Mahita Kadmiel , David Diaz-Jimenez , Robert H. Oakley , Maria G. Petrillo , Bo He , Xiaojiang Xu , John A. Cidlowski
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引用次数: 0
Abstract
The cornea protects the interior of the eye from external agents such as bacteria, viruses, and debris. Synthetic glucocorticoids are widely prescribed in the treatment of ocular infections and disorders. The actions of glucocorticoids are mediated by the glucocorticoid receptor (GR); however, the molecular and physiological functions of GR signaling in the cornea are poorly understood. This study found that treatment of mice with glucocorticoid eye drops led to a profound regulation of the corneal transcriptome. These glucocorticoid-regulated genes were associated with multiple biological functions, including the immune response. To understand the direct role of GR signaling in the cornea, mice with conditional knockout of GRs in the corneal epithelium were generated. Mice lacking corneal GRs exhibited microphthalmia, loss of pupils, a deformed and opaque lens, and mislocalization of key structural proteins within the corneal epithelial layers. Global transcriptomic approaches revealed that loss of GR signaling in the cornea also resulted in the dysregulation of a large cohort of genes strongly associated with an enhanced inflammatory response. Finally, corneal GR signaling was required for preventing neovascularization of blood and lymphatic vessels and thereby immune cell infiltration of the cornea. These results reveal that corneal GR signaling plays a critical role in ocular development and in maintaining the homeostasis of the eye.
角膜保护眼睛内部不受细菌、病毒和碎屑等外部物质的伤害。合成糖皮质激素被广泛用于治疗眼部感染和疾病。糖皮质激素的作用是由糖皮质激素受体(GR)介导的;然而,人们对 GR 信号在角膜中的分子和生理功能知之甚少。这项研究发现,用糖皮质激素滴眼液治疗小鼠会对角膜转录组产生深远的调节作用。这些受糖皮质激素调控的基因与多种生物功能有关,包括免疫反应。为了了解 GR 信号在角膜中的直接作用,研究人员在角膜上皮细胞中产生了条件性 GRs 基因敲除小鼠。缺乏角膜GRs的小鼠表现出小眼球症、瞳孔缩小、晶状体变形和不透明,以及角膜上皮层内关键结构蛋白的错位。全局转录组学方法显示,角膜中 GR 信号的缺失还导致与炎症反应增强密切相关的大量基因失调。最后,角膜 GR 信号对于防止血管和淋巴管新生以及免疫细胞浸润角膜是必需的。这些结果表明,角膜GR信号在眼球发育和维持眼球平衡方面起着关键作用。
期刊介绍:
The American Journal of Pathology, official journal of the American Society for Investigative Pathology, published by Elsevier, Inc., seeks high-quality original research reports, reviews, and commentaries related to the molecular and cellular basis of disease. The editors will consider basic, translational, and clinical investigations that directly address mechanisms of pathogenesis or provide a foundation for future mechanistic inquiries. Examples of such foundational investigations include data mining, identification of biomarkers, molecular pathology, and discovery research. Foundational studies that incorporate deep learning and artificial intelligence are also welcome. High priority is given to studies of human disease and relevant experimental models using molecular, cellular, and organismal approaches.