CGEN-15001, a Novel B7-like Protein, Controls Inflammation in a Translational Rheumatoid Arthritis (RA) Assay and Induces Treg Driven Long-Term Remission in an Autoimmune Disease Model

Iris Hecht¹, Ashley Gilmour², Clare Tange², Donna McIntyre², Joseph R. Podojil³, Kay McNamee⁴, Galit Rotman⁵, Eyal Neria⁵, Mariola Kurowska-Stolarska², Richard O. Williams⁴, Stephen D. Miller³ and Iain B. McInnes^2,6, ¹Therapeutic Proteins, Compugen Ltd., Tel Aviv, Israel, ²Institute of Infection, Immunity and Inflammation, College of Medical, Veterinary and Life Sciences, University of Glasgow, Glasgow, United Kingdom, ³Microbiology-Immunology, Northwestern University, Chicago, IL, ⁴Kennedy Institute of Rheumatology, University of Oxford, Oxford, United Kingdom, ⁵Compugen Ltd., Tel Aviv, Israel, ⁶Institute of Infection, Immunity and Inflammation, College of Medicine, Veterinary Medicine and Life Sciences, University of Glasgow, Glasgow, United Kingdom

Meeting: 2015 ACR/ARHP Annual Meeting

Date of first publication: September 29, 2015

Keywords: co-stimulation, cytokines, T-Regulatory Cells, therapeutic targeting and tolerance

Session Information

Date: Sunday, November 8, 2015

Title: Cytokines, Mediators, Cell-cell Adhesion, Cell Trafficking and Angiogenesis

Session Type: ACR Concurrent Abstract Session

Session Time: 2:30PM-4:00PM

Background/Purpose:

CGEN-15001 is an Fc fusion protein composed of the extracellular domain of a novel B7-like protein. Therapeutic CGEN-15001 treatment is effective in collagen induced arthritis and potentially re-establishes immune tolerance. This is supported by long lasting efficacy in autoimmune disease models, and by establishment of tolerance to donor graft in a bone marrow transplantation model. CGEN-15001 inhibits T cell activation and induces Th1/Th17 to Th2 shift, IL-10 secretion and regulatory T cell (Treg) differentiation.

As Tregs have key role in tolerance, their involvement in the effects of CGEN-15001 was studied in the EAE (experimental autoimmune encephalomyelitis) model of multiple sclerosis by blocking IL-10 or TGFβ which play critical roles in Treg differentiation, or upon transient Treg inactivation by anti-CD25.

The therapeutic potential of CGEN-15001 for RA was studied in co-cultures of cytokine activated T cells (TcK) and macrophages (Mϕ) from RA patients and healthy donors. Such co-cultures mimic the interaction of cells in RA synovium that lead to aberrant cytokine production and provide a translational tool to evaluate potential therapies.

Methods:

CD4+ T cells and monocytes were isolated from healthy donors or RA patients’ blood and cultured for 6 days with TNFα, IL-6 and IL-15 to induce TcK or with M-CSF to induce Mϕ differentiation, respectively. Autologous TcK and Mϕ were co-cultured in the presence of CGEN-15001 or controls for 24hrs. Cytokines were evaluated by luminex.

EAE was induced in SJL mice primed with PLP_139-151in CFA. Mice were treated from onset of remission, 3 times/week for 2 weeks. Anti-IL-10 or anti-TGFβ were injected concomitantly with CGEN-15001. Alternatively, 2 injections of anti-CD25 were given 2 days before treatment with CGEN-15001 or 2 weeks after last treatment. Disease severity was followed.

Results:

In synovial-like Mϕ: TcK co-cultures, CGEN-15001 abrogated secretion of pro-inflammatory cytokines including TNFα, IL-17, IFNγ, GM-CSF, RANTES and MIP-1α. Similarly, inhibition in TNFα secretion was observed in co-cultures from RA patients’ cells.

In EAE, durable remission was induced by a short course of therapeutic treatment. This effect was abrogated by concomitant treatment with anti-TGFb or anti-IL-10, demonstrating a central role for Treg supporting pathways in the therapeutic effects of CGEN-15001. Transient inactivation of Tregs by anti-CD25 before CGEN-15001 treatment did not affect the durable remission achieved by CGEN-15001, however, administration of anti-CD25 2 weeks after the last treatment resulted in transient disease relapse, suggesting that Treg functionality is crucial for the durable effects of CGEN-15001, while at early stages Th1/Th17 to Th2 skew may control the disease.

Conclusion:

The anti-inflammatory activity of CGEN-15001 in a translational assay mimicking RA synovium supports its therapeutic potential in RA. The long remission maintained by active Tregs in the EAE model supports a novel mechanism of re-establishing tolerance to autoantigens. Therefore, these results support the therapeutic potential of CGEN-15001 to reduce inflammation and maintain long-term remission in autoimmune diseases and RA in particular.

Disclosure: I. Hecht, Compugen Ltd., 3; A. Gilmour, None; C. Tange, None; D. McIntyre, ; J. R. Podojil, Compugen, 2; K. McNamee, None; G. Rotman, Compugen, 3; E. Neria, Compugen, 3; M. Kurowska-Stolarska, Compugen, 2; R. O. Williams, None; S. D. Miller, Compugen, 2; I. B. McInnes, Compugen, 2.

To cite this abstract in AMA style:

Hecht I, Gilmour A, Tange C, McIntyre D, Podojil JR, McNamee K, Rotman G, Neria E, Kurowska-Stolarska M, Williams RO, Miller SD, McInnes IB. CGEN-15001, a Novel B7-like Protein, Controls Inflammation in a Translational Rheumatoid Arthritis (RA) Assay and Induces Treg Driven Long-Term Remission in an Autoimmune Disease Model [abstract]. Arthritis Rheumatol. 2015; 67 (suppl 10). https://acrabstracts.org/abstract/cgen-15001-a-novel-b7-like-protein-controls-inflammation-in-a-translational-rheumatoid-arthritis-ra-assay-and-induces-treg-driven-long-term-remission-in-an-autoimmune-disease-model/. Accessed .

« Back to 2015 ACR/ARHP Annual Meeting

ACR Meeting Abstracts - https://acrabstracts.org/abstract/cgen-15001-a-novel-b7-like-protein-controls-inflammation-in-a-translational-rheumatoid-arthritis-ra-assay-and-induces-treg-driven-long-term-remission-in-an-autoimmune-disease-model/