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Ion Cyclotron Resonance as a Tool in Regenerative Medicine

机译:离子回旋共振作为再生医学的工具

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The identification of suitable stem cell cultures and differentiating conditions that are free of xenogenic growth supplements is an important step in finding the clinical applicability of cell therapy in two important fields of human medicine: heart failure and bone remodeling, growth and repair. We recently demonstrated the possibility of obtaining cardiac stem cells (CSCs) from human endomyocardial biopsy specimens. CSCs self-assemble into multi-cellular clusters known as cardiospheres (CSps) that engraft and partially regenerate infarcted myocardium. CSps and cardiosphere-derived-cells (CDCs) were exposed for five days in an incubator regulated for temperature, humidity, and CO2 inside a solenoid system. This system was placed in a magnetically shielded room. The cells were exposed simultaneously to a static magnetic field (MF) and a parallel low-alternating frequency MF, close to the cyclotron frequency corresponding to the charge/mass ratio of the Ca++ ion. In this exposure condition, CSps and CDCs modulate their differentiation turning on cardiogenesis and turning off vasculogenesis. Cardiac markers such as troponin I (TnI) and myosin heavy chain (MHC) were up-regulated. Conversely, angiogenic markers such as vascular endothelial growth factor (VEGF) and kinase domain receptor (KDR) were down-regulated as evidenced by immunocytochemistry. Exposure to the 7 Hz calcium ion cyclotron resonance (ICR) frequency can modulate the cardiogenic vs. angiogenic differentiation process of ex vivo expanded CSCs. This may pave the way for novel approaches in tissue engineering and cell therapy. With regard to bone remodeling, it has been suggested that bone marrow-derived mesenchymal stem cells (MSC) may be considered as a potential therapeutic tool. Using the Ca++-dependent specific differentiation potential of the ELF-MF 7 Hz ICR, we show here that exposure of human MSC to these same MF conditions enhanced the expression of osteoblast differentiation markers such as alkaline phosphatase, osteocalcin, and osteopontin, as analyzed by real-time quantitative PCR, without affecting cell proliferation. As expected, while the differentiation marker factors were up regulated, the ICR electromagnetic field down regulated osteoprotegerin gene expression, a critical regulator of postnatal skeletal development and homeostasis in humans as well as mice.
机译:不含干细胞生长补充剂的合适干细胞培养物和分化条件的鉴定是在人类医学的两个重要领域中发现细胞疗法的临床适用性的重要步骤:心力衰竭和骨重塑,生长和修复。我们最近证明了从人类心肌内膜活检标本中获得心脏干细胞(CSC)的可能性。 CSC自组装成称为心球(CSps)的多细胞簇,这些簇会植入并部分再生梗死心肌。将CSps和心球来源的细胞(CDC)在电磁阀系统内调节温度,湿度和CO2的培养箱中暴露五天。该系统被放置在一个磁屏蔽室中。电池同时暴露于静磁场(MF)和平行的低交替频率MF,接近于与Ca ++离子的电荷/质量比相对应的回旋加速器频率。在这种暴露条件下,CSps和CDC会调节它们的分化,从而开启心脏生成并关闭血管生成。心肌标志物如肌钙蛋白I(TnI)和肌球蛋白重链(MHC)上调。相反,如免疫细胞化学所证明,血管生成标记例如血管内皮生长因子(VEGF)和激酶结构域受体(KDR)被下调。暴露于7 Hz钙离子回旋共振(ICR)频率可以调节离体扩增CSC的心源性与血管生成分化过程。这可能为组织工程和细胞治疗中的新方法铺平道路。关于骨重塑,已经提出骨髓来源的间充质干细胞(MSC)可以被认为是潜在的治疗工具。使用ELF-MF 7 Hz ICR的Ca ++依赖性特异性分化潜能,我们在这里显示,将人类MSC暴露于这些相同的MF条件下,可增强成骨细胞分化标志物(如碱性磷酸酶,骨钙素和骨桥蛋白)的表达,实时定量PCR,不影响细胞增殖。不出所料,虽然分化标记因子被上调,但ICR电磁场下调了骨保护素基因的表达,这是人以及小鼠出生后骨骼发育和体内稳态的关键调节器。

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