Mechanical induction of osteoanabolic Wnt1 promotes osteoblast differentiation via Plat

运行x2 Wnt信号通路 成骨细胞 基因敲除 下调和上调 基因沉默 小干扰RNA 刺激 化学 细胞生物学 内分泌学 癌症研究 内科学 信号转导 医学 生物 转染 生物化学 基因 体外
作者
Mubashir Ahmad,Melanie Haffner‐Luntzer,Astrid Schoppa,Zeynab Najafova,Teodora Lukic,Timur Yorgan,Michael Amling,Thorsten Schinke,Anita Ignatius
出处
期刊:The FASEB Journal [Wiley]
卷期号:38 (4) 被引量:1
标识
DOI:10.1096/fj.202301424rr
摘要

Abstract Physical activity‐induced mechanical stimuli play a crucial role in preserving bone mass and structure by promoting bone formation. While the Wnt pathway is pivotal for mediating the osteoblast response to loading, the exact mechanisms are not fully understood. Here, we found that mechanical stimulation induces osteoblastic Wnt1 expression, resulting in an upregulation of key osteogenic marker genes, including Runx2 and Sp7 , while Wnt1 knockdown using siRNA prevented these effects. RNAseq analysis identified Plat as a major target through which Wnt1 exerts its osteogenic influence. This was corroborated by Plat depletion using siRNA, confirming its positive role in osteogenic differentiation. Moreover, we demonstrated that mechanical stimulation enhances Plat expression, which, in turn leads to increased expression of osteogenic markers like Runx2 and Sp7 . Notably, Plat depletion by siRNA prevented this effect. We have established that Wnt1 regulates Plat expression by activating β‐Catenin. Silencing Wnt1 impairs mechanically induced β‐Catenin activation, subsequently reducing Plat expression. Furthermore, our findings showed that Wnt1 is essential for osteoblasts to respond to mechanical stimulation and induce Runx2 and Sp7 expression, in part through the Wnt1/β‐Catenin/Plat signaling pathway. Additionally, we observed significantly reduced Wnt1 and Plat expression in bones from ovariectomy (OVX)‐induced and age‐related osteoporotic mouse models compared with non‐OVX and young mice, respectively. Overall, our data suggested that Wnt1 and Plat play significant roles in mechanically induced osteogenesis. Their decreased expression in bones from OVX and aged mice highlights their potential involvement in post‐menopausal and age‐related osteoporosis, respectively.
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