Cellular Physiology and Biochemistry (Dec 2016)

RASD1 Knockdown Results in Failure of Oocyte Maturation

  • Youngeun Lee,
  • Kyeoung-Hwa Kim,
  • Hyemin Yoon,
  • Ok-Hee Lee,
  • Eunyoung Kim,
  • Miseon Park,
  • Hoon Jang,
  • Kwonho Hong,
  • Hyuk Song,
  • Jung Jae Ko,
  • Woo Sik Lee,
  • Kyung-Ah Lee,
  • Eun Mi Chang,
  • Youngsok Choi

DOI
https://doi.org/10.1159/000453182
Journal volume & issue
Vol. 40, no. 6
pp. 1289 – 1302

Abstract

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Background: Ras dexamethasone-induced protein (RASD1) is a member of Ras superfamily of small GTPases. RASD1 regulates various signaling pathways involved in iron homeostasis, growth hormone secretion, and circadian rhythm. However, RASD1 function in oocyte remains unknown. Methods: Using immunohistochemistry, immunofluorescence, and quantitative real-time RT-PCR, RASD1 expression in mouse ovary and RASD1 role in oocyte maturation-related gene expression, spindle formation, and chromosome alignment were analyzed. RNAi microinjection and time-lapse video microscopy were used to examine the effect of Rasd1 knockdown on oocyte maturation. Results: RASD1 was highly detected in oocytes transitioning from primordial to secondary follicles. Rasd1 was highly expressed in germinal vesicle (GV), during GV breakdown, and in metaphase I (MI) stage as oocytes mature, and its expression was significantly downregulated in MII stage. With knockdown of Rasd1, maturation in GV oocytes was arrested at MI stage, showing disrupted meiotic spindling and chromosomal misalignment. In addition, Obox4 and Arp2/3, engaged in MI-MII transition and cytokinesis, respectively, were misregulated in GV oocytes by Rasd1 knockdown. Conclusion: These findings suggest that RASD1 is a novel factor in MI-MII oocyte transition and may be involved in regulating the progression of cytokinesis and spindle formation, controlling related signaling pathways during oocyte maturation.

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