Whole Exome Sequencing Identifies Candidate Genes Associated with Hereditary Predisposition to Uveal Melanoma

Mohamed H Abdel-Rahman; Klarke M Sample; Robert Pilarski; Tomas Walsh; Timothy Grosel; Daniel Kinnamon; Getachew Boru; James B Massengill; Lynn Schoenfield; Ben Kelly; David Gordon; Peter Johansson; Meghan J DeBenedictis; Arun Singh; Silvia Casadei; Frederick H Davidorf; Peter White; Andrew W Stacey; James Scarth; Ellie Fewings; Marc Tischkowitz; Mary-Claire King; Nicholas K Hayward; Colleen M Cebulla

doi:10.1016/j.ophtha.2019.11.009

Whole Exome Sequencing Identifies Candidate Genes Associated with Hereditary Predisposition to Uveal Melanoma

Ophthalmology. 2020 May;127(5):668-678. doi: 10.1016/j.ophtha.2019.11.009. Epub 2019 Nov 18.

Authors

Mohamed H Abdel-Rahman¹, Klarke M Sample², Robert Pilarski³, Tomas Walsh⁴, Timothy Grosel², Daniel Kinnamon³, Getachew Boru², James B Massengill², Lynn Schoenfield⁵, Ben Kelly⁶, David Gordon⁶, Peter Johansson⁷, Meghan J DeBenedictis⁸, Arun Singh⁸, Silvia Casadei⁴, Frederick H Davidorf², Peter White⁶, Andrew W Stacey⁹, James Scarth¹⁰, Ellie Fewings¹⁰, Marc Tischkowitz¹¹, Mary-Claire King¹², Nicholas K Hayward⁷, Colleen M Cebulla²

Affiliations

¹ Department of Ophthalmology and Visual Science, Havener Eye Institute, The Ohio State University, Columbus, Ohio; Division of Human Genetics, Department of Internal Medicine, The Ohio State University, Columbus, Ohio. Electronic address: Mohamed.abdel-rahman@osumc.edu.
² Department of Ophthalmology and Visual Science, Havener Eye Institute, The Ohio State University, Columbus, Ohio.
³ Division of Human Genetics, Department of Internal Medicine, The Ohio State University, Columbus, Ohio.
⁴ Department of Genome Sciences, University of Washington, Seattle, Washington.
⁵ Department of Pathology, The Ohio State University, Columbus, Ohio.
⁶ The Institute for Genomic Medicine, Nationwide Children's Hospital, Columbus, Ohio.
⁷ QIMR Berghofer Medical Research Institute, Brisbane, Australia.
⁸ Department of Ophthalmic Oncology, Cole Eye Institute, Cleveland Clinic, Cleveland, Ohio.
⁹ Department of Ophthalmology, University of Washington, Seattle, Washington.
¹⁰ Academic Laboratory of Medical Genetics and National Institute for Health Research Cambridge Biomedical Research Centre, University of Cambridge, Cambridge, United Kingdom.
¹¹ Academic Laboratory of Medical Genetics and National Institute for Health Research Cambridge Biomedical Research Centre, University of Cambridge, Cambridge, United Kingdom; East Anglian Medical Genetics Service, Cambridge University Hospitals, Cambridge, United Kingdom.
¹² Department of Genome Sciences, University of Washington, Seattle, Washington; Department of Medicine, University of Washington, Seattle, Washington.

Abstract

Purpose: To identify susceptibility genes associated with hereditary predisposition to uveal melanoma (UM) in patients with no detectable germline BAP1 alterations.

Design: Retrospective case series from academic referral centers.

Participants: Cohort of 154 UM patients with high risk of hereditary cancer defined as patients with 1 or more of the following: (1) familial UM, (2) young age (<35 years) at diagnosis, (3) personal history of other primary cancers, and (4) family history of 2 or more primary cancers with no detectable mutation or deletion in BAP1 gene.

Methods: Whole exome sequencing, a cancer gene panel, or both were carried out. Probands included 27 patients with familial UM, 1 patient with bilateral UM, 1 patient with congenital UM, and 125 UM patients with strong personal or family histories, or both, of cancer. Functional validation of variants was carried out by immunohistochemistry, reverse-transcriptase polymerase chain reaction, and genotyping.

Main outcome measures: Clinical characterization of UM patients with germline alterations in known cancer genes.

Results: We identified actionable pathogenic variants in 8 known hereditary cancer predisposition genes (PALB2, MLH1, MSH6, CHEK2, SMARCE1, ATM, BRCA1, and CTNNA1) in 9 patients, including 3 of 27 patients (11%) with familial UM and 6 of 127 patients (4.7%) with a high risk for cancer. Two patients showed pathogenic variants in CHEK2 and PALB2, whereas variants in the other genes each occurred in 1 patient. Biallelic inactivation of PALB2 and MLH1 was observed in tumors from the respective patients. The frequencies of pathogenic variants in PALB2, MLH1, and SMARCE1 in UM patients were significantly higher than the observed frequencies in noncancer controls (PALB2: P = 0.02; odds ratio, 8.9; 95% confidence interval, 1.5-30.6; MLH1: P = 0.04; odds ratio, 25.4; 95% confidence interval, 1.2-143; SMARCE1: P = 0.001; odds ratio, 2047; 95% confidence interval, 52-4.5e15, respectively).

Conclusions: The study provided moderate evidence of gene and disease association of germline mutations in PALB2 and MLH1 with hereditary predisposition to UM. It also identified several other candidate susceptibility genes. The results suggest locus heterogeneity in predisposition to UM. Genetic testing for hereditary predisposition to cancer is warranted in UM patients with strong personal or family history of cancers, or both.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Adult
Aged
Aged, 80 and over
Child
Child, Preschool
DNA, Neoplasm / genetics
Exome Sequencing
Female
Genes, Neoplasm / genetics*
Genetic Predisposition to Disease / genetics*
Germ-Line Mutation / genetics
Humans
Immunohistochemistry
Infant
Male
Melanoma / genetics*
Middle Aged
Neoplasm Proteins / genetics*
Retrospective Studies
Reverse Transcriptase Polymerase Chain Reaction
Tumor Suppressor Proteins / genetics
Ubiquitin Thiolesterase / genetics
Uveal Neoplasms / genetics*

Substances

BAP1 protein, human
DNA, Neoplasm
Neoplasm Proteins
Tumor Suppressor Proteins
Ubiquitin Thiolesterase

Supplementary concepts

Uveal melanoma

Abstract

Publication types

MeSH terms

Substances

Supplementary concepts

Grants and funding