Incorporation of Immune Checkpoint Blockade into Chimeric Antigen Receptor T Cells (CAR-Ts): Combination or Built-In CAR-T

Jan 25, 2018International journal of molecular sciences

Adding Immune Checkpoint Blockers to CAR-T Cells: Combined Treatment or Built-In Design

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Abstract

CAR T cell therapy is the first FDA-approved gene therapy demonstrating high efficacy in treating refractory CD19 positive blood cancers.

  • The application of CAR T cells to solid tumors shows mixed results due to mechanisms that suppress local immune responses.
  • Modulating the immunosuppressive environment of tumors with immune-checkpoint blockade could enhance the effectiveness of CAR T cells.
  • The effects of combining CAR T cells with immune-checkpoint blockade in blood cancers are still being explored.
  • This review focuses on the potential synergy between CAR T cells and immune-checkpoint blockade.

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Key numbers

70–94%
Complete Remission Rate
Achieved in refractory B-ALL with CD19-specific CAR-T cells.
3 of 6
Clinical Responses
Patients treated with pembrolizumab alongside CD19-specific CAR-T cells.

Full Text

What this is

  • This review discusses the integration of immune checkpoint blockade with chimeric antigen receptor T cell (CAR-T) therapy.
  • CAR-T cells have shown efficacy in treating hematologic malignancies, but their effectiveness in solid tumors is limited.
  • The potential synergy between CAR-T therapy and immune checkpoint inhibitors is explored, particularly in overcoming tumor-induced immune suppression.

Essence

  • Combining immune checkpoint blockade with CAR-T therapy may enhance the treatment of hematological malignancies and solid tumors. This review evaluates current strategies and clinical evidence supporting this approach.

Key takeaways

  • CAR-T cells have achieved complete remission (CR) rates of 70–94% in refractory B-ALL. This high efficacy contrasts sharply with conventional therapies, where only 8% achieved CR.
  • In a combination approach, six pediatric B-ALL patients treated with pembrolizumab alongside CD19-specific CAR-T cells showed clinical responses, with three patients exhibiting prolonged CAR-T cell persistence.
  • Preclinical models indicate that PD-1 blockade can significantly enhance CAR-T cell activity, leading to increased tumor cell death and improved therapeutic outcomes.

Caveats

  • The effectiveness of immune checkpoint blockade in solid tumors remains uncertain, as some trials have shown modest benefits. Optimal dosing and scheduling of PD-1 blockade are still under investigation.
  • Potential toxicities, such as cytokine release syndrome (CRS) and neurological damage, may arise from combining CAR-T therapy with immune checkpoint inhibitors, necessitating careful monitoring.

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