MicroRNA-21a-5p-modified macrophage exosomes as natural nanocarriers promote bone regeneration by targeting GATA2

Author:

Luo Xin1,Meng Chunxiu1,Zhang Yujue1,Du Qicui1,Hou Caiyao2,Qiang Huifen2,Liu Kun1,Lv Zhaoyong1,Li Jun1,Liu Fengzhen1ORCID

Affiliation:

1. Biomaterials Laboratory, Liaocheng People’s Hospital, Liaocheng Hospital affiliated to Shandong First Medical University , Liaocheng 252000, China

2. Department of Materials Science and Engineering, Liaocheng University , Liaocheng 252000, China

Abstract

Abstract Bone immune responses based on macrophages are critical in the osteogenesis of bone abnormalities. In general, M2 macrophage facilitate the promotion of osteogenesis, as well, M1 macrophage play an important role in early bone healing, as confirmed by previous studies. However, it is not clear how M1 macrophage are involved in the bone immune response. MiR-21a-5p is a highly expressed microRNA in M1 macrophage in contrast to M2. Therefore, the current work sought to ascertain the influence of M1 macrophage on bone healing via exosomal miR-21a-5p and the probable mechanism. We discovered that injecting M1 macrophage exosomes overexpressing miR-21a-5p into bone defect locations enhanced bone regeneration in vivo. Furthermore, by directly targeting GATA2, miR-21a-5p accelerated MC3T3-E1 osteogenic differentiation. Our findings showed that exosomal miR-21a-5p from M1 macrophage may be transported to osteoblasts and target GATA2 to enhance bone defect healing.

Funder

Science Foundation of Shandong Province of China

Publisher

Oxford University Press (OUP)

Subject

Biomaterials

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