Accession Number : AD1035973


Title :   A Gene Expression Profile of BRCAness That Predicts for Responsiveness to Platinum and PARP Inhibitors


Descriptive Note : Technical Report,15 Jul 2010,02 Nov 2016


Corporate Author : Dana Farber Cancer Institute Boston United States


Personal Author(s) : Konstantinopoulos,Panagiotis


Full Text : https://apps.dtic.mil/dtic/tr/fulltext/u2/1035973.pdf


Report Date : 01 Feb 2017


Pagination or Media Count : 32


Abstract : Our results thus far support the hypothesis that the BRCAness profile is able to track diverse molecular mechanisms that cause defective homologous recombination (HR) and that it is associated with survival in patients with sporadic disease and clinical responsiveness to platinum. Specifically, application of the BRCAness profile in the TCGA EOC dataset can identify tumors that have defective HR due to overexpression of certain miRNAs, in the absence of known genetic and epigenetic abnormalities of the HR pathway. Furthermore, the HSP90 inhibitor 17-AAG enhances sensitivity of non-BRCA1/2 mutated ovarian cancer cells to DSB-inducing agents olaparib and carboplatin at very low, sublethal concentrations. Importantly, the mechanism for this synergistic effect seems to be increasing DNA damage via suppressing HR. Finally, high quality RNA from formalin fixed paraffin embedded ovarian cancer sections can be extracted and its detection and quantitation is highly concordant with that obtained from frozen tissue.


Descriptors :   OVARIAN CANCER , chemotherapy , neoplasms , gene expression , metabolic diseases , lymphocytes , therapeutics , clinical trials , breast cancer , oncology , inhibitors , proteins


Subject Categories : Medicine and Medical Research


Distribution Statement : APPROVED FOR PUBLIC RELEASE