Melatonin protects against maternal obesity‐associated oxidative stress and meiotic defects in oocytes via the <scp>SIRT</scp>3‐<scp>SOD</scp>2‐dependent pathway

Han, Longsen; Wang, Haichao; Li, Ling; Li, Xiaoyan; Ge, Juan; Reíter, Russel J.; Wang, Qiang

doi:10.1111/jpi.12431

Cited by 145 publications

(139 citation statements)

References 63 publications

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“…For example, previous studies reported in the rat that intraperitoneal injection of 15 mg/kg MT reduced gastrointestinal motility disorder caused by noise stress, while intraperitoneal injection of 40 mg/kg MT attenuated effectively methotrexate‐induced oxidative stress and small intestinal damage . Oral administration of 30 mg/kg MT to mice fed a high‐fat diet for three consecutive weeks can resist obesity . In addition, rats were given to intraperitoneal injection of MT at a dose of 15 mg/kg/day (body weight) between 7:00 and 8:00 to explore the role of MT in ameliorating cognitive impairment induced by SD .…”

Section: Discussionmentioning

confidence: 80%

Role of melatonin in sleep deprivation‐induced intestinal barrier dysfunction in mice

Gao

Wang

Dong

et al. 2019

Journal of Pineal Research

169

160

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Intestinal diseases caused by sleep deprivation (SD) are severe public health threats worldwide. This study focuses on the effect of melatonin on intestinal mucosal injury and microbiota dysbiosis in sleep‐deprived mice. Mice subjected to SD had significantly elevated norepinephrine levels and decreased melatonin content in plasma. Consistent with the decrease in melatonin levels, we observed a decrease of antioxidant ability, down‐regulation of anti‐inflammatory cytokines and up‐regulation of pro‐inflammatory cytokines in sleep‐deprived mice, which resulted in colonic mucosal injury, including a reduced number of goblet cells, proliferating cell nuclear antigen‐positive cells, expression of MUC2 and tight junction proteins and elevated expression of ATG5, Beclin1, p‐P65 and p‐IκB. High‐throughput pyrosequencing of 16S rRNA demonstrated that the diversity and richness of the colonic microbiota were decreased in sleep‐deprived mice, especially in probiotics, including Akkermansia, Bacteroides and Faecalibacterium. However, the pathogen Aeromonas was markedly increased. By contrast, supplementation with 20 and 40 mg/kg melatonin reversed these SD‐induced changes and improved the mucosal injury and dysbiosis of the microbiota in the colon. Our results suggest that the effect of SD on intestinal barrier dysfunction might be an outcome of melatonin suppression rather than a loss of sleep per se. SD‐induced intestinal barrier dysfunction involved the suppression of melatonin production and activation of the NF‐κB pathway by oxidative stress.

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Section: Discussionmentioning

confidence: 80%

Role of melatonin in sleep deprivation‐induced intestinal barrier dysfunction in mice

Gao

Wang

Dong

et al. 2019

Journal of Pineal Research

169

160

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show abstract

“…Because of the worldwide increase in obesity, female fertility has shown a marked decline. Since mitochondrial SIRT3 is suppressed in obese rodents, which leads to reduced SOD2 and unrestrained ROS formation, Han et al [210] fed melatonin to obese rats. As anticipated, melatonin greatly improved oocyte quality and fertilizability; this was accompanied by an activation (deacetylation) of SIRT3, which induced SOD2 ultimately reducing oxidative stress in the oocytes.…”

Section: The Melatonin/sirt3 Interactionsmentioning

confidence: 99%

“…This suggests that the antioxidant action of melatonin in oocytes depends on stimulation (deacetylation) of SIRT3 which enhances the activity of the antioxidant enzyme, superoxide dismutase. Figure drawn from the data of Han et al [210]. * p > 0.001.…”

Section: Figurementioning

confidence: 99%

Melatonin Mitigates Mitochondrial Meltdown: Interactions with SIRT3

Reíter

Tan

Rosales-Corral

et al. 2018

IJMS

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Melatonin exhibits extraordinary diversity in terms of its functions and distribution. When discovered, it was thought to be uniquely of pineal gland origin. Subsequently, melatonin synthesis was identified in a variety of organs and recently it was shown to be produced in the mitochondria. Since mitochondria exist in every cell, with a few exceptions, it means that every vertebrate, invertebrate, and plant cell produces melatonin. The mitochondrial synthesis of melatonin is not photoperiod-dependent, but it may be inducible under conditions of stress. Mitochondria-produced melatonin is not released into the systemic circulation, but rather is used primarily in its cell of origin. Melatonin’s functions in the mitochondria are highly diverse, not unlike those of sirtuin 3 (SIRT3). SIRT3 is an NAD+-dependent deacetylase which regulates, among many functions, the redox state of the mitochondria. Recent data proves that melatonin and SIRT3 post-translationally collaborate in regulating free radical generation and removal from mitochondria. Since melatonin and SIRT3 have cohabitated in the mitochondria for many eons, we predict that these molecules interact in many other ways to control mitochondrial physiology. It is predicted that these mutual functions will be intensely investigated in the next decade and importantly, we assume that the findings will have significant applications for preventing/delaying some age-related diseases and aging itself.

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“…20 In brief, female ICR mice were primed with pregnant mare serum gonadotropin. 20 In brief, female ICR mice were primed with pregnant mare serum gonadotropin.…”

Section: In Vitro Fertilization and Embryo Culturementioning

confidence: 99%

SETD2 reduction adversely affects the development of mouse early embryos

Huang

2019

J of Cellular Biochemistry

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SET domain‐containing protein 2 (SETD2), the protein of regulating trimethylation status of histone H3 at lysine 36 (H3K36), participates in the maintenance of chromatin architecture, transcription elongation, genome stability, and other biological events. However, its function in preimplantation embryos is still obscure. In this study, specific small interfering RNA was employed to investigate the functions of SETD2. We find that deletion of SETD2 results in the developmental delay of mouse early embryos, indicative of the compromised developmental potential. Remarkably, SETD2 knockdown induces the accumulation of the DNA lesions and apoptotic blastomeres in early embryos. In addition, the methylation level of H3K36 is significantly reduced in two‐cell embryos depleted of SETD2. In summary, our data indicate that SETD2 maintains genome stability perhaps via regulating trimethylation status of H3K36, consequently controlling the embryo quality. These findings pave the avenue for understanding the cross‐talk between epigenome and SETD2 during early embryo development.

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Melatonin protects against maternal obesity‐associated oxidative stress and meiotic defects in oocytes via the SIRT3‐SOD2‐dependent pathway

Cited by 145 publications

References 63 publications

Role of melatonin in sleep deprivation‐induced intestinal barrier dysfunction in mice

Role of melatonin in sleep deprivation‐induced intestinal barrier dysfunction in mice

Melatonin Mitigates Mitochondrial Meltdown: Interactions with SIRT3

SETD2 reduction adversely affects the development of mouse early embryos

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