| Literature DB >> 30714079 |
Peter A Johansson1, Andrew Stark2, Jane M Palmer3, Kieron Bigby4,5,6, Kelly Brooks3, Olivia Rolfe2, Antonia L Pritchard3,7, Kevin Whitehead8, Sunil Warrier2, William Glasson2, Nicholas K Hayward3.
Abstract
There is currently no effective treatment for metastasised uveal melanoma (UM). Recently, it was reported that a UM patient was responsive to checkpoint inhibitor (CI) treatment, due to a high tumour mutation burden correlated with a germline loss-of-function MBD4 mutation. Here, we report on another UM patient who carried an MBD4 germline nonsense variant (p.Leu563Ter) and her tumour showed a fivefold higher than average mutation burden. We confirmed the association between germline loss-of-function variant in MBD4 and CI response. The patient experienced stable disease (10 months) and survived 2 years with metastatic disease, which is twice as long as median survival. Additionally, the frequency of MBD4 loss-of-function variants in reported UM cohorts was > 20 times higher than in an aggregated population genome database (P < 5 × 10-5), implying a potential role as UM predisposition gene. These findings provide a strong basis for the inclusion of MBD4 in the screening of potential UM-prone families as well as stratification of immunotherapy.Entities:
Keywords: Immunotherapy; MBD4; Mutation; Predisposition gene; Uveal melanoma
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Year: 2019 PMID: 30714079 DOI: 10.1007/s00251-019-01108-x
Source DB: PubMed Journal: Immunogenetics ISSN: 0093-7711 Impact factor: 2.846