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Development of a Cyclosporin-A-Induced Immune Tolerant Rat Model to Test Marrow Allograft Cell Type Effects on Bone Repair

机译:环孢菌素A诱导的免疫耐受大鼠模型的开发,以测试骨髓同种异体移植细胞类型对骨修复的影响

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Bone repair is an important concept in tissue engineering, and the ability to repair bone in hypotrophic conditions such as that of irradiated bone, represents a challenge for this field. Previous studies have shown that a combination of bone marrow and (BCP) was effective to repair irradiated bone. However, the origin and role played by each cell type in bone healing still remains unclear. In order to track the grafted cells, the development of an animal model that is immunotolerant to an allograft of bone marrow would be useful. Furthermore, because the immune system interacts with bone turnover, it is of critical importance to demonstrate that immunosuppressive drugs do not interfere with bone repair. After a preliminary study of immunotolerance, cyclosporin-A was chosen to be used in immunosuppressive therapy. Ten rats were included to observe qualitative and quantitative bone repair 8 days and 6 weeks after the creation of bone defects. The defects were filled with an allograft of bone marrow alone or in association with BCP under immunosuppressive treatment (cyclosporin-A). The results showed that there was no significant interaction of cyclosporin-A with osseous regeneration. The use of this new immunotolerant rat model of bone marrow allograft in future studies will provide insight on how the cells within the bone marrow graft contribute to bone healing, especially in irradiated conditions.
机译:骨修复是组织工程中的重要概念,并且在营养不足的条件下(例如受辐照的骨)修复骨的能力是该领域的挑战。先前的研究表明,骨髓和(BCP)组合可有效修复受辐照的骨骼。然而,每种细胞类型在骨愈合中所起的作用和作用仍不清楚。为了追踪移植的细胞,对同种异体骨髓免疫耐受的动物模型的开发将是有用的。此外,由于免疫系统与骨骼更新相互作用,因此证明免疫抑制药物不会干扰骨骼修复至关重要。在对免疫耐受性进行了初步研究之后,选择了环孢菌素A用于免疫抑制治疗。包括十只大鼠,以在骨缺损产生后8天和6周观察定性和定量的骨修复。在免疫抑制治疗下(Cyclsporin-A),单独或与BCP联合植入同种异体骨髓来填充缺损。结果表明,环孢菌素A与骨再生无显着相互作用。在未来的研究中使用这种新的免疫耐受的大鼠异体骨髓移植大鼠模型将提供有关骨髓移植物中细胞如何促进骨愈合的见识,尤其是在辐照条件下。

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