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首页> 外文期刊>American Journal of Physiology >Transcription repression and blocks in cell cycle progression in hypoplastic left heart syndrome
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Transcription repression and blocks in cell cycle progression in hypoplastic left heart syndrome

机译:复杂左心综合征中细胞周期进展中的转录抑制和障碍

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Hypoplastic left heart syndrome (HLHS) is characterized by abnormally developed atrial septum and a severe underdevelopment of the left side of the heart. Despite significant advances in its surgical management, little is known about the molecular abnormalities in this syndrome. To gain molecular insights into HLHS, expression profiling by gene-chip microarray (Affymetrix U133 2.0) and by real-time RT-PCR was performed in the atrial septum of patients diagnosed with HLHS and compared with age-matched non-HLHS patients. Hierarchical clustering of all expressed genes with a P < 0.01 of all tissue samples showed two main clusters, one of HLHS and the other of non-HLHS, suggesting different expression patterns by the two groups. Net affix followed by real-time RT-PCR analysis identified the differentially expressed genes to be those involved in chromatin remodeling, cell cycle regulation, and transcriptional regulation. These included remodeling factors, histone deactylase 2 and SET and MYND domain containing 1; transcription factors, FoxP1, and components of the calcineurin-nuclear factor of activated T cells signaling pathway; and cell cycle regulators, cyclin-dependent kinase (CDK)-4, phosphatase and tensin homolog, and p18. Since these factors play essential roles in heart growth and development, the abnormal expression pattern suggests that these molecules may contribute to the pathogenesis of HLHS.
机译:Hypoplastic左心综合征(HLH)的特征是异常发育的心房隔膜和心脏左侧的严重欠发电。尽管其外科管理有重大进展,但对该综合征中的分子异常知之甚少。为了获得HLH的分子见解,在诊断HLHS患者的心房隔膜中进行基因芯片微阵列(Affymetrix U133 2.0)和实时RT-PCR的表达分析,并与年龄匹配的非HLHS患者进行比较。所有表达基因的所有表达基因的所有表达基因的所有组织样品都显示出两个主要簇,其中一个HLH和其他非HLH,表明两组的不同表达模式。然后净粘合后,实时RT-PCR分析将差异表达基因鉴定为参与染色质重塑,细胞周期调节和转录调节的那些。这些包括重塑因子,组蛋白去庚糖酶2和含有1的组和MyND结构域;转录因子,Foxp1和钙霉素 - 活化T细胞信号通路核因子的组分;和细胞周期调节剂,细胞周期蛋白依赖性激酶(CDK)-4,磷酸酶和三素同源物和P18。由于这些因素在心脏生长和发育中起重要作用,因此异常表达模式表明这些分子可能有助于HLH的发病机制。

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