Abstract:The missense mutations of the BRCT domain of human BRCA1 have been argued to be associated with predisposition to hereditary breast/ovarian cancer. Mutations at the C-terminus of the protein are critical for function and structural excellence. This mutation has been associated with changes in the structure of the protein and loss of interaction with other peptides involved in cell cycle control. In previous studies we have shown that the modification of various mutants in BRCT domain, such as Met1775K is stron… Show more
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