Technology ID
TAB-5065

Enhanced Tumor Reactivity of T Cells Lacking SIT1, LAX1 or TRAT1

E-Numbers
E-004-2024-0
Lead Inventor
Love, Paul
Lead IC
NICHD
Co-Inventors
Dutta, Avik
ICs
NICHD
Applications
Therapeutics
Therapeutic Areas
Oncology
Immunology
Development Stages
Pre-clinical (in vivo)

Summary:

The Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) is actively seeking potential licensees interested in further developing these inhibitory transmembrane adapter proteins as targets for T-cell immunotherapy for the treatment of cancer, infectious diseases, and autoimmune diseases.

Description of Technology:

Cellular immunotherapy holds much promise for the treatment of cancer. However, certain cellular therapies have limited success because of immunosuppression in the tumor microenvironment. Thus, there is an unmet need for improved methods of cellular immunotherapy.

T cells constitutively express inhibitory molecules that limit the activation response to antigens by the T cell antigen receptor (TCR). Among these are the transmembrane adapter proteins SIT1, LAX 1 and TRA T1. These appear to tonically associate with the TCR and inhibit signal transduction. Researchers at the Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) have identified SIT1, LAX 1 and TRA T1 as potential targets for T-cell immunotherapy. Mouse models have demonstrated that deletion of SIT1, LAX1 and TRA T1 – or expression of nonfunctional mutant versions of these proteins in mouse T cells – enhances TCR signaling and significantly increases T cell cytotoxicity against tumor cells. Experiments confirming these results in human T cells are currently underway. This discovery provides a new therapeutic approach to greatly improve clinical outcomes of T-cell immunotherapy in treating cancers. It also holds potential to treat infectious diseases or autoimmune diseases

Potential Commercial Applications:

  • Treatment for cancer
  • Treatment for infectious diseases
  • Treatment for autoimmune diseases

Competitive Advantages:

  • Potentially superior therapeutic benefit in cancer by:
    • Enhancing tumoricidal activity of T-cell immunotherapy
    • Overcoming immunosuppression in the tumor microenvironment
  • Potentially superior therapeutic benefit in infectious diseases by enhancing immune responses to pathogens
  • Potentially superior therapeutic benefit in autoimmune disease by enhancing the generation or function of antigen-specific regulator T cells (Tregs)

Request More Info

Licensing Contact:
Girards, Richard
richard.girards@nih.gov

Collaboration Description

  • Researchers at the NICHD seek licensing for further developing these inhibitory transmembrane adapter proteins as targets for T-cell immunotherapy for the treatment of cancer, infectious diseases, and autoimmune diseases.
Date Published