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Single-cell transcriptomic analysis reveals heterogeneous features of myeloid-derived suppressor cells in newborns

Yao Meng, Yingjiao Cao, Juan He, Rui Dong, Gaoyu Liu, Yingying Chen, Jun Wang, Jie Zhou

2024Frontiers in Immunology11 citationsDOIOpen Access PDF

Abstract

The transitory emergence of myeloid-derived suppressor cells (MDSCs) in infants is important for the homeostasis of the immune system in early life. The composition and functional heterogeneity of MDSCs in newborns remain elusive, hampering the understanding of the importance of MDSCs in neonates. In this study, we unraveled the maturation trajectory of polymorphonuclear (PMN)-MDSCs from the peripheral blood of human newborns by performing single-cell RNA sequencing. Results indicated that neonatal PMN-MDSCs differentiated from self-renewal progenitors, antimicrobial PMN-MDSCs, and immunosuppressive PMN-MDSCs to late PMN-MDSCs with reduced antimicrobial capacity. We also established a simple framework to distinguish these distinct stages by CD177 and CXCR2. Importantly, preterm newborns displayed a reduced abundance of classical PMN-MDSCs but increased late PMN-MDSCs, consistent with their higher susceptibility to infections and inflammation. Furthermore, newborn PMN-MDSCs were distinct from those from cancer patients, which displayed minimum expression of genes about antimicrobial capacity. This study indicates that the heterogeneity of PMN-MDSCs is associated with the maturity of human newborns.

Topics & Concepts

Myeloid-derived Suppressor CellTranscriptomeSuppressorImmunologyImmune systemMyeloidBiologyInflammationCancerGeneGene expressionGeneticsImmune cells in cancerNeonatal Respiratory Health ResearchImmune Response and Inflammation