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Lysosomal dysfunction disturbs porcine oocyte maturation and developmental capacity by disorganizing chromosome/cytoskeleton and activating autophagy/apoptosis

机译:溶酶体功能障碍通过染色体/细胞骨架和激活自噬/凋亡来扰乱猪卵母细胞成熟和发育能力

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摘要

Lysosome, an important organelle in eukaryotes, can sequester macromolecules submitted by the endocytosis and autophagy pathways for degradation and recycling. Massive macromolecular turnover is also vital to the growth and development of mammalian oocytes. However, the functional role of lysosomes in the meiotic maturation of mammalian oocytes remains largely unexplored. Here, by treating in vitro matured porcine cumulus-oocyte complexes (COCs) with chloroquine (CQ), a lysosome inhibitor, we showed that regardless of CQ concentration, lysosomal inhibition affected neither the extrusion of the first polar body (PB1), nor the ROS levels. However, CQ treatment dramatically decreased the rates of oocytes with normal chromosome alignment and cytoskeleton organization (P < 0.05), but boosted the rates of oocytes with apoptosis (P < 0.05). Subsequently, after pathenogenetic activation or in vitro fertilization, the death or fragmentation rates of oocytes treated by CQ (both 35 mu M and 45 mu M) were significantly higher (P < 0.05), whereas the rates of embryo cleavage, embryos developed to blastocysts, and average blastomere number per blastocyst, were all significantly lower (P < 0.05), respectively. Furthermore, CQ (35 mu M) treatment activated the autophagy pathway by elevating the LC3 II/I ratio. Taken together, lysosomes could affect porcine oocyte maturation and subsequent developmental capacity partially through the chromosome organization/cytoskeleton assembly and autophagy/apoptosis pathways. (C) 2019 Elsevier Inc. All rights reserved.
机译:溶酶体是真核生物中一种重要的细胞器,可以隔离由内吞和自噬途径提供的大分子,以便降解和再循环。大分子的大量更新对哺乳动物卵母细胞的生长和发育也至关重要。然而,溶酶体在哺乳动物卵母细胞减数分裂成熟过程中的功能作用仍有待进一步研究。在这里,通过用氯喹(一种溶酶体抑制剂)处理体外成熟的猪卵丘卵母细胞复合物(COC),我们发现,无论CQ浓度如何,溶酶体抑制都不会影响第一极体(PB1)的挤出,也不会影响ROS水平。然而,CQ处理显著降低了染色体排列和细胞骨架组织正常的卵母细胞的比率(P<0.05),但提高了凋亡卵母细胞的比率(P<0.05)。随后,在路径基因激活或体外受精后,CQ(35μM和45μM)处理的卵母细胞的死亡率或碎裂率显著较高(P<0.05),而胚胎卵裂率、胚胎发育成囊胚率和每个囊胚的平均卵裂球数均显著较低(P<0.05)。此外,CQ(35μM)治疗通过提高LC3 II/I比率激活自噬途径。综上所述,溶酶体可部分通过染色体组织/细胞骨架组装和自噬/凋亡途径影响猪卵母细胞成熟和随后的发育能力。(C) 2019爱思唯尔公司版权所有。

著录项

  • 来源
    《Theriogenology》 |2019年第1期|共8页
  • 作者单位

    Northeast Agr Univ Key Lab Anim Cellular &

    Genet Engn Heilongjiang P Harbin 150030 Heilongjiang Peoples R China;

    Northeast Agr Univ Key Lab Anim Cellular &

    Genet Engn Heilongjiang P Harbin 150030 Heilongjiang Peoples R China;

    Northeast Agr Univ Key Lab Anim Cellular &

    Genet Engn Heilongjiang P Harbin 150030 Heilongjiang Peoples R China;

    Northeast Agr Univ Key Lab Anim Cellular &

    Genet Engn Heilongjiang P Harbin 150030 Heilongjiang Peoples R China;

    Northeast Agr Univ Key Lab Anim Cellular &

    Genet Engn Heilongjiang P Harbin 150030 Heilongjiang Peoples R China;

    Northeast Agr Univ Key Lab Anim Cellular &

    Genet Engn Heilongjiang P Harbin 150030 Heilongjiang Peoples R China;

    Northeast Agr Univ Key Lab Anim Cellular &

    Genet Engn Heilongjiang P Harbin 150030 Heilongjiang Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 动物学;
  • 关键词

    Porcine; Oocyte; Blastocyst; Lysosome; Autophagy;

    机译:猪;卵母细胞;胚泡;溶酶体;自噬;
  • 入库时间 2022-08-20 19:20:10

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