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MMP-3 介导的 OPN 裂解参与了氧化铜纳米颗粒诱导的成纤维细胞激活。

MMP-3-mediated cleavage of OPN is involved in copper oxide nanoparticle-induced activation of fibroblasts.

机构信息

Department of Epidemiology and Population Health, School of Public Health and Information Sciences, University of Louisville, 485 E. Gray Street, Louisville, KY, 40202, USA.

Northwestern University Feinberg School of Medicine, Chicago, IL, 60611, USA.

出版信息

Part Fibre Toxicol. 2023 May 22;20(1):22. doi: 10.1186/s12989-023-00532-y.

Abstract

BACKGROUND

Copper oxide nanoparticles (Nano-CuO) are one of the most produced and used nanomaterials. Previous studies have shown that exposure to Nano-CuO caused acute lung injury, inflammation, and fibrosis. However, the mechanisms underlying Nano-CuO-induced lung fibrosis are still unclear. Here, we hypothesized that exposure of human lung epithelial cells and macrophages to Nano-CuO would upregulate MMP-3, which cleaved osteopontin (OPN), resulting in fibroblast activation and lung fibrosis.

METHODS

A triple co-culture model was established to explore the mechanisms underlying Nano-CuO-induced fibroblast activation. Cytotoxicity of Nano-CuO on BEAS-2B, U937* macrophages, and MRC-5 fibroblasts were determined by alamarBlue and MTS assays. The expression or activity of MMP-3, OPN, and fibrosis-associated proteins was determined by Western blot or zymography assay. Migration of MRC-5 fibroblasts was evaluated by wound healing assay. MMP-3 siRNA and an RGD-containing peptide, GRGDSP, were used to explore the role of MMP-3 and cleaved OPN in fibroblast activation.

RESULTS

Exposure to non-cytotoxic doses of Nano-CuO (0.5 and 1 µg/mL) caused increased expression and activity of MMP-3 in the conditioned media of BEAS-2B and U937* cells, but not MRC-5 fibroblasts. Nano-CuO exposure also caused increased production of cleaved OPN fragments, which was abolished by MMP-3 siRNA transfection. Conditioned media from Nano-CuO-exposed BEAS-2B, U937*, or the co-culture of BEAS-2B and U937* caused activation of unexposed MRC-5 fibroblasts. However, direct exposure of MRC-5 fibroblasts to Nano-CuO did not induce their activation. In a triple co-culture system, exposure of BEAS-2B and U937* cells to Nano-CuO caused activation of unexposed MRC-5 fibroblasts, while transfection of MMP-3 siRNA in BEAS-2B and U937* cells significantly inhibited the activation and migration of MRC-5 fibroblasts. In addition, pretreatment with GRGDSP peptide inhibited Nano-CuO-induced activation and migration of MRC-5 fibroblasts in the triple co-culture system.

CONCLUSIONS

Our results demonstrated that Nano-CuO exposure caused increased production of MMP-3 from lung epithelial BEAS-2B cells and U937* macrophages, which cleaved OPN, resulting in the activation of lung fibroblasts MRC-5. These results suggest that MMP-3-cleaved OPN may play a key role in Nano-CuO-induced activation of lung fibroblasts. More investigations are needed to confirm whether these effects are due to the nanoparticles themselves and/or Cu ions.

摘要

背景

氧化铜纳米颗粒(Nano-CuO)是产量和使用量最大的纳米材料之一。先前的研究表明,暴露于 Nano-CuO 会导致急性肺损伤、炎症和纤维化。然而,Nano-CuO 诱导肺纤维化的机制仍不清楚。在这里,我们假设暴露于人肺上皮细胞和巨噬细胞中的 Nano-CuO 会上调 MMP-3,MMP-3 可切割骨桥蛋白(OPN),导致成纤维细胞活化和肺纤维化。

方法

建立了三重共培养模型以探索 Nano-CuO 诱导成纤维细胞活化的机制。通过 alamarBlue 和 MTS 测定法测定 Nano-CuO 对 BEAS-2B、U937*巨噬细胞和 MRC-5 成纤维细胞的细胞毒性。通过 Western blot 或酶谱测定法测定 MMP-3、OPN 和纤维化相关蛋白的表达或活性。通过划痕愈合测定法评估 MRC-5 成纤维细胞的迁移。使用 MMP-3 siRNA 和包含 RGD 的肽(GRGDSP)来研究 MMP-3 和切割的 OPN 在成纤维细胞活化中的作用。

结果

暴露于非细胞毒性剂量的 Nano-CuO(0.5 和 1 µg/mL)会导致 BEAS-2B 和 U937细胞的条件培养基中 MMP-3 的表达和活性增加,但 MRC-5 成纤维细胞则不然。Nano-CuO 暴露还导致切割的 OPN 片段的产生增加,而 MMP-3 siRNA 转染则消除了这一增加。暴露于 Nano-CuO 的 BEAS-2B、U937或 BEAS-2B 和 U937共培养的条件培养基会引起未暴露的 MRC-5 成纤维细胞的活化。然而,直接暴露于 Nano-CuO 的 MRC-5 成纤维细胞不会诱导其活化。在三重共培养系统中,暴露于 BEAS-2B 和 U937细胞的 Nano-CuO 会引起未暴露的 MRC-5 成纤维细胞的活化,而 BEAS-2B 和 U937*细胞中 MMP-3 siRNA 的转染则显著抑制了 MRC-5 成纤维细胞的活化和迁移。此外,GRGDSP 肽预处理可抑制三重共培养系统中 Nano-CuO 诱导的 MRC-5 成纤维细胞的活化和迁移。

结论

我们的结果表明,Nano-CuO 暴露会导致肺上皮 BEAS-2B 细胞和 U937*巨噬细胞中 MMP-3 的产生增加,从而切割 OPN,导致肺成纤维细胞 MRC-5 的活化。这些结果表明,MMP-3 切割的 OPN 可能在 Nano-CuO 诱导的肺成纤维细胞活化中起关键作用。需要进一步的研究来确认这些影响是否归因于纳米颗粒本身和/或 Cu 离子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d669/10201731/2bb9480a0af9/12989_2023_532_Fig9_HTML.jpg

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