MC1R variants in childhood and adolescent melanoma: a retrospective pooled analysis of a multicentre cohort

IMI Study Group; GEM Study Group; M-SKIP Study Group

doi:10.1016/S2352-4642(19)30005-7

MC1R variants in childhood and adolescent melanoma: a retrospective pooled analysis of a multicentre cohort

IMI Study Group, GEM Study Group, M-SKIP Study Group

Cancer Center

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

12 Scopus citations

Abstract

Background: Germline variants in the melanocortin 1 receptor gene (MC1R) might increase the risk of childhood and adolescent melanoma, but a clear conclusion is challenging because of the low number of studies and cases. We assessed the association of MC1R variants with childhood and adolescent melanoma in a large study comparing the prevalence of MC1R variants in child or adolescent patients with melanoma to that in adult patients with melanoma and in healthy adult controls. Methods: In this retrospective pooled analysis, we used the M-SKIP Project, the Italian Melanoma Intergroup, and other European groups (with participants from Australia, Canada, France, Greece, Italy, the Netherlands, Serbia, Spain, Sweden, Turkey, and the USA) to assemble an international multicentre cohort. We gathered phenotypic and genetic data from children or adolescents diagnosed with sporadic single-primary cutaneous melanoma at age 20 years or younger, adult patients with sporadic single-primary cutaneous melanoma diagnosed at age 35 years or older, and healthy adult individuals as controls. We calculated odds ratios (ORs) for childhood and adolescent melanoma associated with MC1R variants by multivariable logistic regression. Subgroup analysis was done for children aged 18 or younger and 14 years or younger. Findings: We analysed data from 233 young patients, 932 adult patients, and 932 healthy adult controls. Children and adolescents had higher odds of carrying MC1R r variants than did adult patients (OR 1·54, 95% CI 1·02–2·33), including when analysis was restricted to patients aged 18 years or younger (1·80, 1·06–3·07). All investigated variants, except Arg160Trp, tended, to varying degrees, to have higher frequencies in young patients than in adult patients, with significantly higher frequencies found for Val60Leu (OR 1·60, 95% CI 1·05–2·44; p=0·04) and Asp294His (2·15, 1·05–4·40; p=0·04). Compared with those of healthy controls, young patients with melanoma had significantly higher frequencies of any MC1R variants. Interpretation: Our pooled analysis of MC1R genetic data of young patients with melanoma showed that MC1R r variants were more prevalent in childhood and adolescent melanoma than in adult melanoma, especially in patients aged 18 years or younger. Our findings support the role of MC1R in childhood and adolescent melanoma susceptibility, with a potential clinical relevance for developing early melanoma detection and preventive strategies. Funding: SPD-Pilot/Project-Award-2015; AIRC-MFAG-11831.

Original language	English (US)
Pages (from-to)	332-342
Number of pages	11
Journal	The Lancet Child and Adolescent Health
Volume	3
Issue number	5
DOIs	https://doi.org/10.1016/S2352-4642(19)30005-7
State	Published - May 2019

ASJC Scopus subject areas

Pediatrics, Perinatology, and Child Health
Developmental and Educational Psychology

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10.1016/S2352-4642(19)30005-7

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@article{f79bd37925c34060b7679c7c67d1615d,

title = "MC1R variants in childhood and adolescent melanoma: a retrospective pooled analysis of a multicentre cohort",

abstract = "Background: Germline variants in the melanocortin 1 receptor gene (MC1R) might increase the risk of childhood and adolescent melanoma, but a clear conclusion is challenging because of the low number of studies and cases. We assessed the association of MC1R variants with childhood and adolescent melanoma in a large study comparing the prevalence of MC1R variants in child or adolescent patients with melanoma to that in adult patients with melanoma and in healthy adult controls. Methods: In this retrospective pooled analysis, we used the M-SKIP Project, the Italian Melanoma Intergroup, and other European groups (with participants from Australia, Canada, France, Greece, Italy, the Netherlands, Serbia, Spain, Sweden, Turkey, and the USA) to assemble an international multicentre cohort. We gathered phenotypic and genetic data from children or adolescents diagnosed with sporadic single-primary cutaneous melanoma at age 20 years or younger, adult patients with sporadic single-primary cutaneous melanoma diagnosed at age 35 years or older, and healthy adult individuals as controls. We calculated odds ratios (ORs) for childhood and adolescent melanoma associated with MC1R variants by multivariable logistic regression. Subgroup analysis was done for children aged 18 or younger and 14 years or younger. Findings: We analysed data from 233 young patients, 932 adult patients, and 932 healthy adult controls. Children and adolescents had higher odds of carrying MC1R r variants than did adult patients (OR 1·54, 95% CI 1·02–2·33), including when analysis was restricted to patients aged 18 years or younger (1·80, 1·06–3·07). All investigated variants, except Arg160Trp, tended, to varying degrees, to have higher frequencies in young patients than in adult patients, with significantly higher frequencies found for Val60Leu (OR 1·60, 95% CI 1·05–2·44; p=0·04) and Asp294His (2·15, 1·05–4·40; p=0·04). Compared with those of healthy controls, young patients with melanoma had significantly higher frequencies of any MC1R variants. Interpretation: Our pooled analysis of MC1R genetic data of young patients with melanoma showed that MC1R r variants were more prevalent in childhood and adolescent melanoma than in adult melanoma, especially in patients aged 18 years or younger. Our findings support the role of MC1R in childhood and adolescent melanoma susceptibility, with a potential clinical relevance for developing early melanoma detection and preventive strategies. Funding: SPD-Pilot/Project-Award-2015; AIRC-MFAG-11831.",

author = "{IMI Study Group} and {GEM Study Group} and {M-SKIP Study Group} and Cristina Pellegrini and Francesca Botta and Daniela Massi and Claudia Martorelli and Fabio Facchetti and Sara Gandini and Patrick Maisonneuve and Avril, {Marie Fran{\c c}oise} and Florence Demenais and {Bressac-de Paillerets}, Brigitte and Veronica Hoiom and Cust, {Anne E.} and Hoda Anton-Culver and Gruber, {Stephen B.} and Gallagher, {Richard P.} and Loraine Marrett and Roberto Zanetti and Terence Dwyer and Thomas, {Nancy E.} and Begg, {Colin B.} and Marianne Berwick and Susana Puig and Miriam Potrony and Eduardo Nagore and Paola Ghiorzo and Chiara Menin and Manganoni, {Ausilia Maria} and Monica Rodolfo and Sonia Brugnara and Emanuela Passoni and Sekulovic, {Lidija Kandolf} and Federica Baldini and Gabriella Guida and Alexandros Stratigos and Fezal Ozdemir and Fabrizio Ayala and Ricardo Fernandez-de-Misa and Pietro Quaglino and Gloria Ribas and Antonella Romanini and Emilia Migliano and Ignazio Stanganelli and Kanetsky, {Peter A.} and Pizzichetta, {Maria Antonietta} and Garc{\'i}a-Borr{\'o}n, {Jose Carlos} and Hongmei Nan and Landi, {Maria Teresa} and Julian Little and Julia Newton-Bishop and Joanne Jeter",

note = "Funding Information: We have received funding for this study from the Society for Pediatric Dermatology (SPD Pilot Project Award 2015 ) and Italian Association for Research on Cancer (AIRC MFAG 11831). PAK has received grants for the Melanoma Susceptibility Study from the National Cancer Institute ( CA75434 , CA80700 , CA092428 ). PG has received funding for the Genoa study from the Italian Association for Research on Cancer ( AIRC IG 15460 ). JL holds a tier 1 Canada Research Chair. The study in the Melanoma Unit, Hospital Cl{\'i}nic (Barcelona, Spain) was supported in part by grants from Fondo de Investigaciones Sanitarias (PI 12/00840, PI15/00956, and PI15/00716) and the CIBER de Enfermedades Raras of the Instituto de Salud Carlos III (Madrid, Spain); was co-funded by EU European Regional Development Funds and by the AGAUR 2014_SGR_603 and 2017_SGR_1134 of the Catalan Government (Spain); and was funded by a grant from Fundaci{\'o} La Marat{\'o} de TV3 (201331–30; Catalonia, Spain), by the European Commission under the 6th Framework Programme (LSHC-CT-2006–018702; GenoMEL), by the CERCA Programme–Generalitat de Catalunya, and by a research grant from the Fundaci{\'o}n Cient{\'i}fica de la Asociaci{\'o}n Espa{\~n}ola Contra el C{\'a}ncer, Spain (GCB15152978SOEN). Part of the work was developed at the building Centro Esther Koplowitz, Barcelona (Spain). M-FA, FD, and BB-dP have received funding from the Hospital Programme for Clinical Research (France, PHRC 2007 AOM 07–195NI 07004). We thank the medical doctors who included some of the patients of this study. We wish to acknowledge the work of Gustave Roussy Biobank (BB-0033–00074) in providing DNA resources. Publisher Copyright: {\textcopyright} 2019 Elsevier Ltd",

year = "2019",

month = may,

doi = "10.1016/S2352-4642(19)30005-7",

language = "English (US)",

volume = "3",

pages = "332--342",

journal = "The Lancet Child and Adolescent Health",

issn = "2352-4642",

publisher = "Elsevier BV",

number = "5",

}

TY - JOUR

T1 - MC1R variants in childhood and adolescent melanoma

T2 - a retrospective pooled analysis of a multicentre cohort

AU - IMI Study Group

AU - GEM Study Group

AU - M-SKIP Study Group

AU - Pellegrini, Cristina

AU - Botta, Francesca

AU - Massi, Daniela

AU - Martorelli, Claudia

AU - Facchetti, Fabio

AU - Gandini, Sara

AU - Maisonneuve, Patrick

AU - Avril, Marie Françoise

AU - Demenais, Florence

AU - Bressac-de Paillerets, Brigitte

AU - Hoiom, Veronica

AU - Cust, Anne E.

AU - Anton-Culver, Hoda

AU - Gruber, Stephen B.

AU - Gallagher, Richard P.

AU - Marrett, Loraine

AU - Zanetti, Roberto

AU - Dwyer, Terence

AU - Thomas, Nancy E.

AU - Begg, Colin B.

AU - Berwick, Marianne

AU - Puig, Susana

AU - Potrony, Miriam

AU - Nagore, Eduardo

AU - Ghiorzo, Paola

AU - Menin, Chiara

AU - Manganoni, Ausilia Maria

AU - Rodolfo, Monica

AU - Brugnara, Sonia

AU - Passoni, Emanuela

AU - Sekulovic, Lidija Kandolf

AU - Baldini, Federica

AU - Guida, Gabriella

AU - Stratigos, Alexandros

AU - Ozdemir, Fezal

AU - Ayala, Fabrizio

AU - Fernandez-de-Misa, Ricardo

AU - Quaglino, Pietro

AU - Ribas, Gloria

AU - Romanini, Antonella

AU - Migliano, Emilia

AU - Stanganelli, Ignazio

AU - Kanetsky, Peter A.

AU - Pizzichetta, Maria Antonietta

AU - García-Borrón, Jose Carlos

AU - Nan, Hongmei

AU - Landi, Maria Teresa

AU - Little, Julian

AU - Newton-Bishop, Julia

AU - Jeter, Joanne

N1 - Funding Information: We have received funding for this study from the Society for Pediatric Dermatology (SPD Pilot Project Award 2015 ) and Italian Association for Research on Cancer (AIRC MFAG 11831). PAK has received grants for the Melanoma Susceptibility Study from the National Cancer Institute ( CA75434 , CA80700 , CA092428 ). PG has received funding for the Genoa study from the Italian Association for Research on Cancer ( AIRC IG 15460 ). JL holds a tier 1 Canada Research Chair. The study in the Melanoma Unit, Hospital Clínic (Barcelona, Spain) was supported in part by grants from Fondo de Investigaciones Sanitarias (PI 12/00840, PI15/00956, and PI15/00716) and the CIBER de Enfermedades Raras of the Instituto de Salud Carlos III (Madrid, Spain); was co-funded by EU European Regional Development Funds and by the AGAUR 2014_SGR_603 and 2017_SGR_1134 of the Catalan Government (Spain); and was funded by a grant from Fundació La Marató de TV3 (201331–30; Catalonia, Spain), by the European Commission under the 6th Framework Programme (LSHC-CT-2006–018702; GenoMEL), by the CERCA Programme–Generalitat de Catalunya, and by a research grant from the Fundación Científica de la Asociación Española Contra el Cáncer, Spain (GCB15152978SOEN). Part of the work was developed at the building Centro Esther Koplowitz, Barcelona (Spain). M-FA, FD, and BB-dP have received funding from the Hospital Programme for Clinical Research (France, PHRC 2007 AOM 07–195NI 07004). We thank the medical doctors who included some of the patients of this study. We wish to acknowledge the work of Gustave Roussy Biobank (BB-0033–00074) in providing DNA resources. Publisher Copyright: © 2019 Elsevier Ltd

PY - 2019/5

Y1 - 2019/5

N2 - Background: Germline variants in the melanocortin 1 receptor gene (MC1R) might increase the risk of childhood and adolescent melanoma, but a clear conclusion is challenging because of the low number of studies and cases. We assessed the association of MC1R variants with childhood and adolescent melanoma in a large study comparing the prevalence of MC1R variants in child or adolescent patients with melanoma to that in adult patients with melanoma and in healthy adult controls. Methods: In this retrospective pooled analysis, we used the M-SKIP Project, the Italian Melanoma Intergroup, and other European groups (with participants from Australia, Canada, France, Greece, Italy, the Netherlands, Serbia, Spain, Sweden, Turkey, and the USA) to assemble an international multicentre cohort. We gathered phenotypic and genetic data from children or adolescents diagnosed with sporadic single-primary cutaneous melanoma at age 20 years or younger, adult patients with sporadic single-primary cutaneous melanoma diagnosed at age 35 years or older, and healthy adult individuals as controls. We calculated odds ratios (ORs) for childhood and adolescent melanoma associated with MC1R variants by multivariable logistic regression. Subgroup analysis was done for children aged 18 or younger and 14 years or younger. Findings: We analysed data from 233 young patients, 932 adult patients, and 932 healthy adult controls. Children and adolescents had higher odds of carrying MC1R r variants than did adult patients (OR 1·54, 95% CI 1·02–2·33), including when analysis was restricted to patients aged 18 years or younger (1·80, 1·06–3·07). All investigated variants, except Arg160Trp, tended, to varying degrees, to have higher frequencies in young patients than in adult patients, with significantly higher frequencies found for Val60Leu (OR 1·60, 95% CI 1·05–2·44; p=0·04) and Asp294His (2·15, 1·05–4·40; p=0·04). Compared with those of healthy controls, young patients with melanoma had significantly higher frequencies of any MC1R variants. Interpretation: Our pooled analysis of MC1R genetic data of young patients with melanoma showed that MC1R r variants were more prevalent in childhood and adolescent melanoma than in adult melanoma, especially in patients aged 18 years or younger. Our findings support the role of MC1R in childhood and adolescent melanoma susceptibility, with a potential clinical relevance for developing early melanoma detection and preventive strategies. Funding: SPD-Pilot/Project-Award-2015; AIRC-MFAG-11831.

AB - Background: Germline variants in the melanocortin 1 receptor gene (MC1R) might increase the risk of childhood and adolescent melanoma, but a clear conclusion is challenging because of the low number of studies and cases. We assessed the association of MC1R variants with childhood and adolescent melanoma in a large study comparing the prevalence of MC1R variants in child or adolescent patients with melanoma to that in adult patients with melanoma and in healthy adult controls. Methods: In this retrospective pooled analysis, we used the M-SKIP Project, the Italian Melanoma Intergroup, and other European groups (with participants from Australia, Canada, France, Greece, Italy, the Netherlands, Serbia, Spain, Sweden, Turkey, and the USA) to assemble an international multicentre cohort. We gathered phenotypic and genetic data from children or adolescents diagnosed with sporadic single-primary cutaneous melanoma at age 20 years or younger, adult patients with sporadic single-primary cutaneous melanoma diagnosed at age 35 years or older, and healthy adult individuals as controls. We calculated odds ratios (ORs) for childhood and adolescent melanoma associated with MC1R variants by multivariable logistic regression. Subgroup analysis was done for children aged 18 or younger and 14 years or younger. Findings: We analysed data from 233 young patients, 932 adult patients, and 932 healthy adult controls. Children and adolescents had higher odds of carrying MC1R r variants than did adult patients (OR 1·54, 95% CI 1·02–2·33), including when analysis was restricted to patients aged 18 years or younger (1·80, 1·06–3·07). All investigated variants, except Arg160Trp, tended, to varying degrees, to have higher frequencies in young patients than in adult patients, with significantly higher frequencies found for Val60Leu (OR 1·60, 95% CI 1·05–2·44; p=0·04) and Asp294His (2·15, 1·05–4·40; p=0·04). Compared with those of healthy controls, young patients with melanoma had significantly higher frequencies of any MC1R variants. Interpretation: Our pooled analysis of MC1R genetic data of young patients with melanoma showed that MC1R r variants were more prevalent in childhood and adolescent melanoma than in adult melanoma, especially in patients aged 18 years or younger. Our findings support the role of MC1R in childhood and adolescent melanoma susceptibility, with a potential clinical relevance for developing early melanoma detection and preventive strategies. Funding: SPD-Pilot/Project-Award-2015; AIRC-MFAG-11831.

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U2 - 10.1016/S2352-4642(19)30005-7

DO - 10.1016/S2352-4642(19)30005-7

M3 - Article

C2 - 30872112

AN - SCOPUS:85064007564

SN - 2352-4642

VL - 3

SP - 332

EP - 342

JO - The Lancet Child and Adolescent Health

JF - The Lancet Child and Adolescent Health

IS - 5

ER -

MC1R variants in childhood and adolescent melanoma: a retrospective pooled analysis of a multicentre cohort

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