Scientific Reports (Jun 2017)

Hatching enzymes disrupt aberrant gonadal degeneration by the autophagy/apoptosis cell fate decision

  • Tapas Chakraborty,
  • Sipra Mohapatra,
  • Megumi Tobayama,
  • Kayoko Ohta,
  • Yong-Woon Ryu,
  • Yukinori Kazeto,
  • Kohei Ohta,
  • Linyan Zhou,
  • Yoshitaka Nagahama,
  • Takahiro Matsubara

DOI
https://doi.org/10.1038/s41598-017-03314-7
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 12

Abstract

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Abstract Environmental stressors, gonadal degenerative diseases and tumour development can significantly alter the oocyte physiology, and species fertility and fitness. To expand the molecular understanding about oocyte degradation, we isolated several spliced variants of Japanese anchovy hatching enzymes (AcHEs; ovastacin homologue) 1 and 2, and analysed their potential in oocyte sustenance. Particularly, AcHE1b, an ovary-specific, steroid-regulated, methylation-dependent, stress-responsive isoform, was neofunctionalized to regulate autophagic oocyte degeneration. AcHE1a and 2 triggered apoptotic degeneration in vitellogenic and mature oocytes, respectively. Progesterone, starvation, and high temperature elevated the total degenerating oocyte population and AcHE1b transcription by hyper-demethylation. Overexpression, knockdown and intracellular zinc ion chelation study confirmed the functional significance of AcHE1b in autophagy induction, possibly to mitigate the stress effects in fish, via ion-homeostasis. Our finding chronicles the importance of AcHEs in stress-influenced apoptosis/autophagy cell fate decision and may prove significant in reproductive failure assessments, gonadal health maintenance and ovarian degenerative disease therapy.