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GATA3 Truncating Mutations Promote Cistromic Re-Programming In Vitro, but Not Mammary Tumor Formation in Mice.

Lisette M Cornelissen ,
Roebi de Bruijn ,
Linda Henneman ,
Yongsoo Kim ,
Wilbert Zwart ,
Jos Jonkers

Abstract

Heterozygous mutations in the transcription factor GATA3 are identified in 10-15% of all breast cancer cases. Most of these are protein-truncating mutations, concentrated within or downstream of the second GATA-type zinc-finger domain. Here, we investigated the functional consequences of expression of two truncated GATA3 mutants, in vitro in breast cancer cell lines and in vivo in the mouse mammary gland. We found that the truncated GATA3 mutants display altered DNA binding activity caused by preferred tethering through FOXA1. In addition, expression of the truncated GATA3 mutants reduces E-cadherin expression and promotes anchorage-independent growth in vitro. However, we could not identify any effects of truncated GATA3 expression on mammary gland development or mammary tumor formation in mice. Together, our results demonstrate that both truncated GATA3 mutants promote cistromic re-programming of GATA3 in vitro, but these mutants are not sufficient to induce tumor formation in mice.

More about this publication

Journal of mammary gland biology and neoplasia

Volume 24
Issue nr. 3
Pages 271-284
Publication date 01-09-2019

Full text links

Publisher website (DOI) 10.1007/s10911-019-09432-4
Europe PubMed Central 31218575
Pubmed 31218575

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