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In vivo tracking of histone H3 lysine 9 acetylation in Xenopus laevis during tail regeneration

机译:尾巴再生过程中非洲爪蟾中组蛋白H3赖氨酸9乙酰化的体内追踪

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摘要

Xenopus laevis tadpoles can completely regenerate their appendages, such as tail and limbs, and therefore provide a unique model to decipher the molecular mechanisms of organ regeneration in vertebrates. Epigenetic modifications are likely to be involved in this remarkable regeneration capacity, but they remain largely unknown. To examine the involvement of histone modification during organ regeneration, we generated transgenic X. laevis ubiquitously expressing a fluorescent modification-specific intracellular antibody (Mintbody) that is able to track histone H3 lysine 9 acetylation (H3K9ac) in vivo through nuclear enhanced green fluorescent protein (EGFP) fluorescence. In embryos ubiquitously expressing H3K9ac-Mintbody, robust fluorescence was observed in the nuclei of somites. Interestingly, H3K9ac-Mintbody signals predominantly accumulated in nuclei of regenerating notochord at 24h postamputation following activation of reactive oxygen species (ROS). Moreover, apocynin (APO), an inhibitor of ROS production, attenuated H3K9ac-Mintbody signals in regenerating notochord. Our results suggest that ROS production is involved in acetylation of H3K9 in regenerating notochord at the onset of tail regeneration. We also show this transgenic Xenopus to be a useful tool to investigate epigenetic modification, not only in organogenesis but also in organ regeneration.
机译:非洲爪蟾t可以完全再生其附属物,例如尾巴和四肢,因此提供了一个独特的模型来解释脊椎动物器官再生的分子机制。表观遗传修饰可能与这种显着的再生能力有关,但在很大程度上仍然未知。为了检查组蛋白修饰在器官再生过程中的参与,我们产生了转基因的X. laevis,广泛表达一种荧光修饰特异性细胞内抗体(Mintbody),该抗体能够通过核增强的绿色荧光蛋白在体内追踪组蛋白H3赖氨酸9乙酰化(H3K9ac)。 (EGFP)荧光。在普遍表达H3K9ac-Mintbody的胚胎中,在体核中观察到了强大的荧光。有趣的是,H3K9ac-Mintbody信号主要是在激活活性氧(ROS)后,在截肢后24h聚集在再生脊索的核中。此外,ROS抑制剂Apocynin(APO)在再生脊索肌中减弱了H3K9ac-Mintbody信号。我们的结果表明,在尾巴再生开始时,ROS的产生与H3K9的乙酰化有关,从而使脊索再生。我们还表明,这种转基因非洲爪蟾是研究表观遗传修饰的有用工具,不仅在器官发生中,而且在器官再生中也是如此。

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