AMD3100 对骨形态发生蛋白-2 诱导的骨再生具有增效作用。

IF 2 Q2 DENTISTRY, ORAL SURGERY & MEDICINE

Maxillofacial Plastic and Reconstructive Surgery Pub Date : 2024-06-17 DOI:10.1186/s40902-024-00431-y

Gyu-Jo Shim, Chung O Lee, Jung-Tae Lee, Hong-Moon Jung, Tae-Geon Kwon

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引用次数: 0

摘要

背景：AMD3100是一种CXCR4拮抗剂，目前用于激活造血干细胞的动员。最近，研究表明 AMD3100 可通过刺激间充质细胞的迁移，增强骨形态发生蛋白-2（BMP-2）诱导的骨形成。然而，如何优化 AMD3100 和 BMP-2 的战略组合尚未明确确定。本研究的目的是评估 AMD3100 在体外和小鼠腓骨缺损愈合模型中对 BMP-2 诱导的骨再生的影响：方法：通过碱性磷酸酶（ALP）活性、ALP染色和钙积累分析AMD3100和BMP-2连续处理后的体外成骨细胞分化和细胞迁移。用 AMD3100 和/或 BMP-2 处理间充质细胞后，对其迁移能力进行了评估。使用临界大小的腓骨缺损模型来评估连续或连续使用 AMD3100 和 BMP-2 处理后的骨形成情况。使用微型计算机断层扫描（micro-CT）和组织学染色分析了缺损处的骨形成程度：结果：与单独使用 AMD3100 或 BMP-2 治疗相比，间充质细胞在连续使用 AMD3100 和 BMP-2 治疗后，成骨分化程度有所提高。与单独使用 BMP-2 或单独使用 AMD3100 相比，使用 AMD3100 和 BMP-2 能明显激活间充质细胞的细胞迁移。显微 CT 和组织形态学分析表明，与未注射 AMD3100 的对照组相比，连续腹腔注射 AMD3100 能显著增加腓骨缺损中 BMP-2 负载支架的新骨形成。此外，与未注射 AMD3100 的连续 BMP-2 处理相比，单次 IP 注射 AMD3100 和随后向腓肠肌缺损的支架注射 BMP-2 均显示出明显的新骨形成：我们的数据表明，单次或连续注射 AMD3100 可促进 BMP-2 诱导的成骨细胞分化和骨再生。AMD3100和BMP-2的这种策略性组合可能是一种很有前景的骨再生疗法。

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Potentiating effect of AMD3100 on bone morphogenetic protein-2 induced bone regeneration.

Background: AMD3100, a CXCR4 antagonist, is currently prescribed for activating the mobilization of hematopoietic stem cells. Recently, AMD3100 was shown to potentiate bone morphogenetic protein-2 (BMP-2)-induced bone formation by stimulating the trafficking of mesenchymal cells. However, optimization of the strategic combination of AMD3100 and BMP-2 has not yet been clearly established. The purpose of this study was to evaluate the effect of AMD3100 on BMP-2-induced bone regeneration in vitro and in a mouse calvarial defect healing model.

Methods: In vitro osteoblastic differentiation and cell migration after sequential treatments with AMD3100 and BMP-2 were analyzed by alkaline phosphatase (ALP) activity, ALP staining, and calcium accumulation. Migration capacity was evaluated after treating mesenchymal cells with AMD3100 and/or BMP-2. A critical-size calvarial defect model was used to evaluate bone formation after sequential or continuous treatment with AMD3100 and BMP-2. The degree of bone formation in the defect was analyzed using micro-computed tomography (micro-CT) and histological staining.

Results: Compared with single treatment using either AMD3100 or BMP-2 alone, sequential treatment with AMD3100 followed by BMP-2 on mesenchymal cells increased osteogenic differentiation. Application of AMD3100 and subsequent BMP-2 significantly activated cell migration on mesenchymal cell than BMP-2 alone or AMD3100 alone. Micro-CT and histomorphometric analysis showed that continuous intraperitoneal (IP) injection of AMD3100 resulted significantly increased new bone formation in BMP-2 loaded scaffold in calvarial defect than control groups without AMD3100 IP injection. Additionally, both single IP injection of AMD3100 and subsequent BMP-2 injection to the scaffold in calvarial defect showed pronounced new bone formation compared to continuous BMP-2 treatment without AMD3100 treatment.

Conclusion: Our data suggest that single or continuous injection of AMD3100 can potentiate BMP-2-induced osteoblastic differentiation and bone regeneration. This strategic combination of AMD3100 and BMP-2 may be a promising therapy for bone regeneration.

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来源期刊

Maxillofacial Plastic and Reconstructive Surgery DENTISTRY, ORAL SURGERY & MEDICINE-

CiteScore

4.30

自引率

13.00%

发文量

审稿时长

13 weeks