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Related Concept Videos

T Cell Activation and Clonal Selection01:22

T Cell Activation and Clonal Selection

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T cells are integral to our adaptive immune system, recognizing and effectively responding to foreign antigens. T cell activation and clonal selection are pivotal in orchestrating this immune response. This article elucidates these mechanisms, detailing the roles of cluster of differentiation (CD) markers, major histocompatibility complex (MHC) molecules, costimulatory signals, and the process of clonal selection.
Naive T cells that have not yet encountered an antigen express two primary CD...
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Diversity of Antigen Receptors01:28

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Antigen receptors are essential components of the immune system crucial in defending the body against foreign invaders. These receptors are present on the surface of B and T cells, enabling them to recognize antigens and mount an appropriate immune response.
Before encountering any antigen, lymphocytes express these receptors. On B cells, the antigen receptor is a membrane-bound antibody molecule called BCR; on T cells, it is a T cell receptor or TCR. B and T cell receptors are composed of two...
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A complementation test is a simple cross to identify whether the two mutations are located on the same gene or different genes. It was first performed by Edward Lewis in the 1940s while working on fruit flies. He developed the test to identify the location and arrangement of different mutations on chromosomes.
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Updated: Jul 19, 2025

In Vitro Tumor Cell Rechallenge For Predictive Evaluation of Chimeric Antigen Receptor T Cell Antitumor Function
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Complementarity-determining region clustering may cause CAR-T cell dysfunction.

Tina Sarén1, Giulia Saronio1, Paula Marti Torrell1

  • 1Uppsala University, Dept Immunology, Genetics, Pathology, Science for Life Laboratory, Uppsala, Sweden.

Nature Communications
|August 10, 2023
PubMed
Summary
This summary is machine-generated.

CAR-T cell therapy design is challenged by CDR loops causing CAR clustering. This leads to antigen-independent T cell activation and dysfunction, impacting cancer treatment efficacy.

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Area of Science:

  • Immunology
  • Cancer Biology
  • Biotechnology

Background:

  • Chimeric antigen receptor (CAR)-T cell therapy shows promise for cancer treatment.
  • Designing optimal CARs is complex, with single-chain variable fragments (scFvs) defining specificity via complementarity-determining regions (CDRs).

Purpose of the Study:

  • To investigate the impact of CDR loops on CAR clustering and T cell function.
  • To identify mechanisms of antigen-independent CAR-T cell activation and dysfunction.

Main Methods:

  • Engineered CARs with identical frameworks but varying CDR sequences.
  • Assessed CAR clustering on T cell surfaces.
  • Measured antigen-independent T cell activation markers (cell size, IFN-γ secretion).
  • Evaluated CAR-T cell exhaustion, cell death, and tumor cell responsiveness.

Main Results:

  • CDR loops were found to mediate CAR clustering on the T cell surface.
  • CAR clustering induced antigen-independent T cell activation, evidenced by increased cell size and IFN-γ secretion.
  • This tonic signaling resulted in CAR-T cell exhaustion, activation-induced cell death, and reduced anti-tumor activity.

Conclusions:

  • Antigen-independent tonic signaling can be triggered by CDR-mediated CAR clustering.
  • This phenomenon, not predictable from scFv sequences alone, impacts CAR-T cell efficacy.
  • Evaluating unstimulated CAR-T cell activity is crucial for predicting therapeutic outcomes.