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SAPCD2 promotes neuroblastoma progression by altering the subcellular distribution of E2F7

Zi-Mu Zhang, Haibo Cao, Zhi-Heng Li, Ran Zhuo, Yanfang Tao, Xiaolu Li, Gen Li, Xinmei Liao, Fang Fang, Yi Xie, Di Wu, Hairong Wang, Jianwei Wang, Yanling Chen, Juanjuan Yu, Si-qi Jia, Randong Yang, Xinyi Guo, Yang Yang, Chenxi Feng, Yunyun Xu, Guang-Hui Qian, Jian Pan

2022Cell Death and Disease17 citationsDOIOpen Access PDF

Abstract

Recent studies uncovered the emerging roles of SAPCD2 (suppressor anaphase-promoting complex domain containing 2) in several types of human cancer. However, the functions and underlying mechanisms of SAPCD2 in the progression of neuroblastoma (NB) remain elusive. Herein, through integrative analysis of public datasets and regulatory network of GSK-J4, a small-molecule drug with anti-NB activity, we identified SAPCD2 as an appealing target with a high connection to poor prognosis in NB. SAPCD2 promoted NB progression in vitro and in vivo. Mechanistically, SAPCD2 could directly bind to cytoplasmic E2F7 but not E2F1, alter the subcellular distribution of E2F7 and regulate E2F activity. Among the E2F family members, the roles of E2F7 in NB are poorly understood. We found that an increasing level of nuclear E2F7 was induced by SAPCD2 knockdown, thereby affecting the expression of genes involved in the cell cycle and chromosome instability. In addition, Selinexor (KTP-330), a clinically available inhibitor of exportin 1 (XPO1), could induce nuclear accumulation of E2F7 and suppress the growth of NB. Overall, our studies suggested a previously unrecognized role of SAPCD2 in the E2F signaling pathway and a potential therapeutic approach for NB, as well as clues for understanding the differences in subcellular distribution of E2F1 and E2F7 during their nucleocytoplasmic shuttling.

Topics & Concepts

BiologyE2FCell biologySubcellular localizationGene knockdownSuppressorCancer researchCell cycleGeneCytoplasmGeneticsNeuroblastoma Research and TreatmentsCancer, Hypoxia, and MetabolismMicrotubule and mitosis dynamics