FKBP5 Regulates the Osteogenesis of Human Adipose-derived Mesenchymal Stem Cells.

IF 2 4区医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL Current Medical Science Pub Date : 2024-11-26 DOI:10.1007/s11596-024-2941-8

Xiao-Yu Tian, Biao Zhu, Wen-Can Fang, Xiang-Bin Zhou, Ning Wu, Hong Li, Ning Wen, Jin Li

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Abstract

Objective: Human adipose-derived stem cells (ASCs) have shown considerable potential for tissue regeneration. FK506 binding protein (FKBP) 5 is a cochaperone of several proteins. The purpose of this work was to explore the function of FKBP5 in ASC osteogenesis.

Methods: Lentivirus infection was used to overexpress or knock down FKBP5 in ASCs. To inhibit FKBP5, SAFit2, a specific inhibitor of FKBP5, was used. Next, the osteogenic capacity of ASCs was evaluated via alkaline phosphatase (ALP) staining, and extracellular calcium precipitation was detected via Alizarin red S staining. The binding proteins of FKBP5 were assessed via proteomics and validated via coimmunoprecipitation experiments.

Results: Following osteogenic induction, FKBP5 expression increased at both the mRNA and protein levels. Interestingly, FKBP5 upregulation by lentivirus infection increased the ability of ASCs to differentiate into osteoblasts, as revealed by ALP staining, while ALP activity also increased. Moreover, increased extracellular calcium precipitation confirmed that FKBP5 overexpression promoted ASC osteogenesis into osteocytes. On the other hand, FKBP5 knockdown or functional suppression with SAFit2 decreased this process. Furthermore, the proteomics and coimmunoprecipitation data demonstrated that FKBP5 bound to a variety of proteins in ASCs. These proteins serve as the molecular chaperone base upon which the osteogenesis-regulating activity of FKBP5 rests.

Conclusion: Our study revealed that FKBP5 enhances the osteogenesis of ASCs, providing a feasible method for clinical bone tissue engineering applications.

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FKBP5 调控人脂肪间充质干细胞的成骨过程

目的：人类脂肪源性干细胞（ASCs）在组织再生方面具有相当大的潜力。FK506结合蛋白（FKBP）5是多种蛋白质的辅伴侣蛋白。本研究旨在探索FKBP5在ASC成骨过程中的功能：方法：利用慢病毒感染在ASCs中过表达或敲除FKBP5。为了抑制FKBP5，使用了FKBP5的特异性抑制剂SAFit2。接着，通过碱性磷酸酶（ALP）染色评估了ASCs的成骨能力，并通过茜素红S染色检测了细胞外钙沉淀。通过蛋白质组学评估了FKBP5的结合蛋白，并通过共沉淀实验进行了验证：结果：成骨诱导后，FKBP5在mRNA和蛋白质水平上的表达均有所增加。有趣的是，慢病毒感染上调FKBP5后，ALP染色显示ASCs分化成成骨细胞的能力增强，同时ALP活性也提高了。此外，细胞外钙沉淀的增加证实了FKBP5的过表达促进了ASC成骨细胞的形成。另一方面，敲除 FKBP5 或使用 SAFit2 进行功能抑制则会减少这一过程。此外，蛋白质组学和共沉淀数据表明，FKBP5 与 ASCs 中的多种蛋白质结合。这些蛋白是FKBP5调节成骨活性的分子伴侣基础：结论：我们的研究发现，FKBP5能增强ASCs的成骨能力，为临床骨组织工程应用提供了一种可行的方法。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Current Medical Science Biochemistry, Genetics and Molecular Biology-Genetics

CiteScore

4.70

自引率

0.00%

发文量

126

期刊介绍： Current Medical Science provides a forum for peer-reviewed papers in the medical sciences, to promote academic exchange between Chinese researchers and doctors and their foreign counterparts. The journal covers the subjects of biomedicine such as physiology, biochemistry, molecular biology, pharmacology, pathology and pathophysiology, etc., and clinical research, such as surgery, internal medicine, obstetrics and gynecology, pediatrics and otorhinolaryngology etc. The articles appearing in Current Medical Science are mainly in English, with a very small number of its papers in German, to pay tribute to its German founder. This journal is the only medical periodical in Western languages sponsored by an educational institution located in the central part of China.