1. Perturbations of the T-cell immune repertoire in kidney transplant rejection.
- Author
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Sigdel, Tara K, Sigdel, Tara K, Fields, Paul A, Liberto, Juliane, Damm, Izabella, Kerwin, Maggie, Hood, Jill, Towfighi, Parhom, Sirota, Marina, Robins, Harlan S, Sarwal, Minnie M, Sigdel, Tara K, Sigdel, Tara K, Fields, Paul A, Liberto, Juliane, Damm, Izabella, Kerwin, Maggie, Hood, Jill, Towfighi, Parhom, Sirota, Marina, Robins, Harlan S, and Sarwal, Minnie M
- Abstract
In this cross-sectional and longitudinal analysis of mapping the T-cell repertoire in kidney transplant recipients, we have investigated and validated T-cell clonality, immune repertoire chronology at rejection, and contemporaneous allograft biopsy quantitative tissue injury, to better understand the pathobiology of acute T-cell fraction, T-cell repertoire and antibody-mediated kidney transplant rejection. To follow the dynamic evolution of T-cell repertoire changes before and after engraftment and during biopsy-confirmed acute rejection, we sequenced 323 peripheral blood samples from 200 unique kidney transplant recipients, with (n=100) and without (n=100) biopsy-confirmed acute rejection. We report that patients who develop acute allograft rejection, have lower (p=0.01) T-cell fraction even before transplantation, followed by its rise after transplantation and at the time of acute rejection accompanied by high TCR repertoire turnover (p=0.004). Acute rejection episodes occurring after the first 6 months post-transplantation, and those with a component of antibody-mediated rejection, had the highest turnover; p=0.0016) of their T-cell repertoire. In conclusion, we validated that detecting repertoire changes in kidney transplantation correlates with post-transplant rejection episodes suggesting that T-cell receptor sequencing may provide recipient pre-transplant and post-transplant predictors of rejection risk.
- Published
- 2022