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Variable Genomic Landscapes of Advanced Melanomas with Heavy Pigmentation

Authors :
Richard S P Huang
Julie Y Tse
Lukas Harries
Ryon P Graf
Douglas I Lin
Karthikeyan Murugesan
Matthew C Hiemenz
Vamsi Parimi
Tyler Janovitz
Brennan Decker
Eric Severson
Mia A Levy
Shakti H Ramkissoon
Julia A Elvin
Jeffrey S Ross
Erik A Williams
Source :
The Oncologist. 27:655-662
Publication Year :
2022
Publisher :
Oxford University Press (OUP), 2022.

Abstract

Background In the current study, we examined the real-world prevalence of highly pigmented advanced melanomas (HPMel) and the clinicopathologic, genomic, and ICPI biomarker signatures of this class of tumors. Materials and Methods Our case archive of clinical melanoma samples for which the ordering physician requested testing for both PD-L1 immunohistochemistry (IHC) and comprehensive genomic profiling (CGP) was screened for HPMel cases, as well as for non-pigmented or lightly pigmented advanced melanoma cases (LPMel). Results Of the 1268 consecutive melanoma biopsies in our archive that had been submitted for PD-L1 IHC, 13.0% (165/1268) were HPMel and 87.0% (1103/1268) were LPMel. In the HPMel cohort, we saw a significantly lower tumor mutational burden (TMB, median 8.8 mutations/Mb) than in the LPMel group (11.4 mut/Mb), although there was substantial overlap. In examining characteristic secondary genomic alterations (GA), we found that the frequencies of GA in TERTp, CDKN2A, TP53, and PTEN were significantly lower in the HPMel cases than in LPMel. A higher rate of GA in CTNNB1, APC, PRKAR1A, and KIT was identified in the HPMel cohort compared with LPMel. Conclusions In this study, we quantified the failure rates of melanoma samples for PD-L1 testing due to high melanin pigmentation and showed that CGP can be used in these patients to identify biomarkers that can guide treatment decisions for HPMel patients. Using this practical clinical definition for tumor pigmentation, our results indicate that HPMel are frequent at 13% of melanoma samples, and in general appear molecularly less developed, with a lower TMB and less frequent secondary GA of melanoma progression.

Details

ISSN :
1549490X and 10837159
Volume :
27
Database :
OpenAIRE
Journal :
The Oncologist
Accession number :
edsair.doi.dedup.....b6ca7bbcced6213f77e3daf6ecbfec66