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Local Application of Isogenic Adipose-Derived Stem Cells Restores Bone Healing Capacity in a Type 2 Diabetes Model

机译:等基因脂肪干细胞的局部应用可恢复2型糖尿病模型的骨愈合能力

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Bone regeneration is typically a reliable process without scar formation. The endocrine disease type 2 diabetes prolongs and impairs this healing process. In a previous work, we showed that angiogenesis and osteogenesis—essential steps of bone regeneration—are deteriorated, accompanied by reduced proliferation in type 2 diabetic bone regeneration. The aim of the study was to improve these mechanisms by local application of adipose-derived stem cells (ASCs) and facilitate bone regeneration in impaired diabetic bone regeneration. The availability of ASCs in great numbers and the relative ease of harvest offers unique advantages over other mesenchymal stem cell entities. A previously described unicortical tibial defect model was utilized in diabetic mice (Leprdb−/−). Isogenic mouse adipose-derived stem cells (mASCs)db−/db− were harvested, transfected with a green fluorescent protein vector, and isografted into tibial defects (150,000 living cells per defect). Alternatively, control groups were treated with Dulbecco’s modified Eagle’s medium or mASCsWT. In addition, wild-type mice were identically treated. By means of immunohistochemistry, proteins specific for angiogenesis, cell proliferation, cell differentiation, and bone formation were analyzed at early (3 days) and late (7 days) stages of bone regeneration. Additionally, histomorphometry was performed to examine bone formation rate and remodeling. Histomorphometry revealed significantly increased bone formation in mASCdb−/db−-treated diabetic mice as compared with the respective control groups. Furthermore, locally applied mASCsdb−/db− significantly enhanced neovascularization and osteogenic differentiation. Moreover, bone remodeling was upregulated in stem cell treatment groups. Local application of mACSs can restore impaired diabetic bone regeneration and may represent a therapeutic option for the future.
机译:骨再生通常是不形成疤痕的可靠过程。内分泌疾病2型糖尿病会延长并损害此愈合过程。在以前的工作中,我们表明血管生成和成骨(骨骼再生的必要步骤)已恶化,伴随着2型糖尿病骨骼再生中增殖的减少。该研究的目的是通过局部应用脂肪干细胞(ASC)来改善这些机制,并在受损的糖尿病骨再生中促进骨再生。与其他间充质干细胞实体相比,大量可获得的ASC和相对容易的收获提供了独特的优势。在糖尿病小鼠中使用了先前描述的单皮质胫骨缺损模型(Lepr db-/-)。收集同基因的小鼠脂肪干细胞(mASCs) db- / db-,用绿色荧光蛋白载体转染,然后同种移植到胫骨缺损中(每个缺损150,000个活细胞)。另外,对照组则使用Dulbecco改良的Eagle培养基或mASCs WT 进行治疗。另外,对野生型小鼠进行了相同的处理。通过免疫组织化学,在骨再生的早期(3天)和晚期(7天)分析了对血管新生,细胞增殖,细胞分化和骨形成具有特异性的蛋白质。另外,进行组织形态计量学以检查骨形成速率和重塑。组织形态计量学显示,与相应对照组相比,mASC db- / db-处理的糖尿病小鼠的骨形成显着增加。此外,局部应用的mASCs db- / db-显着增强了新血管形成和成骨分化。此外,在干细胞治疗组中,骨重塑被上调。 mACS的局部应用可以恢复受损的糖尿病骨再生,并可能代表未来的治疗选择。

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