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Methyl cap binding protein 2: a key epigenetic protein in systemic sclerosis.甲基化 CpG 结合蛋白 2:系统性硬化症中的关键表观遗传蛋白。
Rheumatology (Oxford). 2019 Mar 1;58(3):527-535. doi: 10.1093/rheumatology/key327.
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Targeting TLRs and the inflammasome in systemic sclerosis.靶向系统性硬化症中的 TLRs 和炎性小体。
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Aortic carboxypeptidase-like protein, a WNT ligand, exacerbates nonalcoholic steatohepatitis.主动脉羧肽酶样蛋白,一种 WNT 配体,可加重非酒精性脂肪性肝炎。
J Clin Invest. 2018 Apr 2;128(4):1581-1596. doi: 10.1172/JCI92863. Epub 2018 Mar 19.
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Leptin up-regulates microRNA-27a/b-3p level in hepatic stellate cells.瘦素上调肝星状细胞中 microRNA-27a/b-3p 的水平。
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MicroRNAs in the skin: role in development, homoeostasis and regeneration.皮肤中的微小RNA:在发育、稳态和再生中的作用
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Effect of TGF-β/smad signaling pathway blocking on expression profiles of miR-335, miR-150, miR-194, miR-27a, and miR-199a of hepatic stellate cells (HSCs).转化生长因子-β/信号转导和转录激活因子信号通路阻断对肝星状细胞(HSCs)中miR-335、miR-150、miR-194、miR-27a和miR-199a表达谱的影响。
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Interplay between genetic and epigenetic mechanisms in rheumatoid arthritis.类风湿关节炎中遗传和表观遗传机制之间的相互作用。
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microRNA27a-3p 介导系统性硬化症中 Wnt 拮抗剂 sFRP-1 的减少。

microRNA27a-3p mediates reduction of the Wnt antagonist sFRP-1 in systemic sclerosis.

机构信息

Faculty of Health and Life Sciences, Northumbria University, Newcastle Upon Tyne, UK.

Department of Biosciences, Durham University, Durham, UK.

出版信息

Epigenetics. 2021 Jun-Jul;16(7):808-817. doi: 10.1080/15592294.2020.1827715. Epub 2020 Oct 4.

DOI:10.1080/15592294.2020.1827715
PMID:32965161
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8216176/
Abstract

Systemic Sclerosis (SSc) is an autoimmune connective tissue disease that leads to skin and lung fibrosis. The Wnt pathway is clearly elevated in SSc and is pro-fibrotic via activation of canonical Wnt signalling. sFRP-1 is a Wnt antagonist that acts as a negative regulator of Wnt signalling. We sought to measure the levels of serum sFRP-1 in early diffuse SSc patients compared to healthy controls and if this is regulated by microRNA27a-3p. Ten early diffuse SSc patients and healthy controls sera were taken and sFRP-1 quantified by ELISA. Skin biopsies were also taken in five SSc patients and controls. Fibroblasts were quantified for microRNA27-3p expression by Taqman qRT-PCR with an internal microRNA to normalize. 3'UTR luciferase assays were performed to confirm direct targets of microRNA27a-3p with microRNA overexpression. Fibroblasts were transfected with microRNA27a mimics or scramble controls and using ELISA sFRP-1 was quantified. Furthermore, Collagen, Axin-2, TIMP-1 and MMP-1 were measured. Serum sFRP-1 was significantly reduced in early diffuse SSc patients. We identified microRNA27a-3p-3p as regulating sFRP-1 in dermal fibroblasts. We found significantly elevated microRNA27a-3p in isolated dermal fibroblasts from SSc patients. We confirmed that sFRP-1 is a direct target of microRNA27a-3p through cloning of the 3'UTR into a luciferase vector. ECM genes were also upregulated by microRNA27a-3p-3p and the matrix-degrading enzyme MMP-1 was suppressed. Serum sFRP-1 is reduced in diffuse SSc patients and is regulated by microRNA27a-3p and this is a direct regulation. Modulation of microRNA27a-3p levels could mediate fibrosis regression.

摘要

系统性硬化症(SSc)是一种自身免疫性结缔组织疾病,可导致皮肤和肺部纤维化。Wnt 通路在 SSc 中明显升高,并通过激活经典 Wnt 信号而具有促纤维化作用。sFRP-1 是一种 Wnt 拮抗剂,作为 Wnt 信号的负调节剂。我们试图测量早期弥漫性 SSc 患者与健康对照组相比血清 sFRP-1 的水平,以及这是否受 microRNA27a-3p 的调节。收集了 10 例早期弥漫性 SSc 患者和健康对照组的血清,并通过 ELISA 定量 sFRP-1。还在 5 例 SSc 患者和对照者中采集了皮肤活检。通过 Taqman qRT-PCR 用内源性 microRNA 对成纤维细胞中 microRNA27-3p 的表达进行定量,以进行归一化。进行 3'UTR 荧光素酶测定以确认 microRNA27a-3p 的直接靶标与 microRNA 过表达。用 microRNA27a 模拟物或对照物转染成纤维细胞,并通过 ELISA 定量 sFRP-1。此外,还测量了胶原蛋白、Axin-2、TIMP-1 和 MMP-1。早期弥漫性 SSc 患者血清 sFRP-1 显著降低。我们鉴定出 microRNA27a-3p-3p 是真皮成纤维细胞中 sFRP-1 的调节因子。我们发现 SSc 患者分离的真皮成纤维细胞中 microRNA27a-3p 显著升高。我们通过将 3'UTR 克隆到荧光素酶载体中证实 sFRP-1 是 microRNA27a-3p 的直接靶标。microRNA27a-3p-3p 还上调了 ECM 基因,并且基质降解酶 MMP-1 受到抑制。弥漫性 SSc 患者血清 sFRP-1 降低,受 microRNA27a-3p 调节,这是一种直接调节。调节 microRNA27a-3p 水平可能介导纤维化消退。