| Literature DB >> 28239678 |
Brittany Shonts1, Sai-Ping Lau1, Julien Zuber1,2, Aleksandar Obradovic1, Jianing Fu1,2, Suxiao Yang1,2, Marion Lambert3, Shana Coley1,4, Joshua Weiner1,5, Joseph Thome1,6, Susan DeWolf1,2, Donna L Farber1,5,6, Yufeng Shen7, Sophie Caillat-Zucman3, Govind Bhagat4, Adam Griesemer1,5, Mercedes Martinez8, Tomoaki Kato5, Megan Sykes1,5,6,2.
Abstract
A paradigm in transplantation states that graft-infiltrating T cells are largely non-alloreactive "bystander" cells. However, the origin and specificity of allograft T cells over time has not been investigated in detail in animals or humans. Here, we use polychromatic flow cytometry and high throughput TCR sequencing of serial biopsies to show that gut-resident T cell turnover kinetics in human intestinal allografts are correlated with the balance between intra-graft host-vs-graft (HvG) and graft-vs-host (GvH) reactivities and with clinical outcomes. In the absence of rejection, donor T cells were enriched for GvH-reactive clones that persisted long-term in the graft. Early expansion of GvH clones in the graft correlated with rapid replacement of donor APCs by the recipient. Rejection was associated with transient infiltration by blood-like recipient CD28+ NKG2DHi CD8+ alpha beta T cells, marked predominance of HvG clones, and accelerated T cell turnover in the graft. Ultimately, these recipient T cells acquired a steady state tissue-resident phenotype, but regained CD28 expression during rejections. Increased ratios of GvH to HvG clones were seen in non-rejectors, potentially mitigating the constant threat of rejection posed by HvG clones persisting within the tissue-resident graft T cell population.Entities:
Year: 2016 PMID: 28239678 PMCID: PMC5323244 DOI: 10.1126/sciimmunol.aah3732
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468