Movassagh Mehregan, Philpott Anna
Department of Oncology, University of Cambridge, Hutchison/MRC Research Centre, Addenbrooke's Hospital, Hills Road, Cambridge CB2 2XZ, UK.
Cardiovasc Res. 2008 Aug 1;79(3):436-47. doi: 10.1093/cvr/cvn105. Epub 2008 Apr 27.
Cyclin-dependent kinase inhibitors (CDKIs) play a critical role in negatively regulating the proliferation of cardiomyocytes, although their role in cardiac differentiation remains largely undetermined. We have shown that the most prominent CDKI in Xenopus, p27(Xic1)(Xic1), plays a role in neuronal and myotome differentiation beyond its ability to arrest the cell cycle. Thus, we investigated whether it plays a similar role in cardiomyocyte differentiation.
Xenopus laevis embryos were sectioned, and whole-mount antibody staining and immunofluorescence studies were carried out to determine the total number and percentage of differentiated cardiomyocytes in mitosis. Capped RNA and/or translation-blocking Xic1 morpholino antisense oligonucleotides (Xic1Mo) were microinjected into embryos, and their role on cardiac differentiation was assessed by in situ hybridization and/or PCR. We show that cell-cycling post-gastrulation is not essential for cardiac differentiation in Xenopus embryos, and conversely that some cells can express markers of cardiac differentiation even when still in cycle. A targeted knock-down of Xic1 protein by Xic1Mo microinjection decreases the expression of markers of cardiac differentiation, which can be partially rescued by co-injection of full-length Xic1 RNA, demonstrating that Xic1 is essential for heart formation. Furthermore, using deleted and mutant forms of Xic1, we show that neither its abilities to inhibit the cell cycle nor the great majority of CDK kinase activity are essential for Xic1's function in cardiomyocyte differentiation, an activity that resides in the N-terminus of the molecule.
Altogether, our results demonstrate that the CDKI Xic1 is required in Xenopus cardiac differentiation, and that this function is localized at its N-terminus, but it is distinct from its ability to arrest the cell cycle and inhibit overall CDK kinase activity. Hence, these results suggest that CDKIs play an important direct role in driving cardiomyocyte differentiation in addition to cell-cycle regulation.
细胞周期蛋白依赖性激酶抑制剂(CDKIs)在负向调节心肌细胞增殖中起关键作用,尽管它们在心脏分化中的作用仍 largely 未确定。我们已经表明,非洲爪蟾中最突出的 CDKI,p27(Xic1)(Xic1),在神经元和肌节分化中发挥作用,超出了其阻止细胞周期的能力。因此,我们研究了它在心肌细胞分化中是否发挥类似作用。
将非洲爪蟾胚胎切片,并进行整体抗体染色和免疫荧光研究,以确定有丝分裂中分化心肌细胞的总数和百分比。将加帽 RNA 和/或翻译阻断型 Xic1 吗啉代反义寡核苷酸(Xic1Mo)显微注射到胚胎中,并通过原位杂交和/或 PCR 评估它们对心脏分化的作用。我们表明,原肠胚形成后的细胞周期循环对于非洲爪蟾胚胎中的心脏分化不是必需的,相反,一些细胞即使仍处于细胞周期中也可以表达心脏分化标志物。通过 Xic1Mo 显微注射靶向敲低 Xic1 蛋白会降低心脏分化标志物的表达,通过共注射全长 Xic1 RNA 可以部分挽救这种情况,表明 Xic1 对于心脏形成至关重要。此外,使用 Xic1 的缺失和突变形式,我们表明其抑制细胞周期的能力和绝大多数 CDK 激酶活性对于 Xic1 在心肌细胞分化中的功能都不是必需的,这种活性位于分子的 N 端。
总之,我们的结果表明,CDKI Xic1 在非洲爪蟾心脏分化中是必需的,并且这种功能定位于其 N 端,但它与其阻止细胞周期和抑制整体 CDK 激酶活性的能力不同。因此,这些结果表明,CDKIs 除了细胞周期调节外,在驱动心肌细胞分化中还起重要的直接作用。
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