Author:
Takaku Motoki,Grimm Sara A.,Roberts John D.,Chrysovergis Kaliopi,Bennett Brian D.,Myers Page,Perera Lalith,Tucker Charles J.,Perou Charles M.,Wade Paul A.
Abstract
AbstractGATA3 is frequently mutated in breast cancer; these mutations are widely presumed to be loss of function. Here, we address molecular alterations downstream of a novel class of GATA3 mutations, revealing both gain and loss of function. Mutation of one allele of GATA3 led to loss of binding and decreased expression at a subset of genes, including Progesterone Receptor. At other loci, associated with epithelial to mesenchymal transition, gain of binding at a novel sequence motif correlated with increased gene expression. These results demonstrate that not all GATA3 mutations are equivalent and that these mutations impact breast cancer through gain and loss of function.
Publisher
Cold Spring Harbor Laboratory