Loering Svenja, Cameron Guy J M, Bhatt Nirmal P, Belz Gabrielle T, Foster Paul S, Hansbro Philip M, Starkey Malcolm R
Priority Research Centre's GrowUpWell and Healthy Lungs, School of Biomedical Sciences and Pharmacy, Faculty of Health and Medicine, The University of Newcastle and Hunter Medical Research Institute, Newcastle, NSW, Australia.
The University of Queensland Diamantina Institute, Faculty of Medicine, The University of Queensland Translational Research Institute, Woolloongabba, QLD, Australia.
Immunol Cell Biol. 2021 May;99(5):542-551. doi: 10.1111/imcb.12430. Epub 2021 Jan 13.
Innate lymphoid cells (ILCs) are resident in the lung and are involved in both the maintenance of homeostasis and the pathogenesis of respiratory diseases. In this study, murine lung ILCs were characterized using flow cytometry and the impact of mouse age, sex and strain were assessed. Lung ILCs were found as early as postnatal day 4 and numbers peaked at 2 weeks, and then decreased as the lung matured. During postnatal lung development, ILC expressed differential amounts of group 2 ILC (ILC2)-associated cell surface antigens including ST2, CD90.2 and ICOS. Using Il5 Il13 dual reporter mice, neonates were found to have increased constitutive interleukin (IL)-13 expression compared with adult mice. Neonates and adults had similar ratios of IL-5 CD45 leukocytes; however, these cells were mostly composed of ILCs in neonates and T cells in adults. Sex-specific differences in ILC numbers were also observed, with females having greater numbers of lung ILCs than males in both neonatal and adult mice. Female lung ILCs also expressed higher levels of ICOS and decreased KLRG1. Mouse strain also impacted on lung ILCs with BALB/c mice having more ILCs in the lung and increased expression of ST2 and ICOS compared with C57BL/6J mice. Collectively, these data show that lung ILC numbers, cell surface antigen expression, IL-5 and IL-13 levels differed between neonatal and adult lung ILCs. In addition, cell surface antigens commonly used for ILC2 quantification, such as ST2, CD90.2 and ICOS, differ depending on age, sex and strain and these are important considerations for consistent universal identification of lung ILC2s.
固有淋巴细胞(ILC)存在于肺中,参与体内稳态的维持和呼吸系统疾病的发病机制。在本研究中,使用流式细胞术对小鼠肺ILC进行了表征,并评估了小鼠年龄、性别和品系的影响。早在出生后第4天就发现了肺ILC,其数量在2周时达到峰值,然后随着肺的成熟而减少。在出生后肺发育过程中,ILC表达了不同数量的2型ILC(ILC2)相关细胞表面抗原,包括ST2、CD90.2和ICOS。使用Il5 Il13双报告基因小鼠,发现与成年小鼠相比,新生小鼠的组成性白细胞介素(IL)-13表达增加。新生小鼠和成年小鼠的IL-5 CD45白细胞比例相似;然而,这些细胞在新生小鼠中主要由ILC组成,在成年小鼠中主要由T细胞组成。还观察到ILC数量的性别特异性差异,在新生小鼠和成年小鼠中,雌性肺ILC的数量均多于雄性。雌性肺ILC还表达更高水平的ICOS,而KLRG1表达降低。小鼠品系也对肺ILC有影响,与C57BL/6J小鼠相比,BALB/c小鼠肺中的ILC更多,ST2和ICOS的表达增加。总体而言,这些数据表明,新生小鼠和成年小鼠肺ILC在数量、细胞表面抗原表达、IL-5和IL-13水平上存在差异。此外,常用于定量ILC2的细胞表面抗原,如ST2、CD90.2和ICOS,因年龄、性别和品系而异,这些是一致普遍鉴定肺ILC2的重要考虑因素。
