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富马酸二甲酯通过抑制 MSK1 和 RSK1 的激活以及诱导核 p-c-Jun(S63)和 p-p53(S15)的表达来抑制 MIF 诱导的角质形成细胞增殖。

Dimethylfumarate inhibits MIF-induced proliferation of keratinocytes by inhibiting MSK1 and RSK1 activation and by inducing nuclear p-c-Jun (S63) and p-p53 (S15) expression.

机构信息

Department of Dermatology, Aarhus University Hospital, P.P. Oerumsgade 11, 8000 Aarhus, Denmark.

出版信息

Inflamm Res. 2011 Jul;60(7):643-53. doi: 10.1007/s00011-011-0316-7. Epub 2011 Feb 22.

DOI:10.1007/s00011-011-0316-7
PMID:21340650
Abstract

OBJECTIVE

Dimethylfumarate (DMF) is used in the treatment of psoriasis. Macrophage migration inhibitory factor (MIF) is elevated in patients with severe psoriasis. We studied the effect of DMF on the MIF-induced activation of the mitogen- and stress-activated kinase 1 (MSK1) and p90 kDa ribosomal S6 kinase (RSK1) signaling pathways which regulate the proliferation of human keratinocytes via transcription factors.

METHODS

The effects of DMF on the MIF-induced activation of MSK1, RSK1, cAMP-responsive element-binding protein (CREB), Cox-2 and c-Jun, JunB and p53 were studied by Western blotting using phospho-specific antibodies.

RESULTS

DMF inhibited the MIF-induced phosphorylation of MSK1, RSK1, CREB and JunB, and reduced Cox-2 expression and the proliferation of cultured human keratinocytes. The expression of p-p53 (S15) was induced simultaneously with the inhibition of Cox-2. Addition of DMF before MIF induced nuclear expression of p-c-Jun (S63) and c-Jun. Transfection with small interfering MSK1 and RSK1 RNA before MIF incubation stimulated p-p53 (S15) and nuclear p-c-Jun (S63) similarly to DMF.

CONCLUSION

Our results indicate that the specific inhibitory effects of DMF on RSK1 and MSK1 activation together with the induction of p-c-Jun (S63) and p-p53 (S15) lead to the inhibition of keratinocyte proliferation, partly explaining the anti-psoriatic effect of DMF.

摘要

目的

富马酸二甲酯(DMF)用于治疗银屑病。在严重银屑病患者中,巨噬细胞移动抑制因子(MIF)升高。我们研究了 DMF 对 MIF 诱导的丝裂原和应激激活激酶 1(MSK1)和 p90 核糖体 S6 激酶(RSK1)信号通路的影响,这些信号通路通过转录因子调节人角质形成细胞的增殖。

方法

通过使用磷酸特异性抗体的 Western 印迹法研究 DMF 对 MIF 诱导的 MSK1、RSK1、cAMP 反应元件结合蛋白(CREB)、Cox-2 和 c-Jun、JunB 和 p53 的激活的影响。

结果

DMF 抑制了 MIF 诱导的 MSK1、RSK1、CREB 和 JunB 的磷酸化,并减少了 Cox-2 的表达和培养的人角质形成细胞的增殖。p-p53(S15)的表达与 Cox-2 的抑制同时诱导。在 MIF 诱导之前添加 DMF 诱导核表达 p-c-Jun(S63)和 c-Jun。在用 MIF 孵育之前用小干扰 MSK1 和 RSK1 RNA 转染同样刺激 p-p53(S15)和核 p-c-Jun(S63)。

结论

我们的结果表明,DMF 对 RSK1 和 MSK1 激活的特异性抑制作用以及诱导 p-c-Jun(S63)和 p-p53(S15)导致角质形成细胞增殖的抑制,部分解释了 DMF 的抗银屑病作用。

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Dimethylfumarate inhibits MIF-induced proliferation of keratinocytes by inhibiting MSK1 and RSK1 activation and by inducing nuclear p-c-Jun (S63) and p-p53 (S15) expression.富马酸二甲酯通过抑制 MSK1 和 RSK1 的激活以及诱导核 p-c-Jun(S63)和 p-p53(S15)的表达来抑制 MIF 诱导的角质形成细胞增殖。
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MSK activation and physiological roles.肌肉骨骼激活与生理作用。
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Transcription Factor IRF7 is Involved in Psoriasis Development and Response to Guselkumab Treatment.转录因子IRF7参与银屑病的发展及对古塞库单抗治疗的反应。
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