microRNA-1 Induces Transdifferentiation of Peripheral Blood CD34+ Cells into Cardiomyocytes-like Cells

B. S. Pikir, A. Andrianto, I. G. Suryawan, H. Hermawan, Dian Paramita Kartikasari, P. M. Harsoyo
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Abstract

BACKGROUND: Transdifferentiation is a method to provide cells sources for cellular cardiomyoplasty. CD34+ cells are potential cells sources because these cells can differentiate into cardiomyocytes through several mechanisms. MicroRNA (miR-1) is known to have the ability to inhibit the expression of histone deacetylase 4 (HDAC4). HDAC4 is a gene that essentially contributes in cardiomyocytes differentiation. However, the study reporting an evidence that miR-1 can induce transdifferentiation of CD34+ peripheral blood cells into mature cardiomyocytes is limited.METHODS: CD34+ cells were taken from peripheral blood and isolated using a magnetic-activated cell sorting (MACS) method in vitro. Mature mimics of miR-1 were transfected into isolated CD34+ cells and then incubated for 48 hours for quantification of HDAC4 mRNA using reverse transcription-quantitative polymerase chain reaction (RT-qPCR). On the fifth day after miR-1 transfection, cardiomyocyte-like cells were identified based on their morphology and cardiac troponin expression using immunocytochemistry.RESULTS: Transfection of miR-1 in CD34+ isolated cells decreased HDAC4 gene expression by -0.54 fold at second day and caused a significant increase in percentage of cardiac troponin positive cells (median: 31.34; p<0.05) at fifth-day post-transfection. The efficiency of transdifferentiation was 32%. The miR-1 transfection had a significant negative relationship with HDAC4 gene expression (B=-1.000; p=0.001). HDAC4 gene expression had a negative and significant relationship with the percentage of cardiac troponin-positive cells (B=-0.701; p=0.001).CONCLUSION: This study suggests that miR-1 can induce transdifferentiation of peripheral blood CD34+ cells into cardiomyocytes-like cells by decreasing HDAC4 gene expression.KEYWORDS: transdifferentiation, microRNA-1, CD34, cardiomyocyte, HDAC4
microRNA-1诱导外周血CD34+细胞向心肌细胞样细胞的转分化
背景:转分化是一种为细胞心肌成形术提供细胞来源的方法。CD34+细胞是潜在的细胞来源,因为这些细胞可以通过几种机制分化为心肌细胞。已知MicroRNA (miR-1)具有抑制组蛋白去乙酰化酶4 (HDAC4)表达的能力。HDAC4是一种主要参与心肌细胞分化的基因。然而,报道miR-1可以诱导CD34+外周血细胞转分化为成熟心肌细胞的证据的研究是有限的。方法:从外周血中提取CD34+细胞,采用磁激活细胞分选(MACS)法进行体外分离。将成熟的miR-1模拟物转染到离体CD34+细胞中,培养48小时,用逆转录-定量聚合酶链反应(RT-qPCR)定量HDAC4 mRNA。转染miR-1后第5天,利用免疫细胞化学方法鉴定心肌细胞样细胞的形态和心肌肌钙蛋白的表达。结果:转染miR-1后,第2天HDAC4基因表达降低-0.54倍,心肌肌钙蛋白阳性细胞比例显著增加(中位数:31.34;P <0.05)。转分化效率为32%。miR-1转染与hdac - 4基因表达呈显著负相关(B=-1.000;p = 0.001)。hdac - 4基因表达与心肌肌钙蛋白阳性细胞比例呈显著负相关(B=-0.701;p = 0.001)。结论:本研究提示miR-1可通过降低HDAC4基因表达诱导外周血CD34+细胞向心肌细胞样细胞转分化。关键词:转分化,microRNA-1, CD34,心肌细胞,HDAC4
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