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The Unique Mechanisms of Cellular Proliferation Migration and Apoptosis are Regulated through Oocyte Maturational Development—A Complete Transcriptomic and Histochemical Study

机译:通过卵母细胞成熟发育来调节细胞增殖迁移和凋亡的独特机制-完整的转录组学和组织化学研究

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摘要

The growth and development of oocyte affect the functional activities of the surrounding somatic cells. These cells are regulated by various types of hormones, proteins, metabolites, and regulatory molecules through gap communication, ultimately leading to the development and maturation of oocytes. The close association between somatic cells and oocytes, which together form the cumulus-oocyte complexes (COCs), and their bi-directional communication are crucial for the acquisition of developmental competences by the oocyte. In this study, oocytes were extracted from the ovaries obtained from crossbred landrace gilts and subjected to in vitro maturation. RNA isolated from those oocytes was used for the subsequent microarray analysis. The data obtained shows, for the first time, variable levels of gene expression (fold changes higher than |2| and adjusted p-value < 0.05) belonging to four ontological groups: regulation of cell proliferation (GO:0042127), regulation of cell migration (GO:0030334), and regulation of programmed cell death (GO:0043067) that can be used together as proliferation, migration or apoptosis markers. We have identified several genes of porcine oocytes (ID2, VEGFA, BTG2, ESR1, CCND2, EDNRA, ANGPTL4, TGFBR3, GJA1, LAMA2, KIT, TPM1, VCP, GRID2, MEF2C, RPS3A, PLD1, BTG3, CD47, MITF), whose expression after in vitro maturation (IVM) is downregulated with different degrees. Our results may be helpful in further elucidating the molecular basis and functional significance of a number of gene markers associated with the processes of migration, proliferation and angiogenesis occurring in COCs.
机译:卵母细胞的生长和发育影响周围体细胞的功能活性。这些细胞通过间隙通讯受到各种类型的激素,蛋白质,代谢产物和调节分子的调节,最终导致卵母细胞的发育和成熟。体细胞与卵母细胞之间紧密的联系在一起,形成卵丘-卵母细胞复合体(COC),并且它们的双向通讯对于卵母细胞获得发育能力至关重要。在这项研究中,卵母细胞是从杂交种小母猪的卵巢中提取的,并进行了体外成熟。从那些卵母细胞分离的RNA用于后续的微阵列分析。所获得的数据首次显示了属于四个本体论组的可变水平的基因表达水平(倍数变化高于| 2 |且调整的p值<0.05):细胞增殖的调控(GO:0042127)迁移(GO:0030334)和程序性细胞死亡的调控(GO:0043067),可以一起用作增殖,迁移或凋亡标记。我们已经鉴定了猪卵母细胞的几个基因(ID2,VEGFA,BTG2,ESR1,CCND2,EDNRA,ANGPTL4,TGFBR3,GJA1,LAMA2,KIT,TPM1,VCP,GRID2,MEF2C, RPS3A PLD1 BTG3 CD47 MITF ),它们的体外成熟(IVM)表达在不同程度上下调。我们的结果可能有助于进一步阐明与COC中发生的迁移,增殖和血管生成过程相关的许多基因标记的分子基础和功能重要性。

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