Litcius/Paper detail

Asymmetric cell division safeguards memory CD8 T cell development

Fabienne Gräbnitz, Dominique Stark, Danielle Shlesinger, Anthony Petkidis, Mariana Borsa, Alexander Yermanos, Andreas Carr, Niculò Barandun, Arne Wehling, Miroslav Baláž, Timm Schroeder, Annette Oxenius

2023Cell Reports28 citationsDOIOpen Access PDF

Abstract

The strength of T cell receptor (TCR) stimulation and asymmetric distribution of fate determinants are both implied to affect T cell differentiation. Here, we uncover asymmetric cell division (ACD) as a safeguard mechanism for memory CD8 T cell generation specifically upon strong TCR stimulation. Using live imaging approaches, we find that strong TCR stimulation induces elevated ACD rates, and subsequent single-cell-derived colonies comprise both effector and memory precursor cells. The abundance of memory precursor cells emerging from a single activated T cell positively correlates with first mitosis ACD. Accordingly, preventing ACD by inhibition of protein kinase Cζ (PKCζ) during the first mitosis upon strong TCR stimulation markedly curtails the formation of memory precursor cells. Conversely, no effect of ACD on fate commitment is observed upon weak TCR stimulation. Our data provide relevant mechanistic insights into the role of ACD for CD8 T cell fate regulation upon different activation conditions.

Topics & Concepts

Cell biologyT-cell receptorCell divisionMitosisBiologyStimulationT cellCD8Cytotoxic T cellMemory T cellCellCell growthCell fate determinationNeuroscienceImmunologyImmune systemBiochemistryTranscription factorIn vitroGeneImmune Cell Function and InteractionT-cell and B-cell ImmunologyCAR-T cell therapy research