生物
自然杀伤细胞
细胞生物学
免疫学
子宫
免疫系统
螺旋动脉
细胞分化
淋巴细胞
细胞
受体
Janus激酶3
白细胞介素21
间质细胞
电池类型
淋巴因子激活杀伤细胞
胎儿
白细胞介素15
干细胞
白细胞介素12
细胞功能
蜕膜化
免疫耐受
功能(生物学)
细胞培养
胚胎干细胞
怀孕
子痫前期
细胞疗法
作者
Josselyn D Barahona,Liping Yang,D. Michael Nelson,Wayne M. Yokoyama
出处
期刊:
[Cold Spring Harbor Laboratory]
日期:2025-11-18
标识
DOI:10.1101/2025.11.18.688992
摘要
Abstract Tissue microenvironments shape lymphocyte differentiation to align immune function with local physiological demands. Uterine natural killer cells are critical for reproductive success, yet the molecular cues in the uterus that instruct their specialized identities remain incompletely understood. Here, we identify a TGF-β–dependent differentiation pathway by which circulating conventional NK cells convert into uterine tissue-resident NK cells during murine pregnancy. Loss of TGF-β receptor II expression in Ncr1 -expressing cells disrupted this conversion, markedly reducing tissue-resident NK cells in the gravid uterus. Impaired TGF-β–driven uterine tissue-resident NK cell differentiation during murine pregnancy led to abnormal spiral artery remodeling and increased fetal resorption rates at midgestation, ultimately reducing litter sizes at birth. Collectively, these findings define TGF-β as a pivotal driver of tissue-resident NK cell differentiation in the gravid uterus and establish a mechanistic framework through which the uterine microenvironment programs NK cell identity to meet the physiological demands of gestation.
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