Meta-Analysis and Systematic Review of the Genomics of Mucosal Melanoma

Broit, Natasa; Johansson, Peter; Rodgers, Chloe B.; Walpole, Sebastian; Newell, Felicity; Hayward, Nicholas K.; Pritchard, Antonia L.

doi:10.1158/1541-7786.mcr-20-0839

Cited by 25 publications

(40 citation statements)

References 158 publications

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“…It has been reported that silencing of PTEN cooperates with activated AKT to promote metastasis of melanoma ( 102 , 103 , 106 , 107 ), but MM does not show a weaker performance in metastasis than CM in the clinic possibly because there are other gene alterations in the PI3K pathway promoting invasiveness of tumor ( 108 ). In a cohort of 91 MM patients, 18% of cases show TSC1 loss-of-function mutations which plays a suppressive role in cellular proliferation initiated by mTOR ( 109 ) and a similar result also showed in a recently published meta-analysis review of MM ( 105 ). Due to the limited sample size, the alteration levels for TSC need to be further verified.…”

Section: Mutations and Signaling Pathway Dependency In MMsupporting

confidence: 68%

“…Compared with 12% of PTEN loss in CM where deletions and mutations both account for the changes ( 17 , 79 ), PTEN is deeply deleted in merely 6.0% of MM cases and has hardly any mutations ( 16 ) Furthermore, there is rare co-occurrence of deleted PTEN and amplified KIT that possibly implies that loss of PTEN or gain of KIT are redundant for the activation of the PI3K pathway in MM. This is also supported by the fact that besides KIT and PTEN , mutations in PI3K and AKT homologous of PI3K-AKT-mTOR are scarce (4.8% PIK3CA , 3.8% PIK3CG , and 4.8% AKT3 ) ( 105 ). It has been reported that silencing of PTEN cooperates with activated AKT to promote metastasis of melanoma ( 102 , 103 , 106 , 107 ), but MM does not show a weaker performance in metastasis than CM in the clinic possibly because there are other gene alterations in the PI3K pathway promoting invasiveness of tumor ( 108 ).…”

Section: Mutations and Signaling Pathway Dependency In MMmentioning

confidence: 86%

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Mucosal Melanoma: Pathological Evolution, Pathway Dependency and Targeted Therapy

Xia

et al. 2021

Front. Oncol.

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Mucosal melanoma (MM) is a rare melanoma subtype that originates from melanocytes within sun-protected mucous membranes. Compared with cutaneous melanoma (CM), MM has worse prognosis and lacks effective treatment options. Moreover, the endogenous or exogenous risk factors that influence mucosal melanocyte transformation, as well as the identity of MM precursor lesions, are ambiguous. Consequently, there remains a lack of molecular markers that can be used for early diagnosis, and therefore better management, of MM. In this review, we first summarize the main functions of mucosal melanocytes. Then, using oral mucosal melanoma (OMM) as a model, we discuss the distinct pathologic stages from benign mucosal melanocytes to metastatic MM, mapping the possible evolutionary trajectories that correspond to MM initiation and progression. We highlight key areas of ambiguity during the genetic evolution of MM from its benign lesions, and the resolution of which could aid in the discovery of new biomarkers for MM detection and diagnosis. We outline the key pathways that are altered in MM, including the MAPK pathway, the PI3K/AKT pathway, cell cycle regulation, telomere maintenance, and the RNA maturation process, and discuss targeted therapy strategies for MM currently in use or under investigation.

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Section: Mutations and Signaling Pathway Dependency In MMsupporting

confidence: 68%

Section: Mutations and Signaling Pathway Dependency In MMmentioning

confidence: 86%

Mucosal Melanoma: Pathological Evolution, Pathway Dependency and Targeted Therapy

Xia

et al. 2021

Front. Oncol.

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“…A limitation could be insufficient power to detect associations of SNPs with lower minor allele frequencies (e.g., SLC45A2 rs16891982, MAF 0.017). Another limitation is that our study only included participants with cutaneous melanoma, not mucosal [ 76 , 77 ] or uveal melanomas [ 78 , 79 , 80 ], which seemingly have different genetic landscapes.…”

Section: Discussionmentioning

confidence: 99%

Association of Melanoma-Risk Variants with Primary Melanoma Tumor Prognostic Characteristics and Melanoma-Specific Survival in the GEM Study

et al. 2021

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Genome-wide association studies (GWAS) and candidate pathway studies have identified low-penetrant genetic variants associated with cutaneous melanoma. We investigated the association of melanoma-risk variants with primary melanoma tumor prognostic characteristics and melanoma-specific survival. The Genes, Environment, and Melanoma Study enrolled 3285 European origin participants with incident invasive primary melanoma. For each of 47 melanoma-risk single nucleotide polymorphisms (SNPs), we used linear and logistic regression modeling to estimate, respectively, the per allele mean changes in log of Breslow thickness and odds ratios for presence of ulceration, mitoses, and tumor-infiltrating lymphocytes (TILs). We also used Cox proportional hazards regression modeling to estimate the per allele hazard ratios for melanoma-specific survival. Passing the false discovery threshold (p = 0.0026) were associations of IRF4 rs12203592 and CCND1 rs1485993 with log of Breslow thickness, and association of TERT rs2242652 with presence of mitoses. IRF4 rs12203592 also had nominal associations (p < 0.05) with presence of mitoses and melanoma-specific survival, as well as a borderline association (p = 0.07) with ulceration. CCND1 rs1485993 also had a borderline association with presence of mitoses (p = 0.06). MX2 rs45430 had nominal associations with log of Breslow thickness, presence of mitoses, and melanoma-specific survival. Our study indicates that further research investigating the associations of these genetic variants with underlying biologic pathways related to tumor progression is warranted.

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“…The prevalence of the amplification of CCND1 is controversial [28,29] and the frequency differs among melanoma types, with an established higher detection rate in acral melanoma [30][31][32]. Gene copy numbers and amplification levels are frequently associated with the expression of cyclin D, but, in contrast, the overexpression of the cyclin D does not necessarily follow gene expression alterations, suggesting the influx of other pathways [29].…”

Section: Cdk4/6 Pathway Dysregulation In Melanomamentioning

confidence: 99%

CDK4/6 Inhibitors in Melanoma: A Comprehensive Review

Garutti

Targato

Buriolla

et al. 2021

Cells

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Historically, metastatic melanoma was considered a highly lethal disease. However, recent advances in drug development have allowed a significative improvement in prognosis. In particular, BRAF/MEK inhibitors and anti-PD1 antibodies have completely revolutionized the management of this disease. Nonetheless, not all patients derive a benefit or a durable benefit from these therapies. To overtake this challenges, new clinically active compounds are being tested in the context of clinical trials. CDK4/6 inhibitors are drugs already available in clinical practice and preliminary evidence showed a promising activity also in melanoma. Herein we review the available literature to depict a comprehensive landscape about CDK4/6 inhibitors in melanoma. We present the molecular and genetic background that might justify the usage of these drugs, the preclinical evidence, the clinical available data, and the most promising ongoing clinical trials.

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Meta-Analysis and Systematic Review of the Genomics of Mucosal Melanoma

Cited by 25 publications

References 158 publications

Mucosal Melanoma: Pathological Evolution, Pathway Dependency and Targeted Therapy

Mucosal Melanoma: Pathological Evolution, Pathway Dependency and Targeted Therapy

Association of Melanoma-Risk Variants with Primary Melanoma Tumor Prognostic Characteristics and Melanoma-Specific Survival in the GEM Study

CDK4/6 Inhibitors in Melanoma: A Comprehensive Review

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