Multimodal single-cell protein and RNA profiling unveils dysregulated immature neutrophil dynamics in gestational diabetes mellitus.

多模态单细胞蛋白质和 RNA 分析揭示了妊娠糖尿病中未成熟中性粒细胞动力学的失调。

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Neutrophils are the most abundant leukocytes in human peripheral blood, yet their heterogeneity in pregnancy, especially in gestational diabetes mellitus (GDM), remains incompletely understood. Here, we employed InfinityFlow-based surface marker profiling and single-cell RNA sequencing (scRNA-seq) to delineate neutrophil subsets in healthy and GDM pregnancies. We identified a low-density, immature subgroup (CD10⁻CD49d⁺Ig κ⁺) with distinctive morphology and transcriptomic profiles, contrasted against the CD10⁺ segmented mature neutrophils. In healthy pregnancy, these immature low-density neutrophils (LDNs) expanded by mid-gestation, elevating the immature-to-mature (I-M) neutrophil ratio and circulating myeloid progenitor levels throughout gestation. In GDM, this expansion was markedly blunted, with a consistently lower abundance of immature LDNs and progenitors. Flow cytometry and correlation analyses further linked the lower I-M ratio to impaired insulin sensitivity, underscoring a potential immune-metabolic axis in GDM. Collectively, our study provides a framework for neutrophil phenotyping in pregnancy and links disrupted neutrophil equilibrium and pregnancy complications.

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