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新生儿肝脏中存在自发出现的中性粒细胞群体,其具有与成人不同的独特空间和功能特征。

The neonatal liver hosts a spontaneously occurring neutrophil population, exhibiting distinct spatial and functional characteristics from adults.

机构信息

Center for Gastrointestinal Biology, Departamento de Morfologia, Instituto de Ciências Biológicas, Universidade Federal de Minas Gerais, Av. Pres. Antônio Carlos, 6627 - Pampulha, Belo Horizonte, Minas Gerais, 31270-901, Brazil.

Vascular Biology and Therapeutics Program, Department of Pathology, Yale University, 10 Amistad Street, PO Box 208089, New Haven, CT 06520, United States.

出版信息

J Leukoc Biol. 2024 Nov 27;116(6):1352-1363. doi: 10.1093/jleuko/qiae082.

Abstract

The elusive nature of the liver immune system in newborns remains an important challenge, casting a shadow over our understanding of how to effectively treat and prevent diseases in children. Therefore, deeper exploration into the intricacies of neonatal immunology might be crucial for improved pediatric healthcare. Using liver intravital microscopy, we unveiled a significant population of granulocytes in the hepatic parenchyma of fetuses and newborns. Utilizing high-dimensional immunophenotyping, we showed dynamic alterations predominantly in granulocytes during neonatal development. Liver intravital microscopy from birth through adulthood captures real-time dynamics, showing a substantial presence of Ly6G+ cells that persisted significantly up to 2 wk of age. Using time-of flight mass cytometry, we characterized neonatal Ly6G+ cells as neutrophils, confirmed by morphology and immunohistochemistry. Surprisingly, the embryonic liver hosts a distinct population of neutrophils established as early as the second gestational week, challenging conventional notions about their origin. Additionally, we observed that embryonic neutrophils occupy preferentially the extravascular space, indicating their early establishment within the liver. Hepatic neutrophils in embryos and neonates form unique cell clusters, persisting during the initial days of life, while reduced migratory capabilities in neonates are observed, potentially compensating with increased reactive oxygen species release in response to stimuli. Finally, in vivo imaging of acute neutrophil behavior in a newborn mouse, subjected to focal liver necrosis, unveils that neonatal neutrophils exhibit a reduced migratory response. The study provides unprecedented insights into the intricate interplay of neutrophils within the liver, shedding light on their functional and dynamic characteristics during development.

摘要

新生儿肝脏免疫系统的难以捉摸的性质仍然是一个重要的挑战,这使得我们对如何有效治疗和预防儿童疾病的理解蒙上了一层阴影。因此,深入探索新生儿免疫学的复杂性可能对改善儿科医疗保健至关重要。我们使用肝脏活体显微镜揭示了胎儿和新生儿肝实质中存在大量粒细胞。利用高维免疫表型分析,我们显示了在新生儿发育过程中粒细胞的动态变化。从出生到成年的肝脏活体显微镜捕捉到实时动态,显示出大量 Ly6G+细胞的存在,直到 2 周龄时仍显著存在。使用飞行时间质谱细胞术,我们将新生儿 Ly6G+细胞鉴定为中性粒细胞,这通过形态和免疫组织化学得到了证实。令人惊讶的是,胚胎肝脏中存在着一种独特的中性粒细胞群体,早在第二妊娠期就已建立,这挑战了传统的关于它们起源的观念。此外,我们观察到胚胎中性粒细胞优先占据血管外空间,表明它们在肝脏内的早期建立。胚胎和新生儿的肝脏中性粒细胞形成独特的细胞簇,在生命的最初几天持续存在,而在新生儿中观察到迁移能力降低,可能通过增加对刺激的反应性氧物种释放来补偿。最后,对新生小鼠局灶性肝坏死模型中急性中性粒细胞行为的体内成像揭示了新生儿中性粒细胞表现出迁移反应降低。该研究提供了关于中性粒细胞在肝脏内复杂相互作用的前所未有的见解,阐明了它们在发育过程中的功能和动态特征。

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