| Literature DB >> 33903232 |
Kartika Padhan1, Eirini Moysi1, Alessandra Noto2, Alexander Chassiakos1, Khader Ghneim3, Maria Maddalena Perra2, Sanjana Shah4, Vasilis Papaioannou1, Giulia Fabozzi1, David R Ambrozak5, Antigoni Poultsidi6, Maria Ioannou6, Craig Fenwick2, Samuel Darko4, Daniel C Douek4, Rafick-Pierre Sekaly3, Giuseppe Pantaleo2, Richard A Koup5, Constantinos Petrovas7.
Abstract
The development of follicular helper CD4 T (TFH) cells is a dynamic process resulting in a heterogenous pool of TFH subsets. However, the cellular and molecular determinants of this heterogeneity and the possible mechanistic links between them is not clear. We found that human TFH differentiation is associated with significant changes in phenotypic, chemokine, functional, metabolic and transcriptional profile. Furthermore, this differentiation was associated with distinct positioning to follicular proliferating B cells. Single-cell T cell receptor (TCR) clonotype analysis indicated the transitioning toward PD-1hiCD57hi phenotype. Furthermore, the differentiation of TFH cells was associated with significant reduction in TCR level and drastic changes in immunological synapse formation. TFH synapse lacks a tight cSMAC (central supra molecular activation Cluster) but displays the TCR in peripheral microclusters, which are potentially advantageous in the ability of germinal center (GC) B cells to receive necessary help. Our data reveal significant aspects of human TFH heterogeneity and suggest that the PD-1hiCD57hi TFH cells, in particular, are endowed with distinctive programming and spatial positioning for optimal GC B cell help.Entities:
Keywords: TCR microclusters; TFH cell heterogeneity; immunological synapse
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Year: 2021 PMID: 33903232 PMCID: PMC8106351 DOI: 10.1073/pnas.2016855118
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205