EBioMedicine (Nov 2016)

Ubiquitin-specific Protease-7 Inhibition Impairs Tip60-dependent Foxp3+ T-regulatory Cell Function and Promotes Antitumor Immunity

  • Liqing Wang,
  • Suresh Kumar,
  • Satinder Dahiya,
  • Feng Wang,
  • Jian Wu,
  • Kheng Newick,
  • Rongxiang Han,
  • Arabinda Samanta,
  • Ulf H. Beier,
  • Tatiana Akimova,
  • Tricia R. Bhatti,
  • Benjamin Nicholson,
  • Mathew P. Kodrasov,
  • Saket Agarwal,
  • David E. Sterner,
  • Wei Gu,
  • Joseph Weinstock,
  • Tauseef R. Butt,
  • Steven M. Albelda,
  • Wayne W. Hancock

DOI
https://doi.org/10.1016/j.ebiom.2016.10.018
Journal volume & issue
Vol. 13, no. C
pp. 99 – 112

Abstract

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Foxp3+ T-regulatory (Treg) cells are known to suppress protective host immune responses to a wide variety of solid tumors, but their therapeutic targeting is largely restricted to their transient depletion or “secondary” modulation, e.g. using anti-CTLA-4 monoclonal antibody. Our ongoing studies of the post-translational modifications that regulate Foxp3 demonstrated that the histone/protein acetyltransferase, Tip60, plays a dominant role in promoting acetylation, dimerization and function in Treg cells. We now show that the ubiquitin-specific protease, Usp7, controls Treg function largely by stabilizing the expression and promoting the multimerization of Tip60 and Foxp3. Genetic or pharmacologic targeting of Usp7 impairs Foxp3+ Treg suppressive functions, while conventional T cell responses remain intact. As a result, pharmacologic inhibitors of Usp7 can limit tumor growth in immunocompetent mice, and promote the efficacy of antitumor vaccines and immune checkpoint therapy with anti-PD1 monoclonal antibody in murine models. Hence, pharmacologic therapy with Usp7 inhibitors may have an important role in future cancer immunotherapy.

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