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Cytotoxicity of local anesthetics on rabbit adipose-derived mesenchymal stem cells during early chondrogenic differentiation

机译:局麻药对兔脂肪间充质干细胞早期成软骨分化过程的细胞毒性

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摘要

Local anesthetics (LAs) are commonly used to provide peri-operative pain control in the peripheral joints. In the field of regenerative medicine, adipose-derived mesenchymal stem cells (ADMSCs) are gaining attention as a cellular source for repair and regeneration in degenerative diseases. However, previous studies have demonstrated that the commonly used drugs lidocaine, ropivacaine, bupivacaine and mepivacaine may be toxic to human chondrocytes, which has raised concerns over whether they exert similar negative effects on ADMSCs during early chondrogenic differentiation. In the present in vitro study, the cytotoxicity of different LAs to ADMSCs was determined during early chondrogenic differentiation. At concentrations similar to those after physiological dilution once injected into the degenerative tissues, LAs (1% lidocaine, 0.5% bupivacaine, 0.5% ropivacaine or 2% mepivacaine) and PBS (control group) were incubated with rabbit ADMSCs (rADMSCs) for 60 min. Following further culture for 3 or 7 days, the cell viability, apoptosis and morphological alterations of chondrogenic differentiation were measured by determining the mitochondrial activity, by flow cytometric analysis, Safranine Fast Green double staining and reverse transcription-quantitative polymerase chain reaction of chondrogenesis-associated genes. The results indicated that the mitochondrial activity in rADMSC was decreased and the apoptotic rate was increased, following treatment with LAs (P<0.05). Lidocaine (1%) was less cytotoxic to rADMSCs during early chondrogenesis compared with other LAs. The expression levels of chondrogenesis-associated markers, including collagen I, collagen III and sex-determining region Y box 9 were all decreased at day 3 following exposure to LAs compared with the control group (P<0.05). The expression levels of these chondrogenesis-associated genes began to increase on day 7 following exposure but remained lower compared with the control group (P<0.05). Of note, 2% mepivacaine and 1% lidocaine exhibited a less pronounced negative effect on chondrogenesis-associated gene expression compared with other LAs. Therefore, the present study concluded that LAs are cytotoxic to rADMSCs during early chondrogenesis. Attention should be paid to the different types of LA selected in conjunction with ADMSC injection therapy.
机译:局部麻醉药(LAs)通常用于在周围关节中提供围手术期疼痛控制。在再生医学领域中,脂肪来源的间充质干细胞(ADMSC)作为退化性疾病的修复和再生的细胞来源正在受到关注。但是,以前的研究表明,常用的利多卡因,罗哌卡因,布比卡因和甲哌卡因对人的软骨细胞可能具有毒性,这引起了人们对它们在早期软骨形成分化过程中是否对ADMSC产生类似负面作用的担忧。在目前的体外研究中,在软骨形成的早期分化过程中确定了不同LA对ADMSC的细胞毒性。以与生理稀释液相同的浓度,一旦将其注射入变性组织后,将LAs(1%利多卡因,0.5%布比卡因,0.5%罗哌卡因或2%美比卡因)和PBS(对照组)与兔ADMSCs(rADMSCs)孵育60分钟。进一步培养3或7天后,通过测定线粒体活性,流式细胞仪分析,番红花Fast Green双重染色和与软骨形成相关的逆转录-定量聚合酶链反应,检测软骨形成的细胞活力,凋亡和形态变化。基因。结果表明,用LAs处理后,rADMSC中的线粒体活性降低,凋亡率增加(P <0.05)。与其他LA相比,利多卡因(1%)在早期软骨形成过程中对rADMSC的细胞毒性较小。与对照组相比,暴露于LAs后第3天,软骨生成相关标志物(包括胶原蛋白I,胶原蛋白III和性别决定区域Y框9)的表达水平均降低(P <0.05)。这些与软骨形成相关的基因的表达水平在暴露后第7天开始增加,但与对照组相比仍较低(P <0.05)。值得注意的是,与其他LAs相比,2%的甲哌卡因和1%的利多卡因对与软骨形成相关的基因表达的负面影响较小。因此,本研究得出结论,在早期软骨形成过程中,LAs对rADMSCs具有细胞毒性。应注意结合ADMSC注射疗法选择的不同类型的LA。

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