Fcγ receptor–mediated cross-linking codefines the immunostimulatory activity of anti-human CD96 antibodies
Anne Rogel, … , Emma V. King, Aymen Al-Shamkhani
Anne Rogel, … , Emma V. King, Aymen Al-Shamkhani
Published August 23, 2022
Citation Information: JCI Insight. 2022;7(19):e158444. https://doi.org/10.1172/jci.insight.158444.
View: Text | PDF
Research Article Immunology

Fcγ receptor–mediated cross-linking codefines the immunostimulatory activity of anti-human CD96 antibodies

Abstract

New strategies that augment T cell responses are required to broaden the therapeutic arsenal against cancer. CD96, TIGIT, and CD226 are receptors that bind to a communal ligand, CD155, and transduce either inhibitory or activating signals. The function of TIGIT and CD226 is established, whereas the role of CD96 remains ambiguous. Using a panel of engineered antibodies, we discovered that the T cell stimulatory activity of anti-CD96 antibodies requires antibody cross-linking and is potentiated by Fcγ receptors. Thus, soluble “Fc silent” anti-CD96 antibodies failed to stimulate human T cells, whereas the same antibodies were stimulatory after coating onto plastic surfaces. Remarkably, the activity of soluble anti-CD96 antibodies was reinstated by engineering the Fc domain to a human IgG1 isotype, and it was dependent on antibody trans-cross-linking by FcγRI. In contrast, neither human IgG2 nor variants with increased Fcγ receptor IIB binding possessed stimulatory activity. Anti-CD96 antibodies acted directly on T cells and augmented gene expression networks associated with T cell activation, leading to proliferation, cytokine secretion, and resistance to Treg suppression. Furthermore, CD96 expression correlated with survival in HPV+ head and neck squamous cell carcinoma, and its cross-linking activated tumor-infiltrating T cells, thus highlighting the potential of anti-CD96 antibodies in cancer immunotherapy.

Authors

Anne Rogel, Fathima M. Ibrahim, Stephen M. Thirdborough, Florence Renart-Depontieu, Charles N. Birts, Sarah L. Buchan, Xavier Preville, Emma V. King, Aymen Al-Shamkhani

×

Figure 5

Antibody targeting of human CD96 can overcome Treg suppression.

Options: View larger image (or click on image) Download as PowerPoint
Antibody targeting of human CD96 can overcome Treg suppression. (A) The ...
(A) The expression of CD96 on CD8+ T cells, conventional CD4+ T cells (CD25lo CD127hi), and Tregs (CD25hi CD127lo) was analyzed by flow cytometry in PBMCs from HDs. Data show 1 representative example of 8 HDs. (B–E) CFSE-stained Treg-depleted CD3+ T (Tconv) cells were stimulated for 4 days with plate-bound OKT3 and plate-bound anti-CD96 huG1 antibody (clone 19-134) or a matching IC, either alone or in the presence of purified unlabeled Tregs. (B and C) Representative examples of (B) CFSE dilution and (C) CD25 expression in CFSE+ CD8+ and CFSE+ CD4+ Tconv cells. (D and E) Data show the mean ± SEM of the frequency of (D) dividing cells and (E) CD25+ cells in the CFSE+CD4+ and the CFSE+CD8+ Tconv cell populations, with each symbol representing the mean of triplicate wells for an individual HD. Data are combined from 2 independent experiments. *P ≤ 0.05, **P ≤ 0.01. Two-way ANOVA.