School of Medicine, Griffith University, Gold Coast, Queensland, Australia.
Department of Orthopedic Surgery, Mayo Clinic, Rochester, Minnesota, USA.
Tissue Eng Part A. 2021 Aug;27(15-16):1084-1098. doi: 10.1089/ten.TEA.2020.0218. Epub 2021 Jan 12.
High concentrations of bone morphogenetic protein 2 (BMP2) in bone regeneration cause adverse events (e.g, heterotopic bone formation and acute inflammation). This study examines novel epigenetic strategies (i.e., EZH2 inhibition) for augmenting osteogenesis, thereby aiming to reduce the required BMP2 dose for bone regeneration and minimize these adverse effects. Human bone marrow-derived mesenchymal stem cells (BMSCs) were grown on three-dimensional (3D)-printed medical-grade polycaprolactone scaffolds and incubated in osteogenic media containing 50 ng/mL BMP2 and/or 5 μM GSK126 (EZH2 inhibitor) for 6 days ( = 3 per group and timepoint). Constructs were harvested for realtime quantitative polymerase chain reaction analysis at Day 10 and immunofluorescence (IF) microscopy at Day 21. After pretreating for 6 days and maintaining in osteogenic media for 4 days, BMSC-seeded scaffolds were also implanted in an immunocompromised subcutaneous murine model ( = 39; 3/group/donor and 3 control scaffolds) for histological analysis at 8 weeks. Pretreatment of BMSCs with BMP2 and BMP2/GSK126 costimulated expression of osteoblast-related genes (e.g., , , , and ), as well as protein accumulation (e.g., collagen type 1/ and osteocalcin/) based on IF staining. While implantation for 8 weeks did not result in bone formation, increased angiogenesis was observed in BMP2 and BMP2/GSK126 groups. This study finds that BMP2 and GSK126 costimulate osteogenic differentiation of MSCs on 3D scaffolds and may contribute to enhanced vascularization when implanted to support bone formation. Thus, epigenetic priming with EZH2 inhibitors may have translational potential in bone healing by permitting a reduction of BMP2 dosing to mitigate its side effects. Impact statement While autografts are still the gold standard for bone reconstruction, tissue availability and donor morbidity are significant limitations. Previous attempts to use high concentrations of bone morphogenetic protein 2 (BMP2) have been shown to cause adverse events such as excessive bone formation and acute inflammation. Overall, the utilization of EZH2 inhibitors to modulate gene expression in favor of bone healing has been demonstrated in a tissue engineering strategy. Our study will pave the way to developing tissue engineering strategies involving GSK126 as an adjuvant to increase the effects of BMP2 for stimulating cells of interest on a three-dimensional scaffold for bone regeneration.
高浓度的骨形态发生蛋白 2(BMP2)在骨再生中会引起不良反应(例如异位骨形成和急性炎症)。本研究探讨了新的表观遗传策略(即 EZH2 抑制),以增强成骨作用,从而减少骨再生所需的 BMP2 剂量,并最大程度地减少这些不良反应。将人骨髓间充质干细胞(BMSC)种植在三维(3D)打印的医用聚己内酯支架上,并在含有 50ng/mL BMP2 和/或 5μM GSK126(EZH2 抑制剂)的成骨培养基中孵育 6 天(每组和时间点各 3 个)。在第 10 天进行实时定量聚合酶链反应分析,并在第 21 天进行免疫荧光(IF)显微镜分析,以收集构建体。在预处理 6 天后,在成骨培养基中维持 4 天,然后将 BMSC 接种的支架也植入免疫缺陷皮下小鼠模型中(每组 39 个;每组 3 个供体和 3 个对照支架),在 8 周时进行组织学分析。BMP2 和 BMP2/GSK126 预处理可刺激成骨相关基因(例如,,,,和)的表达以及蛋白质积累(例如,胶原 1/和骨钙素/),这是基于 IF 染色得出的。虽然 8 周的植入并未导致骨形成,但在 BMP2 和 BMP2/GSK126 组中观察到血管生成增加。本研究发现,BMP2 和 GSK126 可在 3D 支架上共同刺激 MSC 的成骨分化,并可能通过植入以支持骨形成来促进血管生成。因此,EZH2 抑制剂的表观遗传启动可能具有通过减少 BMP2 剂量来减轻其副作用从而促进骨愈合的转化潜力。 影响说明 虽然自体移植物仍然是骨重建的金标准,但组织可用性和供体发病率是重大限制。先前使用高浓度骨形态发生蛋白 2(BMP2)的尝试已显示出引起不良反应,例如过度骨形成和急性炎症。总体而言,已经证明在组织工程策略中使用 EZH2 抑制剂来调节有利于骨愈合的基因表达。我们的研究将为开发涉及 GSK126 的组织工程策略铺平道路,以增加 BMP2 对三维支架上感兴趣细胞的刺激作用,从而促进骨再生。
