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1. PKD regulates mitophagy to prevent oxidative stress and mitochondrial dysfunction during mouse oocyte maturation.

2. Loss of AMPK activity induces organelle dysfunction and oxidative stress during oocyte aging.

3. Exposure to nivalenol declines mouse oocyte quality via inducing oxidative stress-related apoptosis and DNA damage†.

4. Melatonin ameliorates ochratoxin A-induced oxidative stress and apoptosis in porcine oocytes.

5. Melatonin reduces oxidative damage in mouse granulosa cells via restraining JNK-dependent autophagy.

6. Melatonin protects oocytes from MEHP exposure-induced meiosis defects in porcine.

7. Protective mechanism of FSH against oxidative damage in mouse ovarian granulosa cells by repressing autophagy.

8. FSH protects mouse granulosa cells from oxidative damage by repressing mitophagy.

9. Melamine Induces Oxidative Stress in Mouse Ovary.

10. Aflatoxin B1 is toxic to porcine oocyte maturation.

11. 3-Nitropropionic acid induces ovarian oxidative stress and impairs follicle in mouse.

12. Mycotoxin-containing diet causes oxidative stress in the mouse.

13. Mitochondrial dysfunction influences apoptosis and autophagy in porcine parthenotes developing in vitro.

15. Modified hydrated sodium calcium aluminosilicate‐supplemented diet protects porcine oocyte quality from zearalenone toxicity.

16. Protective Effects of Melatonin Against Zearalenone Toxicity on Porcine Embryos in vitro.

17. Fumonisin B1 exposure deteriorates oocyte quality by inducing organelle dysfunction and DNA damage in mice.

18. Exposure to PBDE47 affects mouse oocyte quality via mitochondria dysfunction-induced oxidative stress and apoptosis.

19. HT-2 toxin exposure induces mitochondria dysfunction and DNA damage during mouse early embryo development.

20. Nivalenol disrupts mitochondria functions during porcine oocyte meiotic maturation.

21. Exposure to acrylamide induces zygotic genome activation defects of mouse embryos.

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