Litcius/Paper detail

PD-1-stimulated T cell subsets are transcriptionally and functionally distinct

Shalom Lerrer, Anna S. Tocheva, Shoiab Bukhari, Kieran Adam, Adam Mor

2021iScience22 citationsDOIOpen Access PDF

Abstract

Despite the obvious inhibitory outcome of PD-1 signaling, an additional series of functions are activated. We have observed that T cells stimulated through the T cell receptor (TCR) and PD-1 primarily do not proliferate; however, there is a population of cells that proliferates more than through TCR stimulation alone. In this study, we performed flow cytometry and RNA sequencing on individual populations of T cells and discovered that unlike naive T cells, which were inhibited following PD-1 ligation, T cells that proliferated more following PD-1 ligation were associated with effector and central memory phenotypes. We showed that these populations had different gene expression profiles following PD-1 ligation with PD-L1 compared to PD-L2. The presence of transcriptionally and functionally distinct T cell populations responsive to PD-1 ligation provides new insights into the biology of PD-1 and suggest the use of T cell subset-specific approaches to improve the clinical outcome of PD-1 blockade.

Topics & Concepts

LigationT-cell receptorFlow cytometryBiologyT cellCell biologyEffectorPopulationCellMolecular biologyImmunologyChemistryGeneticsMedicineImmune systemEnvironmental healthCancer Immunotherapy and BiomarkersImmune Cell Function and InteractionCAR-T cell therapy research