星形胶质细胞 STAT3 的激活和慢性瘙痒需要 IPR1/TRPC 依赖性 Ca 信号在小鼠中。
Astrocytic STAT3 activation and chronic itch require IPR1/TRPC-dependent Ca signals in mice.
机构信息
Department of Life Innovation, Graduate School of Pharmaceutical Sciences, Kyushu University, Fukuoka, Japan.
RIKEN Center for Biosystems Dynamics Research, Hyogo, Japan; Faculty of Science, Toho University, Chiba, Japan; Shanghai Institute of Immunochemical Studies, Shanghai Tech University, Shanghai, China.
出版信息
J Allergy Clin Immunol. 2021 Apr;147(4):1341-1353. doi: 10.1016/j.jaci.2020.06.039. Epub 2020 Aug 8.
BACKGROUND
Chronic itch is a debilitating symptom of inflammatory skin diseases, but the underlying mechanism is poorly understood. We have recently demonstrated that astrocytes in the spinal dorsal horn become reactive in models of atopic and contact dermatitis via activation of the transcription factor signal transducer and activator of transcription 3 (STAT3) and critically contribute to chronic itch. In general, STAT3 is transiently activated; however, STAT3 activation in reactive astrocytes of chronic itch model mice persistently occurs via an unknown mechanism.
OBJECTIVE
We aimed to determine the mechanisms of persistent activation of astrocytic STAT3 in chronic itch conditions.
METHODS
To determine the factors that are required for persistent activation of astrocytic STAT3, Western blotting and calcium imaging with cultured astrocytes or spinal cord slices were performed. Thereafter, chronic itch model mice were used for genetic and behavioral experiments to confirm the role of the factors determined to mediate persistent STAT3 activation from in vitro and ex vivo experiments in chronic itch.
RESULTS
IP receptor type 1 (IPR1) knockdown in astrocytes suppressed IL-6-induced persistent STAT3 activation and expression of lipocalin-2 (LCN2), an astrocytic STAT3-dependent inflammatory factor that is required for chronic itch. IPR1-dependent astrocytic Ca responses involved Ca influx through the cation channel transient receptor potential canonical (TRPC), which was required for persistent STAT3 activation evoked by IL-6. IL-6 expression was upregulated in dorsal root ganglion neurons in a mouse model of chronic itch. Dorsal root ganglion neuron-specific IL-6 knockdown, spinal astrocyte-specific IPR1 knockdown, and pharmacologic spinal TRPC inhibition attenuated LCN2 expression and chronic itch.
CONCLUSION
Our findings suggest that IPR1/TRPC channel-mediated Ca signals elicited by IL-6 in astrocytes are necessary for persistent STAT3 activation, LCN2 expression, and chronic itch, and they may also provide new targets for therapeutic intervention.
背景
慢性瘙痒是炎症性皮肤病的一种使人虚弱的症状,但潜在的机制尚未被很好地理解。我们最近的研究表明,在特应性皮炎和接触性皮炎模型中,脊髓背角中的星形胶质细胞通过转录因子信号转导和转录激活因子 3(STAT3)的激活而变得活跃,并对慢性瘙痒起关键作用。一般来说,STAT3 是短暂激活的;然而,慢性瘙痒模型小鼠的反应性星形胶质细胞中的 STAT3 激活通过未知机制持续发生。
目的
我们旨在确定慢性瘙痒条件下星形胶质细胞 STAT3 持续激活的机制。
方法
为了确定持续激活星形胶质细胞 STAT3 所需的因素,使用培养的星形胶质细胞或脊髓切片进行 Western blot 分析和钙成像。此后,使用慢性瘙痒模型小鼠进行遗传和行为学实验,以确认从体外和体内实验中确定的介导持续 STAT3 激活的因素在慢性瘙痒中的作用。
结果
星形胶质细胞中 IP 受体 1(IPR1)的敲低抑制了 IL-6 诱导的持续 STAT3 激活和脂联素-2(LCN2)的表达,LCN2 是星形胶质细胞 STAT3 依赖性炎症因子,是慢性瘙痒所必需的。IPR1 依赖性星形胶质细胞 Ca 反应涉及阳离子通道瞬时受体电位经典型(TRPC)的 Ca 内流,这是 IL-6 诱发的持续 STAT3 激活所必需的。在慢性瘙痒的小鼠模型中,背根神经节神经元中 IL-6 的表达上调。背根神经节神经元特异性 IL-6 敲低、脊髓星形胶质细胞特异性 IPR1 敲低和药理学脊髓 TRPC 抑制减轻了 LCN2 的表达和慢性瘙痒。
结论
我们的研究结果表明,星形胶质细胞中由 IL-6 引发的 IPR1/TRPC 通道介导的 Ca 信号对于持续的 STAT3 激活、LCN2 表达和慢性瘙痒是必要的,它们也可能为治疗干预提供新的靶点。
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