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GO 介导的骨髓间充质干细胞在基础和成骨诱导培养基中的差异基因表达。

Differential gene expression of Wharton's jelly-derived mesenchymal cells mediated by graphene oxide in basal and osteo-induced media.

机构信息

Biotechnology Research Institute, Universiti Malaysia Sabah, Jalan UMS, 88400, Kota Kinabalu, Sabah, Malaysia.

出版信息

Mol Biol Rep. 2024 Mar 3;51(1):383. doi: 10.1007/s11033-024-09324-9.

Abstract

BACKGROUND

Graphene oxide (GO) is widespread in scaffold engineering owing to its extraordinary properties such as multiple oxygen functional groups, high hydrophilicity ability and biocompatibility. It is known to promote differentiation in mesenchymal stem cells, but concomitant comparison of its modulation on the expression profiles of Wharton's jelly (WJ)-MSC surface markers, lineage differentiation, and epigenetic regulatory genes in basal and induced condition are still lacking. Unraveling the fundamental mechanisms is essential for the effective utilization of WJ-MSCs incorporated with GO in therapy. This study aims to explore the unique gene expression profiles and epigenetic characteristics of WJ-MSCs influenced by GO.

METHODS AND RESULTS

The characterized GO-coated coverslip served as a substrate for culturing WJ-MSCs. In addition to investigating the impact of GO on cell proliferation and differentiation, we conducted a gene expression study using PCR array, while epigenetic control was assessed through bisulfite sequencing and Western blot analysis. Our findings indicate that the presence of GO maintained the proliferation and survival of WJ-MSCs. In the absence of induction, GO led to minor lipid and glycosaminoglycan deposition in WJ-MSCs. This was evidenced by the sustained expression of pluripotency and lineage-specific genes, demethylation at the OCT4 promoter, and a decrease in H3K9 methylation. In osteo-induced condition, the occurrence of osteogenesis appeared to be guided by BMP/TGF and ERK pathway activation, accompanied by the upregulation of osteogenic-related genes and downregulation of DNMT3b.

CONCLUSIONS

GO in osteo-induced condition create a favorable microenvironment that promotes the osteogenesis of WJ-MSCs by influencing genetic and epigenetic controls. This helps in advancing our knowledge on the use of GO as priming platform and WJ-MSCs an alternate source for bone repair and regeneration.

摘要

背景

氧化石墨烯(GO)因其具有多个含氧官能团、高亲水性和生物相容性等卓越性能,在支架工程中得到了广泛应用。已知其能促进间充质干细胞的分化,但同时比较其对牙髓间充质干细胞(WJ-MSC)表面标志物、谱系分化以及基础和诱导条件下表观遗传调节基因表达谱的调制作用仍然缺乏。揭示其基本机制对于有效利用与 GO 结合的 WJ-MSCs 进行治疗至关重要。本研究旨在探讨 GO 对 WJ-MSCs 影响的独特基因表达谱和表观遗传特征。

方法和结果

经过表征的 GO 涂层盖玻片作为培养 WJ-MSCs 的基质。除了研究 GO 对细胞增殖和分化的影响外,我们还使用 PCR 阵列进行了基因表达研究,同时通过亚硫酸氢盐测序和 Western blot 分析评估了表观遗传控制。我们的研究结果表明,GO 的存在维持了 WJ-MSCs 的增殖和存活。在没有诱导的情况下,GO 导致 WJ-MSCs 中脂质和糖胺聚糖的沉积较少。这表现在多能性和谱系特异性基因的持续表达、OCT4 启动子的去甲基化以及 H3K9 甲基化的减少。在成骨诱导条件下,成骨的发生似乎受到 BMP/TGF 和 ERK 通路激活的引导,伴随着成骨相关基因的上调和 DNMT3b 的下调。

结论

GO 在成骨诱导条件下创造了有利的微环境,通过影响遗传和表观遗传控制来促进 WJ-MSCs 的成骨作用。这有助于我们深入了解 GO 作为启动平台的应用和 WJ-MSCs 作为骨修复和再生替代来源的潜力。

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