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股骨来源的骨骼干细胞的特性及比较

The characterization and comparison of femoral bone-derived skeletal stem cells.

作者信息

Howard Kayla, Ferris William Frank, van de Vyver Mari

机构信息

Experimental Medicine Research Group, Department of Medicine, Faculty of Medicine and Health Sciences, Stellenbosch University, South Africa.

Experimental Medicine Research Group, Department of Medicine, Faculty of Medicine and Health Sciences, Stellenbosch University, South Africa.

出版信息

Biochimie. 2025 Jun;233:88-98. doi: 10.1016/j.biochi.2025.02.010. Epub 2025 Feb 27.

Abstract

Skeletal stem cells (SSCs) reside in various niche locations within long bones to maintain bone homeostasis and facilitate fracture repair. Bone fragility, associated with ageing, increases the susceptibility of the femoral head to fractures due to an increase in bone adipocytes and concomitant loss of structural integrity. However, the specific contribution of epiphyseal SSCs to fragility is unknown. To explore this, a comparative analysis was performed on the transcriptional profiles and lineage commitment of Wistar rat femoral SSCs derived from the bone marrow (BM-), diaphyseal cortical bone (CB-) and proximal epiphyseal trabecular bone (PF-SSCs) isolated from the same long bones. SSCs were characterized based on morphology, immunophenotype (CD90/CD45), growth rate (population doubling time), gene expression profiles and differentiation capacity (Oil Red O, Alizarin Red S). qRT-PCR micro-arrays were performed on SSCs to evaluate the expression of stemness, SSC and lineage-specific markers in both undifferentiated and differentiated states. Our findings support the hypothesis that SSCs from different bone regions exhibit distinct transcriptional profiles, reflecting their specific niche environments. CB-SSCs displayed superior osteogenic potential as evidenced by the expression of key osteogenic genes and higher levels of mineralization. In contrast, PF-SSCs had a reduced osteogenic capacity with a higher adipogenic potential. Overall, the study revealed the importance of niche-specific stem cell properties for use in regenerative medicine applications and provides insight into the potential role of PF-SSCs in bone fragility and fracture risk.

摘要

骨骼干细胞(SSCs)存在于长骨内的各种微环境位置,以维持骨稳态并促进骨折修复。与衰老相关的骨脆性增加,由于骨脂肪细胞增多和结构完整性随之丧失,使得股骨头更易发生骨折。然而,骨骺SSCs对骨脆性的具体作用尚不清楚。为了探究这一点,我们对从同一长骨分离出的Wistar大鼠股骨骨髓来源的SSCs(BM-SSCs)、骨干皮质骨来源的SSCs(CB-SSCs)和近端骨骺小梁骨来源的SSCs(PF-SSCs)的转录谱和谱系定向进行了比较分析。根据形态、免疫表型(CD90/CD45)、生长速率(群体倍增时间)、基因表达谱和分化能力(油红O、茜素红S)对SSCs进行了表征。对SSCs进行qRT-PCR微阵列分析,以评估未分化和分化状态下干性、SSC和谱系特异性标志物的表达。我们的研究结果支持以下假设:来自不同骨区域的SSCs表现出不同的转录谱,反映了它们特定的微环境。关键成骨基因的表达和更高水平的矿化表明CB-SSCs具有卓越的成骨潜力。相比之下,PF-SSCs的成骨能力降低,但具有更高的成脂潜力。总体而言,该研究揭示了微环境特异性干细胞特性在再生医学应用中的重要性,并深入了解了PF-SSCs在骨脆性和骨折风险中的潜在作用。

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