Variable Genomic Landscapes of Advanced Melanomas with Heavy Pigmentation

Huang, Richard S.P.; Tse, Julie Y; Harries, Lukas; Graf, Ryon P.; Lin, Douglas I.; Murugesan, Karthikeyan; Hiemenz, Matthew; Parimi, Vamsi; Janovitz, Tyler; Decker, Brennan; Severson, Eric Allan; Levy, Mia A.; Ramkissoon, Shakti; Elvin, Julia A.; Ross, Jeffrey S.; Williams, Erik

doi:10.1093/oncolo/oyac090

Cited by 3 publications

(2 citation statements)

References 37 publications

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“…In fact, although the data demonstrate that this panel was able to identify mutations in almost all advanced melanoma, in 10% of these, no alterations were identified. In these samples, it might be worth investigating other markers, such as using a panel for fusion genes (e.g., ALK fusions) [28] or a Comprehensive Genomic Profiling (CGP) panel [29,30], allowing the identification of mutations in uncommonly altered genes. With our panel, the primary and metastatic samples showed the same molecular structure; however, the extension to other markers could also be performed to understand whether there are any acquired variants in the metastases that are not present in the primary lesion.…”

Section: Discussionmentioning

confidence: 99%

Molecular Characterization of Advanced-Stage Melanomas in Clinical Practice Using a Laboratory-Developed Next-Generation Sequencing Panel

Maloberti,

De Leo,

Coluccelli

et al. 2024

Diagnostics

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Cutaneous melanoma is one of the most lethal tumors among skin cancers, characterized by complex genetic and molecular alterations that result in uncontrolled cell proliferation and metastatic spread. Next-generation sequencing (NGS) enables the simultaneous examination of numerous genes, making this molecular technique essential for melanoma diagnosis, prognostic stratification, and therapy planning. Herein, we present the experience with our laboratory-designed NGS panel for the routine assessment of advanced-stage melanoma. A total of 260 specimens of advanced-stage melanomas were evaluated utilizing a laboratory-developed multi-gene NGS panel, which allowed the investigation of 229 amplicons in 25 oncogene/oncosuppressor genes. The NGS panel proved to be a reliable tool, failing to produce results in only 1.2% of the samples tested. BRAF and TERT were the two more commonly altered genes in 44.0% and 59.9% of samples, respectively. In 59.3% of the mutated cases, at least two concomitant variants were detected. In eight cases, both primary lesion and metastatic disease were analyzed by NGS. In all specimens (8/8, 100%), a perfect concordance in variants harbored by the primary and recurrence lesions was observed. Finally, this study described the validity of a laboratory-developed multi-gene NGS panel built specifically for advanced-stage melanomas in ordinary clinical practice.

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Section: Discussionmentioning

confidence: 99%

Molecular Characterization of Advanced-Stage Melanomas in Clinical Practice Using a Laboratory-Developed Next-Generation Sequencing Panel

Maloberti,

De Leo,

Coluccelli

et al. 2024

Diagnostics

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“…The paper by Huan R.S.P. et al [ 29 ] is very interesting, in which the authors analysed 1268 melanoma samples for which an IHC investigation for PD-L1 was requested and which were divided into high-pigmented melanoma (HPMel) and low-pigmented melanoma (LPMel), constituting 13.0% and 87.0% of the sample, respectively. In terms of TMB, in the HPMel cohort, TMB was significantly lower (median 8.8 mutations/Mb) than in the LPMel group (11.4 mutations/Mb), while secondary molecular alterations such as TERTp, CDKN2A, TP53, and PTEN were lower in HPMel cases than in LPMel ones.…”

Section: Pd-l1 Tmb and Molecular Featuresmentioning

confidence: 99%

Immunohistochemical Expression of Programmed Cell Death Ligand 1 (PD-L1) in Human Cutaneous Malignant Melanoma: A Narrative Review with Historical Perspectives

Cazzato

Lettini

Colagrande

et al. 2023

Genes

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Programmed death-ligand 1 (PD-L1) is the primary ligand of the receptor programmed death-1 (PD-1) which is constitutively expressed or activated in myeloid, lymphoid (T, B and NK), normal epithelial cells, and cancer. The PD-1/PD-L1 interaction is crucial for the physiological development of immunological tolerance but also in the development of the cancer. Among these, malignant melanoma represents a tumour in which the immunohistochemical expression of PD-L1 is important to guide future therapeutic choices based on the presence/absence of expression. Various clones have been used over time for immunohistochemical determination, and different results and heterogeneity remain among the various studies in the literature. We perform a narrative review of the present studies in order to discuss and take stock of what certain achievements have been made in this field, what challenges remain, and what possible solutions can be found.

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Brightfield Multiplex Immunohistochemistry Assay for PD-L1 Evaluation in Challenging Melanoma Samples

Ugolini,

Tinunin,

Nozzoli

et al. 2024

Applied Immunohistochemistry &Amp; Molecular Morphology

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Targeting the PD1/PD-L1 immune checkpoint pathway has rapidly become a therapeutic strategy for melanoma patients. Indeed, the quantification of PD-L1 expression by immunohistochemistry (IHC) in melanoma samples is already required, in some contexts, to allow access to anti-PD-1/PD-L1 immunotherapy. Despite a rising demand for PD-L1 testing, paralleling increasing cumulative experience in its assessment and quantification, it is fair to recognize that PD-L1 evaluation in melanoma samples still presents some critical issues. The aim of this technical report is to develop and validate a multiplex double staining protocol for PD-L1/SOX10 in Ventana Benchmark Ultra for routine practice. Our results show that double labeling provides the necessary tools to identify PD-L1+ melanoma cells clearly. The simultaneous visualization of 2 different proteins targets allows the topographical relationship between the 2 labeling to be evaluated within the context of the tissue morphology. Future studies are needed to test this technique’s real-world applicability and effectiveness in implementing interpathologist agreement.

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Variable Genomic Landscapes of Advanced Melanomas with Heavy Pigmentation

Cited by 3 publications

References 37 publications

Molecular Characterization of Advanced-Stage Melanomas in Clinical Practice Using a Laboratory-Developed Next-Generation Sequencing Panel

Molecular Characterization of Advanced-Stage Melanomas in Clinical Practice Using a Laboratory-Developed Next-Generation Sequencing Panel

Immunohistochemical Expression of Programmed Cell Death Ligand 1 (PD-L1) in Human Cutaneous Malignant Melanoma: A Narrative Review with Historical Perspectives

Brightfield Multiplex Immunohistochemistry Assay for PD-L1 Evaluation in Challenging Melanoma Samples

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