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Osteoblast-derived VEGF regulates osteoblast differentiation and bone formation during bone repair

机译:成骨细胞衍生的VEGF调节骨修复过程中的成骨细胞分化和骨形成

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摘要

Osteoblast-derived VEGF is important for bone development and postnatal bone homeostasis. Previous studies have demonstrated that VEGF affects bone repair and regeneration; however, the cellular mechanisms by which it works are not fully understood. In this study, we investigated the functions of osteoblast-derived VEGF in healing of a bone defect. The results indicate that osteoblast-derived VEGF plays critical roles at several stages in the repair process. Using transgenic mice with osteoblast-specific deletion of Vegfa, we demonstrated that VEGF promoted macrophage recruitment and angiogenic responses in the inflammation phase, and optimal levels of VEGF were required for coupling of angiogenesis and osteogenesis in areas where repair occurs by intramembranous ossification. VEGF likely functions as a paracrine factor in this process because deletion of Vegfr2 in osteoblastic lineage cells enhanced osteoblastic maturation and mineralization. Furthermore, osteoblast- and hypertrophic chondrocyte–derived VEGF stimulated recruitment of blood vessels and osteoclasts and promoted cartilage resorption at the repair site during the periosteal endochondral ossification stage. Finally, osteoblast-derived VEGF stimulated osteoclast formation in the final remodeling phase of the repair process. These findings provide a basis for clinical strategies to improve bone regeneration and treat defects in bone healing.
机译:成骨细胞衍生的VEGF对于骨骼发育和产后骨骼体内稳态非常重要。先前的研究表明,VEGF影响骨修复和再生。但是,其工作的细胞机制尚未完全了解。在这项研究中,我们调查了成骨细胞衍生的VEGF在骨缺损愈合中的功能。结果表明,成骨细胞源性VEGF在修复过程的多个阶段起着关键作用。使用具有成骨细胞特异性Vegfa缺失的转基因小鼠,我们证明了VEGF在炎症阶段促进了巨噬细胞募集和血管生成反应,并且在通过膜内骨化发生修复的区域中,血管生成和成骨的耦合需要最佳水平的VEGF。 VEGF可能在此过程中充当旁分泌因子,因为成骨细胞系细胞中Vegfr2的缺失增强了成骨细胞的成熟和矿化作用。此外,在骨膜软骨内骨化阶段,成骨细胞和肥大性软骨细胞衍生的VEGF刺激血管和破骨细胞的募集并促进修复部位的软骨吸收。最后,在修复过程的最后重塑阶段,成骨细胞衍生的VEGF刺激破骨细胞形成。这些发现为改善骨再生和治疗骨愈合缺陷的临床策略提供了基础。

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