A novel biologically hierarchical hydrogel with osteoblast precursor‐targeting extracellular vesicles ameliorates bone loss in vivo via the sequential action of antagomiR‐200b‐3p and antagomiR‐130b‐3p

Author:

Dai Hanhao1,Yu Yunlong12,Han Junyong3,Luo Jun2,Song Chao1,Deng Zhibo1,Wu Yijing1,Ke Dianshan12,Xu Jie12

Affiliation:

1. Shengli Clinical Medical College of Fujian Medical University Fuzhou China

2. Department of Orthopedics Fujian Provincial Hospital, Fujian Medical University Fuzhou China

3. Institute for Immunology, Fujian Academy of Medical Sciences Fuzhou China

Abstract

AbstractOsteoporotic fracture is a major health problem plaguing the ageing society, and improving its treatment is an urgent challenge. How to ameliorate bone loss determines the recovery of such fractures. Extracellular vesicle (EV)‐loaded hydrogel has the capacity to treat osteoporotic fractures due to its pro‐osteogenic property. And balancing proliferation and maturation of osteoblast precursors (OBPs) is of great significance to avoid OBP depletion, which is lacking in current treatment. Based on osteoblastogenic miRNAs, this study aimed to explore the efficacies of the combination of hierarchical hydrogel and EVs altering functional miRNAs level in bone loss. Through bioinformatics analyses, we screened out proliferative gene‐targeting miR‐200b‐3p and osteogenic gene‐targeting miR‐130b‐3p. And antagomiR‐200b‐3p (ant‐200b) enhanced OBP proliferation, and antagomiR‐130b‐3p (ant‐130b) promoted OBP differentiation. After confirming the directional effect of Fibronectin (Fn1) on OBPs, we prepared OBP‐targeting EVs. Furthermore, encapsulation of two antagomiRNAs in EVs enhanced the respective effect of ant‐200b and ant‐130b. Notably, hierarchically injectable hydrogel exerted an effective function in promoting the sequential delivery of EVs‐200b and EVs‐130b. Importantly, hierarchical hydrogel containing dual EVs effectively ameliorated bone loss. Overall, hierarchical hydrogel based on two antagomiRNAs effectively improves bone loss in vivo due to its role in promoting OBP proliferation and maturation sequentially.

Publisher

Wiley

Subject

Cell Biology,General Medicine

Reference55 articles.

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