Improvement of Genetic Testing for Cutaneous Melanoma in Countries With Low to Moderate Incidence

Delaunay, J.; Martin, Ludovic; Paillerets, Brigitte Bressac-de; Duru, Gérard; Ingster, Olivier; Thomas, Luc

doi:10.1001/jamadermatol.2017.2926

Cited by 9 publications

(4 citation statements)

References 46 publications

(110 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…2019 . Patients with MPM were classified as either ‘first diagnosis at age ≤ 40 years’ or ‘first diagnosis at age > 40 years’, based on literature suggesting that younger patients with melanoma are more likely to harbour genetic mutations …”

Section: Methodsmentioning

confidence: 99%

The interplay of sun damage and genetic risk in Australian multiple and single primary melanoma cases and controls

et al. 2020

View full text Add to dashboard Cite

Summary Background Skin phenotype, host genotype and ultraviolet (UV) damage play a role in the development of melanoma. Objectives To ascertain whether the level of UV damage at the site of melanomas was associated with genetic polymorphisms. Methods Deep phenotyping was performed on 1244 individuals; 281 with multiple primary melanomas (MPMs), 304 with single primary melanoma (SPM) and 659 convenience controls. Genotype data was generated using the Illumina CoreExome microarray platform, assaying over 500 000 single‐nucleotide polymorphisms. A subset of variants were combined to assess a polygenic risk score (PRS) for melanoma. Results Most MPM cases were diagnosed in patients aged > 40 years, in sites with visible chronic UV damage. Women and those diagnosed at age ≤ 40 years were less likely to have perilesional UV damage. Patients with MPM had higher frequencies of MITF E318K, MC1R R‐alleles and the ASIP risk haplotype. Individuals who had melanoma in a visibly UV‐damaged site were more likely to carry MC1R rs75570604 [odds ratio (OR) 2·5], 9q31.2 rs10816595 (OR 1·4) and MTAP rs869329 (OR 1·4). These same alleles were more common in patients with MPM who were diagnosed at age ≤ 40 years. The mean PRS was significantly higher in MPM than in SPM and controls. Naevus count was comparable in early‐onset MPM cases and those diagnosed at age > 40 years. Conclusions Our cohort demonstrated higher frequencies of previously reported alleles associated with melanoma. MPM melanomas more commonly occur in UV‐damaged areas, and these individuals are more likely to carry MC1R red hair colour alleles. Awareness of the interplay of genetic vulnerability with UV damage can stratify risk and guide recommendations for melanoma screening. What's already known about this topic? Skin phenotype, host genotype and ultraviolet (UV) damage all play a role in melanoma development. One of the main risk factors is a personal history of melanoma; second and subsequent primary melanomas account for over 20% of all melanomas registered in Queensland. Multiple loci are associated with melanoma risk, including many low‐penetrance loci, which may have a cumulatively significant risk. Population‐wide screening programmes for melanoma are not yet economically viable. What does this study add? Patients diagnosed with melanoma at age ≤ 40 years were more likely than older patients to have melanomas in non‐UV‐damaged sites. Patients with multiple melanomas had higher frequencies of MITF E318K, MC1R R‐alleles, and the ASIP extended risk haplotype than patients with single melanoma. CDKN2A, MC1R and MTAP variants were more frequent in patients who developed melanomas at a younger age, but also in those whose melanomas were all on visibly UV‐damaged sites. What is the translational message? Incorporating these genetic findings into the known risk factors of skin phenotype and visible UV damage may allow for a more customized and economically feasible approach to early detection of melanoma, particularly in younger patients. Plain la...

show abstract

Section: Methodsmentioning

confidence: 99%

The interplay of sun damage and genetic risk in Australian multiple and single primary melanoma cases and controls

et al. 2020

View full text Add to dashboard Cite

show abstract

“…Current guidelines for genetic testing in melanoma are restricted to CDK2NA screening and employ the rule of twos, threes, and fours ( Delaunay et al., 2017 ). According to this rule, genetic testing is indicated for subjects with ≥2, ≥3, or ≥4 primary melanomas or genetically related cancers depending on the general population incidence.…”

Section: Future Perspectivesmentioning

confidence: 99%

New Insights into Melanoma Tumor Syndromes

Rashid¹,

Gupta²,

McCormick³

2022

JID Innovations

View full text Add to dashboard Cite

“…Notably, rs17119461 and rs17119490 were found to be nominally associated with pancreatic cancer, which shares genetic risk with familial melanoma (Wu et al, 2014). Some melanoma genetic testing panels for patients meeting specific criteria include intermediate risk variants, such as MITF c.952 G>A that have a low minor allele frequency (w0.0015) (Delaunay et al, 2017). Thus, if validated in additional studies, rs17119461 may be a potential candidate for genetic testing in populations at high risk for melanoma.…”

Section: Relationship Of Chromosome Arm 10q Variants To Occurrence Ofmentioning

confidence: 99%

Relationship of Chromosome Arm 10q Variants to Occurrence of Multiple Primary Melanoma in the Population-Based Genes, Environment, and Melanoma (GEM) Study

Miles

Orlow

Kanetsky

et al. 2019

Journal of Investigative Dermatology

View full text Add to dashboard Cite

previously reported that touch-evoked scratching was elicited only by stimulation at the skin adjacent to a site of acute itch or the border of the dry skintreated area on the rostral back (Akiyama et al., 2012; Iwanaga et al., 2018). Therefore, it appears that, although Ab-fibers innervating the chemical-injected site or the skin within the treatment area drive a circuit for antimechanical itch, a subset of LTMRs innervating the adjacent skin mediates touch-evoked itch. In summary, we show that alloknesis in an IMQ-induced psoriatic mouse model is associated with a loss of the epidermal nerve endings of Ab-fibers but not Merkel cells. By contrast, alloknesis in dry skin and aged skin is associated with a loss of Merkel cells (Feng et al., 2018). Considering that the Merkel cells are innervated by Ab-fibers, the loss of sustained discharge of Ab-fibers from Merkel cells is essential for alloknesis. Ab-fibers in hairy skin likely innervate neuropeptide Y-positive inhibitory interneurons in the spinal cord to gate mechanical itch in normal conditions (Bourane et al., 2015). Our findings suggest that reactivation of Ab-fibers can reduce alloknesis under chronic itch condition. High-frequency transcutaneous electrical nerve stimulation activates Ab-fibers and temporarily relives generalized itch (Wallengren, 2004). Additionally, massage therapy works for certain types of itch (Gü rol et al., 2010; Schachner et al., 1998). Although antipruritic effects of those therapies are expected to be temporary, the approach to regain Ab-fibers could be considered as a novel strategy for treating chronic itch.

show abstract

Improvement of Genetic Testing for Cutaneous Melanoma in Countries With Low to Moderate Incidence

Cited by 9 publications

References 46 publications

The interplay of sun damage and genetic risk in Australian multiple and single primary melanoma cases and controls

The interplay of sun damage and genetic risk in Australian multiple and single primary melanoma cases and controls

New Insights into Melanoma Tumor Syndromes

Relationship of Chromosome Arm 10q Variants to Occurrence of Multiple Primary Melanoma in the Population-Based Genes, Environment, and Melanoma (GEM) Study

Contact Info

Product

Resources

About