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AKT Pathway Affects Bone Regeneration in Nonunion Treated with Umbilical Cord-Derived Mesenchymal Stem Cells

机译:AKT通路影响脐带间充质干细胞治疗的骨不连中的骨再生。

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摘要

We have previously grafted human umbilical cord-derived mesenchymal stem cells (hUC-MSCs) with blood plasma to treat rat tibia nonunion. To further examine the biological characteristics of this process, we applied an established hUC-MSCs-treated rat nonunion model with the addition of an inhibitor of AKT. SD rats (80) were randomly divided into four groups: a fracture group (positive control); a nonunion group (negative control); a hUC-MSCs grafting with blood plasma group; and a hUC-MSCs grafting with blood plasma & AKT blocker group. The animals were sacrificed under deep anesthesia at 4 and 8 weeks post fracture for analysis. The fracture line became less defined at 4 weeks and disappeared at 8 weeks postoperatively in both the hUC-MSCs grafting with blood plasma and grafting with blood plasma & the AKT blocker, which is similar to the fracture group. Histological immunofluorescence studies showed that the numbers of hUC-MSCs in the calluses were significantly higher in the hUC-MSCs grafting with blood plasma than those in group with the AKT blocker. More bone morphogenetic protein 2 and bone sialoprotein expression and less osteoprotegerin and bone gla protein expression were observed in the AKT blocker group compared to the hUC-MSCs grafting with blood plasma. AKT gene expression in the AKT blocker group was decreased 50 % compared to the hUC-MSCs with plasma group and decreased 70 % compared to the fracture group, while the elastic modulus was decreased. In summary, our work demonstrates that AKT may play a role in modulating osteogenesis induced by hUC-MSCs.
机译:我们先前已将血浆与人脐带来源的间充质干细胞(hUC-MSC)移植在一起,以治疗大鼠胫骨骨不连。为了进一步检查该过程的生物学特性,我们应用了建立的hUC-MSCs处理的大鼠骨不连模型,并添加了AKT抑制剂。 SD大鼠(80只)随机分为四组:骨折组(阳性对照组);骨折组(对照组)。一个不工会团体(阴性对照); hUC-MSCs移植至血浆组;和hUC-MSCs移植血浆和AKT阻断剂组。骨折后第4和8周在深度麻醉下处死动物以进行分析。在hUC-MSCs血浆移植以及血浆和AKT阻断剂移植后,骨折线在4周时变得不太清晰,在术后8周时消失,这与骨折组相似。组织学免疫荧光研究表明,在血浆中移植的hUC-MSC中,愈伤组织中hUC-MSC的数量明显高于AKT阻断剂组。与移植血浆的hUC-MSC相比,AKT阻断剂组观察到更多的骨形态发生蛋白2和骨唾液蛋白表达,以及更少的骨保护素和骨gla蛋白表达。与血浆组hUC-MSC相比,AKT阻滞剂组的AKT基因表达降低50%,与骨折组相比降低70%,而弹性模量降低。总之,我们的工作表明AKT可能在调节hUC-MSC诱导的成骨过程中发挥作用。

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