| Literature DB >> 22266096 |
Siker Kimbung1, Ewa Biskup2, Ida Johansson1, Kristina Aaltonen1, Astrid Ottosson-Wadlund3, Sofia Gruvberger-Saal1, Heather Cunliffe4, Bengt Fadeel3, Niklas Loman1, Pontus Berglund1, Ingrid Hedenfalk5.
Abstract
Although pre-clinical and clinical studies on PARP1 inhibitors, alone and in combination with DNA-damaging agents, show promising results, further ways to improve and broaden the scope of application of this therapeutic approach are warranted. To this end, we have investigated the possibility of improving the response of BRCA1 mutant breast cancer cells to PARP1 inhibition by co-targeting the PI3K pathway. Human breast cancer cell lines with or without the expression of BRCA1 and/or PTEN were treated with PARP1 and PI3K inhibitors as single agents and in combination. PARP1 inhibition induced DNA damage conferring a G2/M arrest and decrease in viability, paralleled by the induction of apoptosis. PI3K inhibition alone caused a G1 arrest and decreased cell growth. Most importantly, sequential combination of PARP and PI3K inhibitors interacted synergistically to significantly decrease growth compared to PARP inhibition alone. Global transcriptional profiling revealed that this decrease in growth was associated with down-regulation of macromolecule biosynthesis and the induction of apoptosis. Taken together, these results suggest an improved treatment strategy for BRCA1-mutant and possibly also triple-negative breast cancers with similar molecular defects.Entities:
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Year: 2012 PMID: 22266096 DOI: 10.1016/j.canlet.2012.01.015
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679