A bioactive material with dual integrin-targeting ligands regulates specific endogenous cell adhesion and promotes vascularized bone regeneration in adult and fetal bone defects

一种具有双重整合素靶向配体的生物活性材料,可调节特定的内源性细胞黏附,并促进成人和胎儿骨缺损部位的血管化骨再生。

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作者:Dake Hao ,Ruiwu Liu ,Tomas Gonzalez Fernandez ,Christopher Pivetti ,Jordan Elizabeth Jackson ,Edwin Samuel Kulubya ,Hong-Jiang Jiang ,Hai-Yang Ju ,Wen-Liang Liu ,Alyssa Panitch ,Kit S Lam ,J Kent Leach ,Diana L Farmer ,Aijun Wang

Abstract

Significant progress has been made in designing bone materials capable of directing endogenous cells to promote vascularized bone regeneration. However, current strategies lack regulation of the specific endogenous cell populations for vascularized bone regeneration, thus leading to adverse tissue formation and decreased regenerative efficiency. Here, we engineered a biomaterial to regulate endogenous cell adhesion and promote vascularized bone regeneration. The biomaterial works by presenting two synthetic ligands, LLP2A and LXW7, explicitly targeting integrins α4β1 and αvβ3, respectively, expressed on the surfaces of the cells related to bone formation and vascularization, such as mesenchymal stem cells (MSCs), osteoblasts, endothelial progenitor cells (EPCs), and endothelial cells (ECs). In vitro, the LLP2A/LXW7 modified biomaterial improved the adhesion of MSCs, osteoblasts, EPCs, and ECs via integrin α4β1 and αvβ3, respectively. In an adult rat calvarial bone defect model, the LLP2A/LXW7 modified biomaterial enhanced bone formation and vascularization by synergistically regulating endogenous cells with osteogenic and angiogenic potentials, such as DLX5+ cells, osteocalcin+ cells, CD34+/CD45- cells and CD31+ cells. In a fetal sheep spinal bone defect model, the LLP2A/LXW7 modified biomaterial augmented bone formation and vascularization without any adverse effects. This innovative biomaterial offers an off-the-shelf, easy-to-use, and biologically safe product suitable for vascularized bone regeneration in both fetal and adult disease environments. Keywords: Adult and fetal bone defects; Bone formation; Endogenous stem cells; Integrin-based ligands; Vascularization.

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