Functional characterization of CHEK2 variants in a Saccharomyces cerevisiae system

Citation:

Delimitsou A, Fostira F, Kalfakakou D, Apostolou P, Konstantopoulou I, Kroupis C, Papavassiliou AG, Kleibl Z, Stratikos E, Voutsinas GE, et al. Functional characterization of CHEK2 variants in a Saccharomyces cerevisiae system. Hum.Mutat. [Internet]. 2019;40(5):631 - 648.

Abstract:

Genetic testing for cancer predisposition leads to the identification of a number of variants with uncertain significance. To some extent, variants of BRCA1/2 have been classified, in contrast to variants of other genes. CHEK2 is a typical example, in which a large number of variants of unknown clinical significance were identified and still remained unclassified. Herein, the CHEK2 variant assessment was performed through an in vivo, yeast-based, functional assay. In total, 120 germline CHEK2 missense variants, distributed along the protein sequence, and two large in-frame deletions were tested, originating from genetic test results in breast cancer families, or selected from the ClinVar database. Of these, 32 missense and two in-frame deletions behaved as non-functional, 73 as functional, and 15 as semi-functional, after comparing growth rates of each strain with positive and negative controls. The majority of non-functional variants were localized in the CHK2 kinase and forkhead-associated domains. In vivo results from the non-functional variants were in agreement with in silico predictions, and, where available, with strong breast cancer family history, to a great extent. The results of the largest, to date, yeast-based assay, evaluating CHEK2 variants, can complement and assist in the classification of rare CHEK2 variants with unclear clinical significance

Notes:

IS - 1098-1004 (Electronic) IS - 1059-7794 (Linking) LA - eng PT - Journal Article PT - Research Support, Non-U.S. Gov't RN - EC 2.7.1.11 (Checkpoint Kinase 2) RN - EC 2.7.11.1 (CHEK2 protein, human) SB - IM

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