阿斯匹林触发的Resolvin D1与地塞米松治疗Sjögren综合征样NOD/ShiLtJ小鼠的初步研究

Justin T Easley, Joel W Nelson, Rachel E Mellas, Salah Sommakia, Chunhua Wu, Bryan Trump, Olga J Baker
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引用次数: 11

摘要

Resolvin D1 (RvD1)及其阿斯匹林触发的外显体形式(AT-RvD1)是内源性脂质介质(来源于二十二碳六烯酸,DHA),在复杂疾病模型中控制炎症的持续时间和程度。我们之前的研究表明,rvd1介导的信号通路在啮齿动物和人类的唾液腺中表达和活跃。此外,用RvD1处理唾液细胞可阻断TNF-α-介导的炎症信号并改善上皮的完整性。本初步研究的目的是确定AT-RvD1与地塞米松(DEX)治疗NOD/ShiLtJ Sjögren综合征(SS)小鼠模型下颌下腺(SMG)炎症(即淋巴细胞浸润、细胞因子表达和凋亡)的可行性,然后再进行更大规模的实验。从4周龄开始,NOD/ShiLtJ小鼠每周2次静脉注射NaCl(0.9%,阴性对照)、at - rvd1 (0.01-0.1 mg/kg)或DEX (4.125-8.25 mg/kg),连续14周。在18周龄时,收集SMG进行病理分析和检测ss相关炎症基因。单独使用AT-RvD1不影响NOD/ShiLtJ小鼠淋巴细胞浸润,而DEX部分阻止淋巴细胞浸润。有趣的是,AT-RvD1和DEX均引起ss相关炎症基因的下调和细胞凋亡的减少。这项初步研究的结果表明,单独使用AT-RvD1和DEX进行全身治疗可以减轻NOD/ShiLtJ小鼠的炎症反应;因此,无论是单独使用还是联合使用,它们都可能被认为是治疗SS患者的潜在治疗工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Aspirin-Triggered Resolvin D1 Versus Dexamethasone in the Treatment of Sjögren's Syndrome-Like NOD/ShiLtJ Mice - A Pilot Study.

Aspirin-Triggered Resolvin D1 Versus Dexamethasone in the Treatment of Sjögren's Syndrome-Like NOD/ShiLtJ Mice - A Pilot Study.

Aspirin-Triggered Resolvin D1 Versus Dexamethasone in the Treatment of Sjögren's Syndrome-Like NOD/ShiLtJ Mice - A Pilot Study.

Aspirin-Triggered Resolvin D1 Versus Dexamethasone in the Treatment of Sjögren's Syndrome-Like NOD/ShiLtJ Mice - A Pilot Study.

Resolvin D1 (RvD1) and its aspirin-triggered epimeric form (AT-RvD1) are endogenous lipid mediators (derived from docosahexaenoic acid, DHA) that control the duration and magnitude of inflammation in models of complex diseases. Our previous studies demonstrated that RvD1-mediated signaling pathways are expressed and active in salivary glands from rodents and humans. Furthermore, treatment of salivary cells with RvD1 blocked TNF-α-mediated inflammatory signals and improved epithelial integrity. The purpose of this pilot study was to determine the feasibility of treatment with AT-RvD1 versus dexamethasone (DEX) on inflammation (i.e., lymphocytic infiltration, cytokine expression and apoptosis) observed in submandibular glands (SMG) from the NOD/ShiLtJ Sjögren's syndrome (SS) mouse model before experimenting with a larger population. NOD/ShiLtJ mice were treated intravenously with NaCl (0.9%, negative control), AT-RvD1 (0.01-0.1 mg/kg) or DEX (4.125-8.25 mg/kg) twice a week for 14 weeks beginning at 4 weeks of age. At 18 weeks of age, SMG were collected for pathological analysis and detection of SS-associated inflammatory genes. The AT-RvD1 treatment alone did not affect lymphocytic infiltration seen in NOD/ShiLtJ mice while DEX partially prevented lymphocytic infiltration. Interestingly, both AT-RvD1 and DEX caused downregulation of SS-associated inflammatory genes and reduction of apoptosis. Results from this pilot study suggest that a systemic treatment with AT-RvD1 and DEX alone attenuated inflammatory responses observed in the NOD/ShiLtJ mice; therefore, they may be considered as potential therapeutic tools in treating SS patients when used alone or in combination.

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