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内皮祖细胞的动员:肌肉骨骼创伤的全身血管反应

Mobilization of endothelial precursor cells: systemic vascular response to musculoskeletal trauma.

作者信息

Laing A J, Dillon J P, Condon E T, Street J T, Wang J H, McGuinness A J, Redmond H P

机构信息

Departments of Surgical Research and Orthopaedic Surgery, Cork University Hospital, Cork, Ireland.

出版信息

J Orthop Res. 2007 Jan;25(1):44-50. doi: 10.1002/jor.20228.

Abstract

Postnatal vasculogenesis, the process by which vascular committed bone marrow stem cells or endothelial precursor cells (EPC) migrate, differentiate, and incorporate into the nacent endothelium contributing to physiological and pathological neovascularization, has stimulated much interest. Its contribution to tumor nonvascularization, wound healing, and revascularization associated with skeletal and cardiac muscles ischaemia is established. We evaluated the mobilization of EPCs in response to musculoskeletal trauma. Blood from patients (n = 15) following AO type 42a1 closed diaphyseal tibial fractures was analyzed for CD34 and AC133 cell surface marker expression. Immunomagnetically enriched CD34+ mononuclear cell (MNC(CD34+)) populations were cultured and examined for phenotypic and functional vascular endothelial differentiation. Circulating MNC(CD34+) levels increased sevenfold by day 3 postinjury. Circulating MNC(AC133+) increased 2.5-fold. Enriched MNC(CD34+) populations from day 3 samples in culture exhibited cell cluster formation with sprouting spindles. These cells bound UEA-1 and incorporated fluorescent DiI-Ac-LDL intracellularily. Our findings suggest a systemic provascular response is initiated in response to musculoskeletal trauma. Its therapeutic manipulation may have implications for the potential enhancement of fracture healing.

摘要

出生后血管生成是指血管定向骨髓干细胞或内皮祖细胞(EPC)迁移、分化并整合到新生内皮中,从而促进生理和病理新生血管形成的过程,这一过程已引起了广泛关注。其对肿瘤血管生成、伤口愈合以及与骨骼肌和心肌缺血相关的血管再生的作用已得到证实。我们评估了EPCs对肌肉骨骼创伤的反应。对15例AO 42a1型闭合性胫骨干骨折患者的血液进行分析,检测CD34和AC133细胞表面标志物的表达。对免疫磁珠富集的CD34 + 单核细胞(MNC(CD34+))群体进行培养,并检测其表型和功能性血管内皮分化情况。损伤后第3天,循环中的MNC(CD34+)水平增加了7倍。循环中的MNC(AC133+)增加了2.5倍。培养第3天样本中富集的MNC(CD34+)群体呈现出带有发芽纺锤体的细胞簇形成。这些细胞结合UEA-1并在细胞内摄取荧光DiI-Ac-LDL。我们的研究结果表明,针对肌肉骨骼创伤会引发全身性促血管反应。对其进行治疗性调控可能对潜在增强骨折愈合具有重要意义。

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