Bakr Farrah, Kulkarni Anjana, Mounsey Stephen, Mitchell Tracey, Whittaker Sean, Lacy Katie
St John's Institute of Dermatology Guy's and St Thomas' NHS Trust London UK.
Department of Clinical Genetics Guy's and St Thomas' NHS Trust London UK.
JEADV Clin Pract. 2024 Sep;3(4):1236-1239. doi: 10.1002/jvc2.382. Epub 2024 Feb 13.
variants have been identified in familial melanoma (FM) as well as a number of other germline and somatic malignancies. The functional validation of variants identified from the screening of patients with melanoma gene susceptibility panels is key to understanding the clinical significance of identified variants. Here we report a novel, likely pathogenic missense variant (p.G95V) in FM and investigate its functional impact. We demonstrate loss of function owing to the inability of the mutant POT1 protein to bind telomeric DNA compared to its wild-type counterpart. This study provides important functional validation of a novel variant in FM.
在家族性黑色素瘤(FM)以及许多其他种系和体细胞恶性肿瘤中已鉴定出变异。对黑色素瘤基因易感性检测筛选出的患者所鉴定变异进行功能验证,对于理解所鉴定变异的临床意义至关重要。在此,我们报告FM中一种新的、可能致病的错义变异(p.G95V),并研究其功能影响。我们证明,与野生型对应物相比,突变型POT1蛋白无法结合端粒DNA,导致功能丧失。本研究为FM中的一种新变异提供了重要的功能验证。
