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Manipulation of B-cell responses with histone deacetylase inhibitors

Author

Listed:
  • Michaela Waibel

    (Cancer Therapeutics Program, Peter MacCallum Cancer Centre
    The University of Melbourne)

  • Ailsa J. Christiansen

    (Cancer Therapeutics Program, Peter MacCallum Cancer Centre
    The University of Melbourne)

  • Margaret L. Hibbs

    (Leukocyte Signaling Laboratory, Monash University, Level 6 Burnet Institute)

  • Jake Shortt

    (Cancer Therapeutics Program, Peter MacCallum Cancer Centre
    The University of Melbourne
    Monash University School of Clinical Sciences, Monash Medical Centre
    Monash Medical Centre)

  • Sarah A. Jones

    (Monash University School of Clinical Sciences, Monash Medical Centre)

  • Ian Simpson

    (Monash Medical Centre)

  • Amanda Light

    (The Walter and Eliza Hall Institute of Medical Research)

  • Kristy O’Donnell

    (The Walter and Eliza Hall Institute of Medical Research)

  • Eric F. Morand

    (Monash University School of Clinical Sciences, Monash Medical Centre)

  • David M. Tarlinton

    (The Walter and Eliza Hall Institute of Medical Research)

  • Ricky W. Johnstone

    (Cancer Therapeutics Program, Peter MacCallum Cancer Centre
    The University of Melbourne)

  • Edwin D. Hawkins

    (Cancer Therapeutics Program, Peter MacCallum Cancer Centre
    The University of Melbourne
    Present address: Imperial College London, Sir Alexander Fleming Building, London SW72AZ, UK)

Abstract

Histone deacetylase inhibitors (HDACi) are approved for treating certain haematological malignancies, however, recent evidence also illustrates they are modulators of the immune system. In experimental models, HDACi are particularly potent against malignancies originating from the B-lymphocyte lineage. Here we examine the ability of this class of compounds to modify both protective and autoimmune antibody responses. In vitro, HDACi affect B-cell proliferation, survival and differentiation in an HDAC-class-dependent manner. Strikingly, treatment of lupus-prone Mrl/lpr mice with the HDACi panobinostat significantly reduces autoreactive plasma-cell numbers, autoantibodies and nephritis, while other immune parameters remain largely unaffected. Immunized control mice treated with panobinostat or the clinically approved HDACi vorinostat have significantly impaired primary antibody responses, but these treatments surprisingly spare circulating memory B cells. These studies indicate that panobinostat is a potential therapy for B-cell-driven autoimmune conditions and HDACi do not induce major long-term detrimental effects on B-cell memory.

Suggested Citation

  • Michaela Waibel & Ailsa J. Christiansen & Margaret L. Hibbs & Jake Shortt & Sarah A. Jones & Ian Simpson & Amanda Light & Kristy O’Donnell & Eric F. Morand & David M. Tarlinton & Ricky W. Johnstone & , 2015. "Manipulation of B-cell responses with histone deacetylase inhibitors," Nature Communications, Nature, vol. 6(1), pages 1-12, November.
    • Handle: RePEc:nat:natcom:v:6:y:2015:i:1:d:10.1038_ncomms7838
    DOI: 10.1038/ncomms7838
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