OncoImmunology (Dec 2022)

Differential expression of CCR8 in tumors versus normal tissue allows specific depletion of tumor-infiltrating T regulatory cells by GS-1811, a novel Fc-optimized anti-CCR8 antibody

  • Jessica D. Weaver,
  • Edward C. Stack,
  • Joshua A. Buggé,
  • Changyun Hu,
  • Lara McGrath,
  • Amy Mueller,
  • Masie Wong,
  • Boris Klebanov,
  • Tanzila Rahman,
  • Rosemary Kaufman,
  • Christine Fregeau,
  • Vikki Spaulding,
  • Michelle Priess,
  • Kristen Legendre,
  • Sarah Jaffe,
  • Dhruvkumar Upadhyay,
  • Anirudh Singh,
  • Chang-Ai Xu,
  • Kristin Krukenberg,
  • Yan Zhang,
  • Yassine Ezzyat,
  • Dorothée Saddier Axe,
  • Michelle R. Kuhne,
  • Michael A. Meehl,
  • Donald R. Shaffer,
  • Brian M. Weist,
  • Dmitri Wiederschain,
  • Fabien Depis,
  • Monica Gostissa

DOI
https://doi.org/10.1080/2162402X.2022.2141007
Journal volume & issue
Vol. 11, no. 1

Abstract

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The presence of T regulatory (Treg) cells in the tumor microenvironment is associated with poor prognosis and resistance to therapies aimed at reactivating anti-tumor immune responses. Therefore, depletion of tumor-infiltrating Tregs is a potential approach to overcome resistance to immunotherapy. However, identifying Treg-specific targets to drive such selective depletion is challenging. CCR8 has recently emerged as one of these potential targets. Here, we describe GS-1811, a novel therapeutic monoclonal antibody that specifically binds to human CCR8 and is designed to selectively deplete tumor-infiltrating Tregs. We validate previous findings showing restricted expression of CCR8 on tumor Tregs, and precisely quantify CCR8 receptor densities on tumor and normal tissue T cell subsets, demonstrating a window for selective depletion of Tregs in the tumor. Importantly, we show that GS-1811 depleting activity is limited to cells expressing CCR8 at levels comparable to tumor-infiltrating Tregs. Targeting CCR8 in mouse tumor models results in robust anti-tumor efficacy, which is dependent on Treg depleting activity, and synergizes with PD-1 inhibition to promote anti-tumor responses in PD-1 resistant models. Our data support clinical development of GS-1811 to target CCR8 in cancer and drive tumor Treg depletion in order to promote anti-tumor immunity.

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