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白细胞介素 17A 是炎症性皮肤病肝脾淀粉样变性的关键细胞因子。

IL-17A Is the Critical Cytokine for Liver and Spleen Amyloidosis in Inflammatory Skin Disease.

机构信息

Department of Dermatology, Mie University Graduate School of Medicine, 2-174 Edobashi, Tsu 514-8507, Japan.

Department of Personalized Cancer Immunotherapy, Mie University Graduate School of Medicine, 2-174 Edobashi, Tsu 514-8507, Japan.

出版信息

Int J Mol Sci. 2022 May 20;23(10):5726. doi: 10.3390/ijms23105726.

DOI:10.3390/ijms23105726
PMID:35628531
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9147816/
Abstract

Systemic amyloidosis is recognized as a serious complication of rheumatoid arthritis or inflammatory bowel disease, but also of inflammatory skin disease. However, the detailed molecular mechanism of amyloidosis associated with cutaneous inflammation remains unclear, and therapeutic approaches are limited. Here, we investigated the pathophysiology of amyloidosis secondary to cutaneous inflammation and the therapeutic effects of Janus kinase (JAK) inhibitors by examining a mouse model of spontaneous dermatitis (KCASP1Tg mice). Moreover, KCASP1Tg mice were crossed with interleukin-17A (IL-17A) knockout mice to generate IL-17A-/KCASP1Tg and examine the role of IL-17A in amyloidosis under cutaneous inflammation. KCASP1Tg mice showed severe amyloid deposition in the liver and spleen. Increased serum-neutral fat levels and decreased lymphocyte production were observed in the spleen. Overproduction of amyloidosis was partially ameliorated by the administration of JAK inhibitors and was further improved in IL-17A-/KCASP1Tg mice. IL-17A-producing cells included CD4, gamma delta, and CD8 T cells. In summary, our results from the analysis of a mouse model of dermatitis revealed that skin-derived inflammatory cytokines can induce amyloid deposition in the liver and spleen, and that the administration of JAK inhibitors and, even more, IL-17A ablation, reduced amyloidosis. This study demonstrates that active control of skin inflammation is essential to prevent internal organ amyloidosis.

摘要

系统性淀粉样变被认为是类风湿关节炎或炎症性肠病的严重并发症,但也与炎症性皮肤病有关。然而,与皮肤炎症相关的淀粉样变的详细分子机制仍不清楚,且治疗方法有限。在这里,我们通过研究自发性皮炎(KCASP1Tg 小鼠)的小鼠模型,研究了皮肤炎症继发淀粉样变的病理生理学和 Janus 激酶(JAK)抑制剂的治疗效果。此外,我们还将 KCASP1Tg 小鼠与白细胞介素-17A(IL-17A)敲除小鼠杂交,以生成 IL-17A-/KCASP1Tg,并在皮肤炎症下研究 IL-17A 在淀粉样变中的作用。KCASP1Tg 小鼠在肝脏和脾脏中表现出严重的淀粉样沉积。在脾脏中观察到血清中性脂肪水平升高和淋巴细胞生成减少。JAK 抑制剂的给药部分改善了淀粉样变的过度产生,并在 IL-17A-/KCASP1Tg 小鼠中进一步改善。淀粉样变过度产生的细胞包括 CD4、γδ和 CD8 T 细胞。总之,我们对皮炎小鼠模型的分析结果表明,皮肤来源的炎症性细胞因子可诱导肝脏和脾脏中的淀粉样沉积,而 JAK 抑制剂的给药,甚至 IL-17A 的缺失,可减少淀粉样变。本研究表明,积极控制皮肤炎症对于预防内脏器官淀粉样变至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ab52/9147816/632e426402b3/ijms-23-05726-g005.jpg
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