Identification and function of a C3 hiIL-33 +fibroblast population in the lungs

Aishwarya Atakkatan, N. Gour, Aishwarya Magesh, H. Yong, S. Lajoie
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Abstract

Complement component C3 is known to be predominantly expressed by epithelial and immune cells, however, we have found that fibroblasts are a primary source of C3 in murine and human lungs. Specifically, C3 is majorly expressed in adventitial fibroblasts. Moreover, we found that C3 hifibroblasts are characterized by the expression of IL-33. Further, C3 and IL-33 are not only markers of a novel subset of pulmonary adventitial fibroblasts but form a functional axis where C3 drives the expression of IL-33. As compared to other adventitial fibroblasts, this C3 hiIL-33 +subset is enriched for matrix genes, especially type I collagen (COL1A1). These cells require a functional C3− IL-33 axis to maintain their matrix identity. Impairing C3 not only reduces their ability to make collagen but guides them towards a lipofibroblast program characterized by lower collagen content and higher lipid accumulation. As we and others have published that C3 is a key driver of allergic airway inflammation, we wanted to understand how exposure to allergen affected C3 hiIL-33 +fibroblasts. Using a murine model of airway allergy, we observed a significant increase in the C3 hiIL33 +fibroblast population in lung samples from house dust mite (HDM)-treated mice compared to the PBS control group. Recently, IL-33 +fibroblasts were found to support ILC2 recruitment during helminth infection. As we have found C3 is critical to maintain IL-33 in these cells, we aim to understand if C3 hiIL-33 +fibroblasts participate in allergy by mediating cellular crosstalk with ILC2s and T cells during type 2 immune responses. Supported by grants from NIH R01AI27644 and the Johns Hopkins Catalyst Award to Dr. Stephane Lajoie.
肺中C3 hiIL-33 +成纤维细胞群的鉴定和功能
补体成分C3已知主要由上皮细胞和免疫细胞表达,然而,我们发现成纤维细胞是小鼠和人肺中C3的主要来源。具体来说,C3主要表达于外层成纤维细胞中。此外,我们发现C3组织成纤维细胞以IL-33的表达为特征。此外,C3和IL-33不仅是肺外膜成纤维细胞新亚群的标志物,而且还形成了一个功能轴,其中C3驱动IL-33的表达。与其他外层成纤维细胞相比,这个C3 hiIL-33 +亚群富含基质基因,尤其是I型胶原(COL1A1)。这些细胞需要一个功能性的C3 - IL-33轴来维持它们的基质特性。损害C3不仅会降低它们制造胶原蛋白的能力,还会引导它们进入以胶原蛋白含量低和脂质积累高为特征的脂肪成纤维细胞程序。正如我们和其他人已经发表的C3是过敏性气道炎症的关键驱动因素,我们想了解暴露于过敏原如何影响C3 hiIL-33 +成纤维细胞。使用小鼠气道过敏模型,我们观察到与PBS对照组相比,屋尘螨(HDM)处理小鼠肺样本中C3 hiIL33 +成纤维细胞数量显着增加。最近,IL-33 +成纤维细胞被发现在蠕虫感染期间支持ILC2的募集。由于我们已经发现C3对于维持这些细胞中的IL-33至关重要,我们的目标是了解C3 hiIL-33 +成纤维细胞是否通过在2型免疫反应中介导ILC2s和T细胞的细胞串音参与过敏。由NIH R01AI27644和约翰霍普金斯催化剂奖Stephane Lajoie博士资助。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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