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Silencing of SENP2 in Multiple Myeloma Induces Bortezomib Resistance by Activating NF-κB Through the Modulation of IκBα Sumoylation

Hong-Yi Xie, Yuanliang Gu, Wenjuan Wang, Xuyao Wang, Xiao-Juan Ye, Chao Xin, Mengjiao Lü, B. Ashok Reddy, Peng Shu

2020Scientific Reports27 citationsDOIOpen Access PDF

Abstract

The proteasome inhibitor bortezomib is the most successfully applied chemotherapeutic drug for treating multiple myeloma. However, its clinical efficacy reduced due to resistance development. The underlying molecular mechanisms of bortezomib resistance are poorly understood. In this study, by combining in silico analysis and sgRNA library based drug resistance screening assay, we identified SENP2 (Sentrin/SUMO-specific proteases-2) as a bortezomib sensitive gene and found its expression highly downregulated in bortezomib resistant multiple myeloma patient's samples. Furthermore, down regulation of SENP2 in multiple myeloma cell line RPMI8226 alleviated bortezomib induced cell proliferation inhibition and apoptosis, whereas, overexpression of SENP2 sensitized these cells to bortezomib treatment. We further demonstrate that knockdown of SENP2 in RPMI8226 cells increased SUMO2 conjugated IκBα that resulted in the activation of NF-κB. Taken together, we report that silencing of SENP2 and consequent activation of NF-κB through the modulation of IκBα sumoylation as a novel mechanism inducing bortezomib resistance in multiple myeloma.

Topics & Concepts

BortezomibMultiple myelomaGene silencingSUMO proteinGene knockdownCancer researchProteasome inhibitorApoptosisChemistryProteasomeRNA interferenceNF-κBDownregulation and upregulationBiologyPharmacologyUbiquitinImmunologyGeneBiochemistryRNAMultiple Myeloma Research and TreatmentsUbiquitin and proteasome pathwaysProtein Degradation and Inhibitors