Targeting autophagy increases the efficacy of proteasome inhibitor treatment in multiple myeloma by induction of apoptosis and activation of JNK

Background The therapeutic armamentarium in multiple myeloma has been significantly broadened by proteasome inhibitors, highly efficient means in controlling of multiple myeloma. Despite the developments of therapeutic regimen in treatment of multiple myeloma, still the complete remission requires a...

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Veröffentlicht in:BMC cancer 2022-07, Vol.22 (1), p.1-735, Article 735
Hauptverfasser: Salimi, Azam, Schroeder, Kema Marlen, Schemionek-Reinders, Mirle, Vieri, Margherita, Maletzke, Saskia, Gezer, Deniz, Masouleh, Behzad Kharabi, Appelmann, Iris
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Sprache:eng
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Zusammenfassung:Background The therapeutic armamentarium in multiple myeloma has been significantly broadened by proteasome inhibitors, highly efficient means in controlling of multiple myeloma. Despite the developments of therapeutic regimen in treatment of multiple myeloma, still the complete remission requires a novel therapeutic strategy with significant difference in outcomes. Proteasome inhibitors induce autophagy and ER stress, both pivotal pathways for protein homeostasis. Recent studies showed that the IRE1[alpha]-XBP1 axis of the unfolded protein response (UPR) is up-regulated in multiple myeloma patients. In addition, XBP1 is crucial for the maintenance of viability of acute lymphoblastic leukemia (ALL). Results We analyzed the efficacy of targeting IRE1[alpha]-XBP1 axis and autophagy in combination with proteasome inhibitor, ixazomib in treatment of multiple myeloma. In this present study, we first show that targeting the IRE1[alpha]-XBP1 axis with small molecule inhibitors (STF-083010, A106) together with the ixazomib induces cell cycle arrest with an additive cytotoxic effect in multiple myeloma. Further, we examined the efficacy of autophagy inhibitors (bafilomycin A, BAF and chloroquine, CQ) together with ixazomib in multiple myeloma and observed that this combination treatment synergistically reduced cell viability in multiple myeloma cell lines (viable cells Ixa: 51.8 [+ or -] 3.3, Ixa + BAF: 18.3 [+ or -] 7.2, Ixa + CQ: 38.4 [+ or -] 3.7) and patient-derived multiple myeloma cells (Ixa: 59.6 [+ or -] 4.4, Ixa + CQ: 7.0 [+ or -] 2.1). We observed, however, that this combined strategy leads to activation of stress-induced c-Jun N-terminal kinase (JNK). Cytotoxicity mediated by combined proteasome and autophagy inhibition was reversed by addition of the specific JNK inhibitor JNK-In-8 (viable cells: Ixa + BAF: 11.6 [+ or -] 7.0, Ixa + BAF + JNK-In-8: 30.9 [+ or -] 6.1). Conclusion In this study we showed that combined inhibition of autophagy and the proteasome synergistically induces cell death in multiple myeloma. Hence, we consider the implication of pharmaceutical inhibition of autophagy together with proteasome inhibition and UPR-directed therapy as promising novel in vitro treatment strategy against multiple myeloma. Keywords: Autophagy, Multiple myeloma, Proteasome inhibition, Jnk
ISSN:1471-2407
1471-2407
DOI:10.1186/s12885-022-09775-y