4.3 Article

Resensitising proteasome inhibitor-resistant myeloma with sphingosine kinase 2 inhibition

NEOPLASIA (2022)

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Journal

NEOPLASIA
Volume 24, Issue 1, Pages -

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.neo.2021.11.009

Keywords

Myeloma; Bortezomib; Resistance; Sphingolipid; Unfolded protein response

Categories

Oncology

Funding

  1. MF and MH Joyner Scholarship
  2. Royal Adelaide Hospital (RAH) Research Fund Dawes Scholarship
  3. Australian Government Research Training Program Scholarship
  4. RAH Research Fund Florey Fellowship
  5. National Cancer Institute [RO1 CA184464, RO1 CA194264]
  6. Leukemia & Lymphoma Society Specialized Center of Research [SCOR-12206-17]
  7. Dr. Miriam and Sheldon G. Adelson Research Foundation
  8. National Health and Medical Research Council of Australia (NHMRC) Peter Doherty Biomedical Early Career Fellowship [1071945]
  9. Servier Staff Barry Young Research Establishment Fellowship through the Royal Australasian College of Physicians
  10. Viertel Foundation Clinical Investigator Award
  11. Fay Fuller Foundation
  12. NHMRC [1162954, 1042589, 1156693]

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The introduction of the proteasome inhibitor bortezomib has improved patient survival in myeloma, but acquired resistance remains a challenge. Researchers have found that inhibiting sphingolipid metabolism can resensitize bortezomib-resistant myeloma, and this approach also works with other proteasome inhibitors like carfilzomib.
The introduction of the proteasome inhibitor bortezomib into treatment regimens for myeloma has led to substantial improvement in patient survival. However, whilst bortezomib elicits initial responses in many myeloma patients, this haematological malignancy remains incurable due to the development of acquired bortezomib resistance. With other patients presenting with disease that is intrinsically bortezomib resistant, it is clear that new therapeutic approaches are desperately required to target bortezomib-resistant myeloma. We have previously shown that targeting sphingolipid metabolism with the sphingosine kinase 2 (SK2) inhibitor K145 in combination with bortezomib induces synergistic death of bortezomib-naive myeloma. In the current study, we have demonstrated that targeting sphingolipid metabolism with K145 synergises with bortezomib and effectively resensitises bortezomib-resistant myeloma to this proteasome inhibitor. Notably, these effects were dependent on enhanced activation of the unfolded protein response, and were observed in numerous separate myeloma models that appear to have different mechanisms of bortezomib resistance, including a new bortezomib-resistant myeloma model we describe which possesses a clinically relevant proteasome mutation. Furthermore, K145 also displayed synergy with the next-generation proteasome inhibitor carfilzomib in bortezomib-resistant and carfilzomib-resistant myeloma cells. Together, these findings indicate that targeting sphingolipid metabolism via SK2 inhibition may be effective in combination with a broad spectrum of proteasome inhibitors in the proteasome inhibitor resistant setting, and is an approach worth clinical exploration.

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