1. Functional characterization of 84 PALB2 variants of uncertain significance
- Author
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Mandy Ducy, Jacques Simard, Bing Xia, Fergus J. Couch, Amélie Rodrigue, Chunling Hu, Thiago T. Gomes, Tzeh Keong Foo, Alvaro N.A. Monteiro, Timothy D. Wiltshire, Marcelo A. Carvalho, Jean-Yves Masson, Anil Belur Nagaraj, and Kun Y. Lee
- Subjects
0301 basic medicine ,Genetics ,DNA repair ,DNA damage ,PALB2 ,RAD51 ,030105 genetics & heredity ,Biology ,Article ,Germline ,Human genetics ,homologous recombination repair ,3. Good health ,03 medical and health sciences ,breast cancer ,PARP inhibitor ,030104 developmental biology ,variant of uncertain significance (VUS) ,Missense mutation ,Genetics (clinical) - Abstract
Purpose Inherited pathogenic variants in PALB2 are associated with increased risk of breast and pancreatic cancer. However, the functional and clinical relevance of many missense variants of uncertain significance (VUS) identified through clinical genetic testing is unclear. The ability of patient-derived germline missense VUS to disrupt PALB2 function was assessed to identify variants with potential clinical relevance. Methods The influence of 84 VUS on PALB2 function was evaluated using a cellular homology directed DNA repair (HDR) assay and VUS impacting activity were further characterized using secondary functional assays. Results Four (~5%) variants (p.L24S,c.71T>C; p.L35P,c.104T>C; pI944N,c.2831T>A; and p.L1070P,c.3209T>C) disrupted PALB2-mediated HDR activity. These variants conferred sensitivity to cisplatin and a poly(ADP-ribose) polymerase (PARP) inhibitor and reduced RAD51 foci formation in response to DNA damage. The p.L24S and p.L35P variants disrupted BRCA1–PALB2 protein complexes, p.I944N was associated with protein instability, and both p.I944N and p.L1070P mislocalized PALB2 to the cytoplasm. Conclusion These findings show that the HDR assay is an effective method for screening the influence of inherited variants on PALB2 function, that four missense variants impact PALB2 function and may influence cancer risk and response to therapy, and suggest that few inherited PALB2 missense variants disrupt PALB2 function in DNA repair.
- Published
- 2020
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