both. The variant allele was also associated with increased naevus count and non-blue eye colour. Functional analysis of E318K showed that MITF encoded by the variant allele had impaired sumoylation and differentially regulated several MITF targets. These data indicate that MITF is a melanoma-predisposition gene and highlight the utility of whole-genome sequencing to identify novel rare variants associated with disease susceptibility.

AB - So far, two genes associated with familial melanoma have been identified, accounting for a minority of genetic risk in families. Mutations in CDKN2A account for approximately 40% of familial cases, and predisposing mutations in CDK4 have been reported in a very small number of melanoma kindreds. Here we report the whole-genome sequencing of probands from several melanoma families, which we performed in order to identify other genes associated with familial melanoma. We identify one individual carrying a novel germline variant (coding DNA sequence c.G1075A; protein sequence p.E318K; rs149617956) in the melanoma-lineage-specific oncogene microphthalmia-associated transcription factor (MITF). Although the variant co-segregated with melanoma in some but not all cases in the family, linkage analysis of 31 families subsequently identified to carry the variant generated a log of odds (lod) score of 2.7 under a dominant model, indicating E318K as a possible intermediate risk variant. Consistent with this, the E318K variant was significantly associated with melanoma in a large Australian case-control sample. Likewise, it was similarly associated in an independent case-control sample from the United Kingdom. In the Australian sample, the variant allele was significantly over-represented in cases with a family history of melanoma, multiple primary melanomas, or both. The variant allele was also associated with increased naevus count and non-blue eye colour. Functional analysis of E318K showed that MITF encoded by the variant allele had impaired sumoylation and differentially regulated several MITF targets. These data indicate that MITF is a melanoma-predisposition gene and highlight the utility of whole-genome sequencing to identify novel rare variants associated with disease susceptibility.

UR - https://www.scopus.com/pages/publications/82555187007

U2 - 10.1038/nature10630

DO - 10.1038/nature10630

M3 - Article

SN - 0028-0836

VL - 480

SP - 99

EP - 103

JO - Nature

JF - Nature

IS - 7375

ER -

A novel recurrent mutation in MITF predisposes to familial and sporadic melanoma

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