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Low-dose nicotine reduces the homing ability of murine BMSCs during fracture healing

机译:小剂量尼古丁降低骨折愈合过程中小鼠骨髓间充质干细胞的归巢能力

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摘要

Wound and fracture healing are affected by exposure to nicotine and other compounds in cigarettes. This study examined the effects of exposure to low-dose nicotine at sub-toxic concentrations on the proliferation, differentiation and migration of bone marrow stem cells (BMSCs) in vitro and their homing to fracture site in C57BL/6 mice. BMSCs were investigated in cells treated with or without nicotine (1 μM to 1 mM). Different concentrations of nicotine exhibited varied effects on BMSCs growth regulation and bone differentiation. CCK8 test significantly increased at a high nicotine concentration of 1 mM while calcium nodule staining with Alizarin red decreased at the same concentration. In vitro scratch test, Transwell tests and in vivo BMSCs homing tests showed negative effects on BMSCs migration at 10 μM to 1 mM nicotine test. Real-time PCR analysis revealed the down-regulation of SDF-1, CXCR4 and CXCR7, which were members of the potent chemotactic signaling system. Western blot analysis indicated the down-regulated expression levels of periostin expressed by nicotine-treated osteoblasts (1 μM to 100 μM). Micro CT results showed that nicotine delayed the fracture healing in mice. Our data suggest that exposure to low-dose nicotine concentrations may affect bone formation by inhibiting the migration and homing of BMSCs, which may be an important risk factor for bone healing delay in smoking patients.
机译:接触香烟中的尼古丁和其他化合物会影响伤口和骨折的愈合。这项研究检查了在亚毒性浓度下暴露于低剂量尼古丁对C57BL / 6小鼠体外骨髓干细胞(BMSCs)增殖,分化和迁移及其归巢至骨折部位的影响。在用或不用烟碱(1μM至1 mM)处理的细胞中研究了BMSC。不同浓度的尼古丁对BMSCs的生长调节和骨分化表现出不同的影响。在1 mM的高烟碱浓度下,CCK8测试显着增加,而在相同浓度下,用茜素红对钙结节的染色减少。体外划痕测试,Transwell测试和体内BMSCs归巢测试显示,在10μM到1 mM的尼古丁测试中,对BMSCs迁移具有负面影响。实时PCR分析显示,SDF-1,CXCR4和CXCR7被下调,它们是有效趋化信号系统的成员。 Western印迹分析表明,尼古丁处理的成骨细胞表达的骨膜素表达水平下调(1μM至100μM)。 Micro CT结果表明,尼古丁延缓了小鼠的骨折愈合。我们的数据表明,低剂量尼古丁浓度的暴露可能会通过抑制BMSC的迁移和归巢而影响骨骼形成,而BMSC可能是吸烟患者骨骼愈合延迟的重要危险因素。

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