Cellular Biology Section, Cardiothoracic Surgery Research Program, National Heart Lung and Blood Institute, National Institutes of Health, Bethesda, MD 20892, USA.
Cellular Biology Section, Cardiothoracic Surgery Research Program, National Heart Lung and Blood Institute, National Institutes of Health, Bethesda, MD 20892, USA.
Exp Cell Res. 2014 Apr 15;323(1):56-65. doi: 10.1016/j.yexcr.2014.02.015. Epub 2014 Feb 27.
Studying the proliferative ability of human bone marrow derived mesenchymal stem cells in hypoxic conditions can help us achieve the effective regeneration of ischemic injured myocardium. Cardiac-type fatty acid binding protein (FABP3) is a specific biomarker of muscle and heart tissue injury. This protein is purported to be involved in early myocardial development, adult myocardial tissue repair and responsible for the modulation of cell growth and proliferation. We have investigated the role of FABP3 in human bone marrow derived mesenchymal stem cells under ischemic conditions. MSCs from 12 donors were cultured either in standard normoxic or modified hypoxic conditions, and the differential expression of FABP3 was tested by quantitative (RT)PCR and western blot. We also established stable FABP3 expression in MSCs and searched for variation in cellular proliferation and differentiation bioprocesses affected by hypoxic conditions. We identified: (1) the FABP3 differential expression pattern in the MSCs under hypoxic conditions; (2) over-expression of FABP3 inhibited the growth and proliferation of the MSCs; however, improved their survival in low oxygen environments; (3) the cell growth factors and positive cell cycle regulation genes, such as PCNA, APC, CCNB1, CCNB2 and CDC6 were all down-regulated; while the key negative cell cycle regulation genes TP53, BRCA1, CASP3 and CDKN1A were significantly up-regulated in the cells with FABP3 overexpression. Our data suggested that FABP3 was up-regulated under hypoxia; also negatively regulated the cell metabolic process and the mitotic cell cycle. Overexpression of FABP3 inhibited cell growth and proliferation via negative regulation of the cell cycle and down-regulation of cell growth factors, but enhances cell survival in hypoxic or ischemic conditions.
研究低氧条件下骨髓间充质干细胞的增殖能力有助于实现缺血性损伤心肌的有效再生。心脏型脂肪酸结合蛋白(FABP3)是肌肉和心脏组织损伤的特异性生物标志物。该蛋白据称参与早期心肌发育、成人心肌组织修复,并负责调节细胞生长和增殖。我们研究了 FABP3 在缺血条件下对人骨髓间充质干细胞的作用。将来自 12 个供体的 MSC 在标准常氧或改良低氧条件下培养,并通过定量(RT)PCR 和 Western blot 测试 FABP3 的差异表达。我们还在 MSC 中建立了稳定的 FABP3 表达,并寻找受低氧条件影响的细胞增殖和分化生物过程的变化。我们确定:(1)MSC 在低氧条件下的 FABP3 差异表达模式;(2)FABP3 的过表达抑制 MSC 的生长和增殖,但改善了它们在低氧环境中的存活;(3)细胞生长因子和阳性细胞周期调节基因,如 PCNA、APC、CCNB1、CCNB2 和 CDC6 均下调;而 FABP3 过表达的细胞中关键的负细胞周期调节基因 TP53、BRCA1、CASP3 和 CDKN1A 则显著上调。我们的数据表明 FABP3 在低氧下上调;还负调控细胞代谢过程和有丝分裂细胞周期。FABP3 的过表达通过负调控细胞周期和下调细胞生长因子来抑制细胞生长和增殖,但增强细胞在低氧或缺血条件下的存活。