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Gene Expression Analysis of Zebrafish Heart Regeneration

机译:斑马鱼心脏再生的基因表达分析

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摘要

Mammalian hearts cannot regenerate. In contrast, zebrafish hearts regenerate even when up to 20% of the ventricle is amputated. The mechanism of zebrafish heart regeneration is not understood. To systematically characterize this process at the molecular level, we generated transcriptional profiles of zebrafish cardiac regeneration by microarray analyses. Distinct gene clusters were identified based on temporal expression patterns. Genes coding for wound response/inflammatory factors, secreted molecules, and matrix metalloproteinases are expressed in regenerating heart in sequential patterns. Comparisons of gene expression profiles between heart and fin regeneration revealed a set of regeneration core molecules as well as tissue-specific factors. The expression patterns of several secreted molecules around the wound suggest that they play important roles in heart regeneration. We found that both platelet-derived growth factor-a and -b (pdgf-a and pdgf-b) are upregulated in regenerating zebrafish hearts. PDGF-B homodimers induce DNA synthesis in adult zebrafish cardiomyocytes. In addition, we demonstrate that a chemical inhibitor of PDGF receptor decreases DNA synthesis of cardiomyocytes both in vitro and in vivo during regeneration. Our data indicate that zebrafish heart regeneration is associated with sequentially upregulated wound healing genes and growth factors and suggest that PDGF signaling is required.
机译:哺乳动物的心灵无法再生。相反,即使截断了20%的心室,斑马鱼的心脏也会再生。斑马鱼心脏再生的机制尚不清楚。为了在分子水平上系统表征该过程,我们通过微阵列分析产生了斑马鱼心脏再生的转录谱。基于时间表达模式鉴定了不同的基因簇。编码伤口反应/炎症因子,分泌分子和基质金属蛋白酶的基因在再生心脏中以顺序模式表达。心脏和鳍再生之间基因表达谱的比较揭示了一组再生核心分子以及组织特异性因子。伤口周围几种分泌分子的表达模式表明它们在心脏再生中起重要作用。我们发现血小板源性生长因子-a和-b(pdgf-a和pdgf-b)在再生斑马鱼心脏中均被上调。 PDGF-B同型二聚体诱导成年斑马鱼心肌细胞中的DNA合成。此外,我们证明了PDGF受体的化学抑制剂可降低再生过程中体外和体内心肌细胞的DNA合成。我们的数据表明斑马鱼心脏再生与顺序上调的伤口愈合基因和生长因子有关,并提示需要PDGF信号传导。

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