Sirt3-dependent deacetylation of SOD2 plays a protective role against oxidative stress in oocytes from diabetic mice.
Xiaohui LiuLiang ZhangPan WangXiaoyan LiDanhong QiuLing LiJiaqi ZhangXiaojing HouLongsen HanJuan GeMo LiLing GuQiang WangPublished in: Cell cycle (Georgetown, Tex.) (2017)
Maternal diabetes has been demonstrated to adversely affect oocyte quality in mouse oocytes. However, the potential molecular mechanisms are poorly understood. Here, we established a type I diabetic mouse model and detected the increased reactive oxygen species (ROS) levels and decreased Sirt3 expression in oocytes from diabetic mice. Furthermore, we found that forced expression of Sirt3 in diabetic oocytes significantly attenuates such an excessive production of ROS. The acetylation status of lysine 68 of superoxide dismutase (SOD2K68) is dependent on Sirt3 in oocytes. In line with this, SOD2K68 acetylation levels were markedly increased in diabetic oocytes, and Sirt3 overexpression could effectively suppress this tendency. Importantly, the deacetylation-mimetic mutant SOD2K68R is capable of partly preventing the oxidative stress in oocytes from diabetic mice. In conclusion, our findings support a model where Sirt3 plays a protective role against oxidative stress in oocytes exposed to maternal diabetes through deacetylating SOD2K68.
Keyphrases
- oxidative stress
- ischemia reperfusion injury
- type diabetes
- dna damage
- reactive oxygen species
- amyotrophic lateral sclerosis
- poor prognosis
- mouse model
- diabetic rats
- induced apoptosis
- cardiovascular disease
- cell death
- cell proliferation
- physical activity
- signaling pathway
- long non coding rna
- body mass index
- hydrogen peroxide
- transcription factor
- pregnancy outcomes
- endoplasmic reticulum stress
- binding protein
- gestational age
- heat shock
- heat stress