Long noncoding RNA LINP1 regulates repair of DNA double-strand breaks in triple-negative breast cancer

Authors
Zhang Y1, He Q1, Hu Z1, Feng Y1,2, Fan L1, Tang Z1, Yuan J1, Shan W1, Li C1,3, Hu X1,3, Tanyi JL3, Fan Y4, Huang Q5, Montone K6, Dang CV2,7,8, Zhang L1,3,8.
06-15-2016
12:00pm
PST
Categories
RNA & Disease
Speaker
Roman Camarda
Abstract
Long noncoding RNAs (lncRNAs) play critical roles during tumorigenesis by functioning as scaffolds that regulate proteinprotein, protein-DNA or protein-RNA interactions. Using a clinically guided genetic screening approach, we identified lncRNA in nonhomologous end joining (NHEJ) pathway 1 (LINP1), which is overexpressed in human triple-negative breast cancer. We found that LINP1 enhances repair of DNA double-strand breaks by serving as a scaffold linking Ku80 and DNA-PKcs, thereby coordinating the NHEJ pathway. Importantly, blocking LINP1, which is regulated by p53 and epidermal growth factor receptor (EGFR) signaling, increases the sensitivity of the tumor-cell response to radiotherapy in breast cancer.