Germline loss‐of‐function variants in MBD4 are rare in Finnish patients with uveal melanoma

Germline loss‐of‐function variants in MBD4 are rare in Finnish patients with uveal melanoma

Uveal melanoma (UM) is a rare intraocular cancer with the highest incidence in northern latitudes. Metastases develop in approximately 50% of patients, whereafter the median survival is 13 months. Generally, the mutation burden of these tumors is low. Germline variants predisposing to UM have been p...

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Bibliographic Details
Published in:Pigment cell and melanoma research Vol. 33; no. 5; pp. 756 - 762
Main Authors: Repo, Pauliina, Jäntti, Johannes E., Järvinen, Reetta‐Stiina, Rantala, Elina S., Täll, Martin, Raivio, Virpi, Kivelä, Tero T., Turunen, Joni A.
Format: Journal Article
Language:English
Published: England Wiley Subscription Services, Inc 01-09-2020
Subjects:
BRCA1 protein
BRCA1‐associated protein 1
CpG islands
familial cancer
hypermutated phenotype
Immune checkpoint inhibitors
Melanoma
Metastases
methyl‐CpG‐binding domain 4
Mutation
Tumors
uveal melanoma
MBD4
hypermutated phenotype
immune checkpoint inhibitors
familial cancer
uveal melanoma
BAP1
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Summary:Uveal melanoma (UM) is a rare intraocular cancer with the highest incidence in northern latitudes. Metastases develop in approximately 50% of patients, whereafter the median survival is 13 months. Generally, the mutation burden of these tumors is low. Germline variants predisposing to UM have been previously described in BRCA1‐associated protein 1 (BAP1). Recently, germline and somatic loss‐of‐function (LOF) variants in the methyl‐CpG‐binding domain 4 (MBD4) gene have been found to cause a hypermutated UM, and MBD4 also has been put forward as a gene predisposing to UM. We sequenced for MBD4 germline variants in 440 Finnish patients with UM and identified seven rare exonic missense variants in 16 (3.6%) patients, of which one likely alters MBD4 function. The frequency of likely pathogenic variants in our cohort is 0.23% (1/432; 95% CI, 0.01–1.28). We identified no LOF variants though their frequency in the Finnish population is 0.052%. Thus, our data do not support the suggestion that MBD4 germline variants predispose to UM. Somatic loss of MBD4 might modify the mutational burden in UM and change its response to immune checkpoint inhibitors.
Bibliography:Funding information
This work was supported by the Helsinki University Hospital Research Fund [grant number TYH2017218 to T.T.K.]; the Cancer Foundation Finland [to T.T.K.]; the Sigrid Jusélius Foundation [to T.T.K]; and the Eye Foundation [to J.A.T.].
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ISSN:1755-1471
1755-148X
DOI:10.1111/pcmr.12892