QSER1 preserves the suppressive status of the pro-apoptotic genes to prevent apoptosis

Activation of the pro-apoptotic genes by the p53 family is a critical step in induction of apoptosis. However, the molecular signaling underlying their suppression remains largely unknown. Here, we report a general role of QSER1 in preventing apoptosis. QSER1 is widely up-regulated in multiple cancers, and its up-regulation correlates with poor clinic outcomes. QSER1 knockdown significantly promotes apoptosis in both p53 wild type and mutant cancer cells. Interestingly, we show that QSER1 and p53 occupy distinct cis-regulatory regions in a common subset of the pro-apoptotic genes, and function antagonistically to maintain their proper expression. Furthermore, we identify a key regulatory DNA element named QSER1 binding site in PUMA (QBP). Deletion of QBP de-represses PUMA and induces apoptosis. Mechanistically, QSER1 functions together with SIN3A to suppress PUMA in a p53-dependent and -independent manner, suggesting that QSER1 inhibition might be a potential therapeutic strategy to induce apoptosis in cancers.

Automated summary

QSER1 plays a general role in preventing apoptosis and is up-regulated in multiple cancers. It functions antagonistically with p53 to maintain the expression of pro-apoptotic genes and suppresses PUMA in a p53-dependent and -independent manner. Inhibition of QSER1 might be a potential therapeutic strategy to induce apoptosis in cancer cells.