胸腺肽-β4在小鼠卵母细胞和早期胚胎中的表达与分布规律
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Expression and Distribution of Thymosin-β4 in Mouse Oocytes and Early Embryos
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    摘要:

    胸腺肽-β4(thymosin-β4,Tb4)是一种重要的 G-actin遮蔽因子(G-actin sequestering factor),在细胞微丝活动中有着调节G-actin活性的作用. 以往报道证实了Tb4在细胞中具有广泛的生理作用,但其在哺乳动物卵母细胞成熟和早期胚胎发育等方面的作用,迄今还没有系统的研究报道. 以昆明白小鼠卵巢、卵母细胞和早期胚胎作为实验材料,以免疫( 荧光) 组织化学和RT-PCR技术为主要研究方法,对Tb4的表达与分布进行了研究. 结果显示,Tb4在相关发育过程中,存在差异性的表达和定位变化.结果表明,在小鼠卵母细胞成熟和早期胚胎的发育过程,Tb4能够通过表达与分布的变化对细胞微丝活动和细胞增殖活动进行调控,对小鼠卵母细胞成熟、早期胚胎发育以及胚胎着床过程有重要的作用.

    Abstract:

    Thymosin-β4 (thymosin-β4, Tb4) is an important G-actin sequestering factor in cells, which could regulate the activity of G-actin in various microfilaments events. Previously, many researches have reported that Tb4 has broad cellular and physiological functions, but until now, there is lack of systematic research on mammal oocytes and early embryonic development. Tb4 is a small hydrophilic peptide, initially, which separated and purified from bovine thymus component Ⅴ, with a molecular mass of 5 ku, and compose of 43 amino acid residues. Tb4 molecule is highly conservative, which has been founded in a variety of tissues and organs in vertebrates, and also exists in part invertebrates. This peptide has extensive biological functions. Recent studies have shown that it closely relate with many physiological and pathological activities, such as immune regulation, neurological development, wound healing , inflammatory response, angiogenesis, apoptosis, tumor occurrence and migration. Dynamic events of microfilaments in cells always accompany with G-actin activity, while Tb4 could bind G-actin with a ratio of 1∶1 to inhibit G-actin to polymerize into microfilaments. In cells, nearly half of G-actin are bound with various of sequestering factors, which effects on both G-actin activity regulation and its reservation, while Tb4 is the chief executer of G-actin sequestering factor family. The ovaries, oocytes and early embryos of Kunming mouse was used to investigate the expression and distribution of Tb4 in oocytes and eary embryos. During the experiment, the immuno-histochemistry, immuno-fluorescence-histochemistry and RT-PCR technique were utilized as chief study methods. The discipline of Tb4 expression and distribution in oocytes maturation and early embryonic development were studied both in vivo and vitro. The results showed that Tb4 were different in expression and localization during mouse oocytes maturation and early embryonic development. Immuno-histochemistry results illustrated that, accompany with follicle growing, the expression amount of Tb4 peptide in vitro oocytes is gradually increased. There are different distribution characteristics of Tb4 in GV stage oocytes, which featured by chromatin configuration, such as divided the configuration into NSN, pNSN and SN type. In other stages of oocytes maturation and early embryonic development, Tb4 could locate both in nuclear and cytoplasm, and the expression amount always changing regularly, which are closely related with cells growing status and the cell cycle. AIOD value of Tb4 was not significantly different in the process of oocytes maturation in vivo, but the fluorescence intensity rapidly increased form 8-cell embryos to blastula stages in the process of embryonic development. The tendency of Tb4 mRNA transcription are similar to the peptide expression in those stages. Specifically, in early implantation blastula, Tb4 peptide highly expresses in implanted lateral cells of blastula, indicating that Tb4 can regulate the microfilaments depolymerization in embryos implantation, so Tb4 plays an important role in the process of embryos implantation. The research concluded that, Tb4 could regulate microfilaments events (such as polymerization and depolymerization) and proliferation of cells in the developmental processes through the changes of its expression and localization. Overall, Tb4 plays an important role for mouse oocytes maturation, early embryonic development and embryos implantation.

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张岩,李树蜂,杨彩荣,郑可佳,李宁,严云勤.胸腺肽-β4在小鼠卵母细胞和早期胚胎中的表达与分布规律[J].生物化学与生物物理进展,2009,36(9):1193-1201

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  • 收稿日期:2009-01-16
  • 最后修改日期:2009-03-16
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  • 在线发布日期: 2009-03-30
  • 出版日期: 2009-09-20