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Melatonin protects against defects induced by Enniatin B1 during porcine early embryo development

机译:褪黑激素在猪早期胚胎发育期间保护肌苷B1诱导的缺陷

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摘要

Exogenous factors influence embryo development. Enniatin B1 (EB1), one emerging mycotoxin of Fusarium fungi, can cause damage to cells and mouse blastocysts. However, the toxicity of EB1 on porcine embryo development and whether melatonin can eliminate the detrimental effects of EB1 on embryos remain unclear. Here, this work demonstrated that EB1 significantly decreased the cleavage and blastocyst rates and blastocyst cell number of embryos in a dose and time dependent manner. Further study displayed that EB1 obviously destroyed nuclear remodeling dynamics. Importantly, EB1 triggered embryo apoptosis through downregulating the expression of Sod1,Gpx4, Cat and Bcl2l1 while upregulating the transcription of Bax and Caspase3. Moreover, EB1 significantly disrupted the transcription of Dnmt1, Dnmt3a, Tet1 and Tet3, further leading to incomplete DNA demethylation of CenRep, Oct4, Nanog and Sox2, thus, the expression of Eif1a, Oct4, Nanog and Sox2 remarkably decreased. Whereas EB1-exposed embryos were treated with melatonin, these disorders were obviously ameliorated, and the development ability of embryos was also rescued. In conclusion, EB1 exerted detrimental effects on porcine early embryos, while melatonin effectively rescued EB1-mediated defects in embryos. This work provides a novel insight into the improvement of embryo quality and the promotion of human and animal reproduction.
机译:外源性因素影响胚胎发育。 EnniatiN B1(EB1),一种新出现的镰刀菌真菌的霉菌毒素,可能对细胞和小鼠胚泡造成损伤。然而,EB1对猪胚胎发育的毒性以及褪黑素是否可以消除EB1对胚胎的不清楚尚不清楚。这里,这项工作表明EB1以剂量和时间依赖性方式显着降低了胚胎的裂缝和胚泡细胞数。进一步的研究表明,EB1明显地破坏了核重塑动力学。重要的是,通过下调SOD1的表达,EB1触发胚胎细胞凋亡,GPX4,CAT和BCL2L1,同时上调Bax和Caspase3的转录。此外,EB1显着破坏了DNMT1,DNMT3A,TET1和TET3的转录,进一步导致CENREP,OCT4,纳米和SOX2的不完全DNA去甲基化,因此,EIF1A,OCT4,NANOG和SOX2的表达显着降低。虽然EB1暴露的胚胎被褪黑素处理,但这些疾病显然是改善的,并且还救出了胚胎的发育能力。总之,EB1对猪早期胚胎产生了不利影响,而褪黑素有效地拯救了胚胎中的EB1介导的缺陷。这项工作为改善胚胎质量和促进人类和动物繁殖提供了新的洞察力。

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