Targeting actin-bundling protein L-plastin as an anabolic therapy for bone loss.
Xiaoqun LiLipeng WangBiaotong HuangYanqiu GuYing LuoXin ZhiYan HuHao ZhangZhengrong GuJin CuiLiehu CaoJiawei GuoYajun WangQirong ZhouHao JiangChao FangWeizong WengXiaofei ChenXiao ChenXiaolong LiPublished in: Science advances (2020)
The actin-bundling protein L-plastin (LPL) mediates the resorption activity of osteoclasts, but its therapeutic potential in pathological bone loss remains unexplored. Here, we report that LPL knockout mice show increased bone mass and cortical thickness with more mononuclear tartrate-resistant acid phosphatase-positive cells, osteoblasts, CD31hiEmcnhi endothelial vessels, and fewer multinuclear osteoclasts in the bone marrow and periosteum. LPL deletion impeded preosteoclasts fusion by inhibiting filopodia formation and increased the number of preosteoclasts, which release platelet-derived growth factor-BB to promote CD31hiEmcnhi vessel growth and bone formation. LPL expression is regulated by the phosphatidylinositol 3-kinase/AKT/specific protein 1 axis in response to receptor activator of nuclear factor-κB ligand. Furthermore, we identified an LPL inhibitor, oroxylin A, that could maintain bone mass in ovariectomy-induced osteoporosis and accelerate bone fracture healing in mice. In conclusion, we showed that LPL regulates osteoclasts fusion, and targeting LPL serves as a novel anabolic therapy for pathological bone loss.
Keyphrases
- bone loss
- growth factor
- nuclear factor
- bone marrow
- binding protein
- toll like receptor
- signaling pathway
- protein protein
- amino acid
- mesenchymal stem cells
- protein kinase
- cancer therapy
- poor prognosis
- bone mineral density
- type diabetes
- cell proliferation
- endothelial cells
- postmenopausal women
- diabetic rats
- peripheral blood
- body composition
- high glucose
- cell migration
- adipose tissue
- oxidative stress
- hip fracture