Quantifying T cell receptor mechanics at membrane junctions using DNA origami tension sensors.
Yuesong HuJhordan RogersYuxin DuanArventh VelusamySteven NarumSarah Al AbdullatifKhalid SalaitaPublished in: Nature nanotechnology (2024)
The T cell receptor (TCR) is thought to be a mechanosensor, meaning that it transmits mechanical force to its antigen and leverages the force to amplify the specificity and magnitude of TCR signalling. Although a variety of molecular probes have been proposed to quantify TCR mechanics, these probes are immobilized on hard substrates, and thus fail to reveal fluid TCR-antigen interactions in the physiological context of cell membranes. Here we developed DNA origami tension sensors (DOTS) which bear force sensors on a DNA origami breadboard and allow mapping of TCR mechanotransduction at dynamic intermembrane junctions. We quantified the mechanical forces at fluid TCR-antigen bonds and observed their dependence on cell state, antigen mobility, antigen potency, antigen height and F-actin activity. The programmability of DOTS allows us to tether these to microparticles to mechanically screen antigens in high throughput using flow cytometry. Additionally, DOTS were anchored onto live B cells, allowing quantification of TCR mechanics at immune cell-cell junctions.
Keyphrases
- single molecule
- regulatory t cells
- single cell
- high throughput
- living cells
- flow cytometry
- cell therapy
- dendritic cells
- fluorescent probe
- small molecule
- high resolution
- body mass index
- photodynamic therapy
- circulating tumor
- molecularly imprinted
- dna methylation
- bone marrow
- immune response
- stem cells
- physical activity
- genome wide
- nucleic acid
- solid phase extraction
- advanced cancer