Abstract
AbstractIn 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 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) biopsyconfirmed acute rejection. The results of these studies highlight, for the first time, 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 TCRs. In conclusion, further prospective validation studies are needed to evaluate the clinical utility of peripheral blood TCR analysis for both pre- and post-transplant immune risk assessment and prediction of different mechanisms of graft rejection.
Publisher
Cold Spring Harbor Laboratory