Inherited Genetic Variants Associated with Melanoma BRAF/NRAS Subtypes

Thomas, Nancy E.; Edmiston, Sharon N.; Orlow, Irene; Kanetsky, Peter A.; Luo, Li; Gibbs, David C.; Parrish, Eloise; Hao, Honglin; Busam, Klaus J.; Armstrong, Bruce K.; Kricker, Anne; Cust, Anne E.; Anton‐Culver, Hoda; Gruber, Stephen B.; Gallagher, Richard P.; Zanetti, Roberto; Rosso, Stefano; Sacchetto, Lidia; Dwyer, Terence; Ollila, David W.; Begg, Colin B.; Berwick, Marianne; Conway, Kathleen

doi:10.1016/j.jid.2018.04.025

Cited by 12 publications

(9 citation statements)

References 52 publications

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“…Evidence suggests that histological factors may affect tumour aggressiveness and patient prognosis in melanoma and KCs . One study, for example, found that two SNVs in IRF4 and PLA2G6 were associated with BRAF / NRAS melanoma subtypes . However, PRS studies to date have combined histological subtypes together, which could lead to confounding.…”

Section: Discussionmentioning

confidence: 99%

Genome‐wide association studies and polygenic risk scores for skin cancer: clinically useful yet?

Roberts

Asgari

Toland³

2019

Br J Dermatol

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Summary Background Genome‐wide association studies (GWAS) have identified thousands of susceptibility variants, although most have been associated with small individual risk estimates that offer little predictive value. However, combining multiple variants into polygenic risk scores (PRS) may be more informative. Multiple studies have developed PRS composed of GWAS‐identified variants for cutaneous cancers. This review highlights data from these studies. Objectives To review published GWAS and PRS studies for melanoma, cutaneous squamous cell carcinoma (cSCC) and basal cell carcinoma (BCC), and discuss their potential clinical utility. Methods We searched PubMed and the National Human Genome Research Institute–European Bioinformatics Institute GWAS catalogue to identify relevant studies. Results Results from 21 GWAS (11 melanoma, 3 cSCC, 7 BCC) and 11 PRS studies are summarized. Six loci in pigmentation genes overlap between these three cancers (ASIP/RALY, IRF4, MC1R, OCA2, SLC45A2 and TYR). Additional loci overlap for cSCC/BCC and BCC/melanoma, but no other loci are shared between cSCC and melanoma. PRS for melanoma show roughly two‐to‐threefold increases in risk and modest improvements in risk prediction (2–7% increases). PRS are associated with twofold and threefold increases in risk of cSCC and BCC, respectively, with small improvements (2% increase) in predictive ability. Conclusions Existing data indicate that PRS may offer small, but potentially meaningful, improvements to risk prediction. Additional research is needed to clarify the potential utility of PRS in cutaneous carcinomas. Clinical translation will require well‐powered validation studies incorporating known risk factors to evaluate PRS as tools for screening. What's already known about this topic? Over 50 susceptibility loci for melanoma, basal cell carcinoma (BCC) and cutaneous squamous cell carcinoma (cSCC) have been identified in genome‐wide association studies (GWAS). Polygenic risk scores (PRS) using variants identified from GWAS have also been developed for melanoma, BCC and cSCC, and investigated with respect to clinical risk prediction. What does this study add? This review provides an overview of GWAS findings and the potential clinical utility of PRS for melanoma, BCC and cSCC.

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Section: Discussionmentioning

confidence: 99%

Genome‐wide association studies and polygenic risk scores for skin cancer: clinically useful yet?

Roberts

Asgari

Toland³

2019

Br J Dermatol

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“…Cutaneous melanomas are categorized byfourgenomicsubtypes: mutant BRAF, mutant RAS(mainly NRAS), mutant NF1, and triple-wild-type. In one study, germline DNAfrom 1,223 participantswas genotyped for 47 SNVs previously associated with melanoma risk [53]. Melanomas were also interrogated for BRAFand NRASmutations.…”

Section: Germline Variant By Somatic Mutation (Gxm) Associationin Transmentioning

confidence: 99%

“…The rs12203592(T)alleleof IRF4was associated with decreased risk of BRAF V600E and BRAF V600K mutations, but an increased likelihood ofother BRAFexon 15 mutations (Table 2). The rs132985(T) allele of PLA2G6was associated with increased likelihood of BRAF V600E and other BRAFexon 15 mutations(Table 2) [53] Germline MC1Rvariantsalso influence the somaticmutational landscape of melanoma. These variants are associated with red hair, freckling, and sun sensitivity.…”

Section: Germline Variant By Somatic Mutation (Gxm) Associationin Transmentioning

confidence: 99%

Germline Variants Impact Somatic Events during Tumorigenesis

2019

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Cancer is characterized by diverse genetic alterations in both germline and somatic genomes that disrupt normal biology and providea selective advantage to cells during tumorigenesis. Germline and somatic genomes have been extensively studied independently, leading to numerous biological insights. Analyses integrating data from both genomes have identified genetic variants impacting somatic events in tumors, including hotspot driver mutations. Interactions among specific germline variants and somatic eventsinfluence cancer subtypes, treatment response, and clinical outcomes. Investigation of these complex interactions is increasing our understanding of aberrant pathwaysin tumorsthat may uncover novel therapeutic targets. Here, we review the literature describing the role germline genetic variantsplay in promoting selection of and generation of specific mutations during tumorigenesis.

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“…Около 25% всех злокачественных опухолей имеют нарушения регуляции сигнального каскада MAPK, связанные с увеличением продукции активирующих лигандов, а также наличием активирующих мутаций в генах семейств RTKs, RAS и RAF [3]. При меланоме кожи нарушения в MAPK сигнальном каскаде связаны, как правило, с активирующей мутацией в гене BRAF в 50% случаев или с мутацией в гене NRAS в 15% случаев [4]. Данный факт демонстрирует важность контроля регуляции MAPK в гомеостазе меланоцитов.…”

Section: Introductionunclassified

The combination of mutations in BRAF and NRAS genes within a one tumor in patients with cutaneous melanoma

2019

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The paper provides a clinical description and analysis of two melanoma cases with mutations in the BRAF and NRAS gene within one tumor. Until recently, it was believed that mutations in the BRAF and NRAS genes are exclusive and do not occur within the same tumor. Later it was revealed that these mutations can exist within one tumor, but this is still quite a rare phenomenon. Molecular genetic analysis of the tumor obtained from both patients showed a mutation in the 15 exon of the BRAF gene c.1799T>A (V600E) and exon 2 of the NRAS p.G13S gene (p.37 G>A). The expression level of non-mutant NRAS protein was different in both cases. In conclusion, so in one patient, despite the presence of a mutation in the NRAS gene, the level of expression of the non-mutant protein was absent, which can be related to possible posttranscriptional disorders in the regulation of gene expression.

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Inherited Genetic Variants Associated with Melanoma BRAF/NRAS Subtypes

Cited by 12 publications

References 52 publications

Genome‐wide association studies and polygenic risk scores for skin cancer: clinically useful yet?

Genome‐wide association studies and polygenic risk scores for skin cancer: clinically useful yet?

Germline Variants Impact Somatic Events during Tumorigenesis

The combination of mutations in BRAF and NRAS genes within a one tumor in patients with cutaneous melanoma

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