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CD57(+) CD4 T Cells Underlie Belatacept-Resistant Allograft Rejection.


ABSTRACT: Belatacept is a B7-specific fusion protein used to prevent allograft rejection by blocking T cell costimulation. Generally efficacious, it fails to prevent acute rejection in a sizable minority of patients. In experimental models, memory T cells mediate costimulation blockade-resistant rejection (CoBRR), but this remains undefined in humans. To explore relationships between individual patients' immune cell phenotypes and CoBRR, we studied patients receiving belatacept or conventional calcineurin inhibitor-based immunosuppression. We identified a population of CD57(+) PD1(-) CD4 T cells present prior to transplantation that correlated with CoBRR. Contrary to data recognizing CD57 as a marker of senescence on CD8 T cells, we discovered a nonsenescent, cytolytic phenotype associated with CD57 on CD4 T cells. Moreover, CD57(+) CD4 T cells expressed high levels of adhesion molecules implicated in experimental CoBRR, were CD28(-) , expressed a transcriptional phenotype broadly defining allograft rejection and were shown to be present in rejecting human kidney allografts. These data implicate CD57(+) CD4 T cells in clinical CoBRR. If prospectively validated, this characteristic could identify patients at higher risk for acute rejection on belatacept-based therapy.

SUBMITTER: Espinosa J 

PROVIDER: S-EPMC4867077 | biostudies-literature | 2016 Apr

REPOSITORIES: biostudies-literature

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CD57(+) CD4 T Cells Underlie Belatacept-Resistant Allograft Rejection.

Espinosa J J   Herr F F   Tharp G G   Bosinger S S   Song M M   Farris A B AB   George R R   Cheeseman J J   Stempora L L   Townsend R R   Durrbach A A   Kirk A D AD  

American journal of transplantation : official journal of the American Society of Transplantation and the American Society of Transplant Surgeons 20160114 4


Belatacept is a B7-specific fusion protein used to prevent allograft rejection by blocking T cell costimulation. Generally efficacious, it fails to prevent acute rejection in a sizable minority of patients. In experimental models, memory T cells mediate costimulation blockade-resistant rejection (CoBRR), but this remains undefined in humans. To explore relationships between individual patients' immune cell phenotypes and CoBRR, we studied patients receiving belatacept or conventional calcineurin  ...[more]

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