ILF2 Is a Regulator of RNA Splicing and DNA Damage Response in 1q21-Amplified Multiple Myeloma

ILF2是1q21扩增型多发性骨髓瘤中RNA剪接和DNA损伤反应的调节因子

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作者:Matteo Marchesini ,Yamini Ogoti ,Elena Fiorini ,Anil Aktas Samur ,Luigi Nezi ,Marianna D'Anca ,Paola Storti ,Mehmet Kemal Samur ,Irene Ganan-Gomez ,Maria Teresa Fulciniti ,Nipun Mistry ,Shan Jiang ,Naran Bao ,Valentina Marchica ,Antonino Neri ,Carlos Bueso-Ramos ,Chang-Jiun Wu ,Li Zhang ,Han Liang ,Xinxin Peng ,Nicola Giuliani ,Giulio Draetta ,Karen Clise-Dwyer ,Hagop Kantarjian ,Nikhil Munshi ,Robert Orlowski ,Guillermo Garcia-Manero ,Ronald A DePinho ,Simona Colla

Abstract

Amplification of 1q21 occurs in approximately 30% of de novo and 70% of relapsed multiple myeloma (MM) and is correlated with disease progression and drug resistance. Here, we provide evidence that the 1q21 amplification-driven overexpression of ILF2 in MM promotes tolerance of genomic instability and drives resistance to DNA-damaging agents. Mechanistically, elevated ILF2 expression exerts resistance to genotoxic agents by modulating YB-1 nuclear localization and interaction with the splicing factor U2AF65, which promotes mRNA processing and the stabilization of transcripts involved in homologous recombination in response to DNA damage. The intimate link between 1q21-amplified ILF2 and the regulation of RNA splicing of DNA repair genes may be exploited to optimize the use of DNA-damaging agents in patients with high-risk MM. Keywords: 1q21 amplification; DNA damage; DNA repair; ILF2; multiple myeloma; splicing.

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