The Prognostic Significance of Low-Frequency Somatic Mutations in Metastatic Cutaneous Melanoma

Xiaobei Zhao; Paul Little; Alan P Hoyle; Guillaume J Pegna; Michele C Hayward; Anastasia Ivanova; Joel S Parker; David L Marron; Matthew G Soloway; Heejoon Jo; Ashley H Salazar; Michael P Papakonstantinou; Deeanna M Bouchard; Stuart R Jefferys; Katherine A Hoadley; David W Ollila; Jill S Frank; Nancy E Thomas; Paul B Googe; Ashley J Ezzell; Frances A Collichio; Carrie B Lee; H Shelton Earp; Norman E Sharpless; Willy Hugo; James S Wilmott; Camelia Quek; Nicola Waddell; Peter A Johansson; John F Thompson; Nicholas K Hayward; Graham J Mann; Roger S Lo; Douglas B Johnson; Richard A Scolyer; D Neil Hayes; Stergios J Moschos

doi:10.3389/fonc.2018.00584

The Prognostic Significance of Low-Frequency Somatic Mutations in Metastatic Cutaneous Melanoma

Front Oncol. 2019 Jan 4:8:584. doi: 10.3389/fonc.2018.00584. eCollection 2018.

Authors

Xiaobei Zhao¹, Paul Little², Alan P Hoyle¹, Guillaume J Pegna³, Michele C Hayward¹, Anastasia Ivanova^{1

2}, Joel S Parker¹, David L Marron¹, Matthew G Soloway¹, Heejoon Jo¹, Ashley H Salazar¹, Michael P Papakonstantinou¹, Deeanna M Bouchard¹, Stuart R Jefferys¹, Katherine A Hoadley¹, David W Ollila^{1

4

5}, Jill S Frank^{1

5}, Nancy E Thomas^{1

5

6}, Paul B Googe^{1

5

6}, Ashley J Ezzell⁷, Frances A Collichio^{1

3

5}, Carrie B Lee^{1

3

5}, H Shelton Earp¹, Norman E Sharpless¹, Willy Hugo⁸, James S Wilmott⁹, Camelia Quek⁹, Nicola Waddell¹⁰, Peter A Johansson¹⁰, John F Thompson⁹, Nicholas K Hayward¹⁰, Graham J Mann⁹, Roger S Lo⁸, Douglas B Johnson¹¹, Richard A Scolyer¹⁰, D Neil Hayes^{1

3}, Stergios J Moschos^{1

3

5}

Affiliations

¹ Lineberger Comprehensive Cancer Center, The University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.
² Department of Biostatistics, Gillings School of Public Health, The University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.
³ Division of Hematology/Oncology, Department of Medicine, The University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.
⁴ Division of Surgical Oncology, Department of Surgery, The University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.
⁵ Melanoma Program, The University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.
⁶ Department of Dermatology, The University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.
⁷ Department of Cell Biology & Physiology, Histology Research Core Facility, The University of North Carolina at Chapel Hill, Chapel Hill, NC, United States.
⁸ Division of Dermatology, Department of Medicine, Jonsson Comprehensive Cancer Center, University of California, Los Angeles, Los Angeles, CA, United States.
⁹ Melanoma Institute Australia, The University of Sydney, Sydney, NSW, Australia.
¹⁰ Queensland Institute of Medical Research-QIMR Berghofer Medical Research Institute, Herston, QLD, Australia.
¹¹ Department of Medicine, Vanderbilt-Ingram Cancer Center, Nashville, TN, United States.

Abstract

Background: Little is known about the prognostic significance of somatically mutated genes in metastatic melanoma (MM). We have employed a combined clinical and bioinformatics approach on tumor samples from cutaneous melanoma (SKCM) as part of The Cancer Genome Atlas project (TCGA) to identify mutated genes with potential clinical relevance. Methods: After limiting our DNA sequencing analysis to MM samples (n = 356) and to the CANCER CENSUS gene list, we filtered out mutations with low functional significance (snpEFF). We performed Cox analysis on 53 genes that were mutated in ≥3% of samples, and had ≥50% difference in incidence of mutations in deceased subjects versus alive subjects. Results: Four genes were potentially prognostic [RAC1, FGFR1, CARD11, CIITA; false discovery rate (FDR) < 0.2]. We identified 18 additional genes (e.g., SPEN, PDGFRB, GNAS, MAP2K1, EGFR, TSC2) that were less likely to have prognostic value (FDR < 0.4). Most somatic mutations in these 22 genes were infrequent (< 10%), associated with high somatic mutation burden, and were evenly distributed across all exons, except for RAC1 and MAP2K1. Mutations in only 9 of these 22 genes were also identified by RNA sequencing in >75% of the samples that exhibited corresponding DNA mutations. The low frequency, UV signature type and RNA expression of the 22 genes in MM samples were confirmed in a separate multi-institution validation cohort (n = 413). An underpowered analysis within a subset of this validation cohort with available patient follow-up (n = 224) showed that somatic mutations in SPEN and RAC1 reached borderline prognostic significance [log-rank favorable (p = 0.09) and adverse (p = 0.07), respectively]. Somatic mutations in SPEN, and to a lesser extent RAC1, were not associated with definite gene copy number or RNA expression alterations. High (>2+) nuclear plus cytoplasmic expression intensity for SPEN was associated with longer melanoma-specific overall survival (OS) compared to lower (≤ 2+) nuclear intensity (p = 0.048). We conclude that expressed somatic mutations in infrequently mutated genes beyond the well-characterized ones (e.g., BRAF, RAS, CDKN2A, PTEN, TP53), such as RAC1 and SPEN, may have prognostic significance in MM.

Keywords: RAC1; RNA sequencing; SPEN; The Cancer Genome Atlas Project; UV signature; cutaneous melanoma; next generation sequencing; prognostic significance.

Abstract

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