Aging profoundly affects immune-system function, promoting susceptibility to pathogens, cancers and chronic inflammation. We previously identified a population of IL-10-producing, T follicular helper-like cells (" "), linked to suppressed vaccine responses in aged mice. Here, we integrate single-cell ( )RNA-seq, scATAC-seq and genome-scale modeling to characterize Tfh10 - and the full CD4 memory T cell ( ) compartment - in young and old mice.
View Article and Find Full Text PDFRunx proteins (also known as Runt-domain transcription factors) have been studied for a long time as key regulators of cellular differentiation. RUNX2 has been described as essential for osteogenesis, whereas RUNX1 and RUNX3 are known to control blood cell development during different stages of cell lineage specification. However, recent studies show evidence of complex relationships between RUNX proteins, chromatin-modifying machinery, the cytoskeleton and different transcription factors in various non-embryonic contexts, including mature T cell homeostasis, inflammation and cancer.
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