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李依, 李雪徽, 叶鼎, 张茹, 刘成杰, 何牡丹, 王厚鹏, 胡炜, 孙永华. 2024: 内源合成的DHA通过促进孕烯醇酮生成来调节斑马鱼卵细胞成熟. 动物学研究, 45(1): 176-188. DOI: 10.24272/j.issn.2095-8137.2023.032
引用本文: 李依, 李雪徽, 叶鼎, 张茹, 刘成杰, 何牡丹, 王厚鹏, 胡炜, 孙永华. 2024: 内源合成的DHA通过促进孕烯醇酮生成来调节斑马鱼卵细胞成熟. 动物学研究, 45(1): 176-188. DOI: 10.24272/j.issn.2095-8137.2023.032
Yi Li, Xuehui Li, Ding Ye, Ru Zhang, Chengjie Liu, Mudan He, Houpeng Wang, Wei Hu, Yonghua Sun. 2024. Endogenous biosynthesis of docosahexaenoic acid (DHA) regulates fish oocyte maturation by promoting pregnenolone production. Zoological Research, 45(1): 176-188. DOI: 10.24272/j.issn.2095-8137.2023.032
Citation: Yi Li, Xuehui Li, Ding Ye, Ru Zhang, Chengjie Liu, Mudan He, Houpeng Wang, Wei Hu, Yonghua Sun. 2024. Endogenous biosynthesis of docosahexaenoic acid (DHA) regulates fish oocyte maturation by promoting pregnenolone production. Zoological Research, 45(1): 176-188. DOI: 10.24272/j.issn.2095-8137.2023.032

内源合成的DHA通过促进孕烯醇酮生成来调节斑马鱼卵细胞成熟

Endogenous biosynthesis of docosahexaenoic acid (DHA) regulates fish oocyte maturation by promoting pregnenolone production

  • 摘要: 众多的证据表明,omega-3多不饱和脂肪酸(n-3 PUFAs),尤其是二十二碳六烯酸(22:6n-3, DHA)对包括人类在内的脊椎动物的生殖健康具有重要作用。然而,这一现象背后的调控机制在很大程度上仍属未知。该研究以DHA合成缺陷的脂肪酸延长酶elovl2突变(elovl2-/-)斑马鱼和内源DHA合成增强的omega-3去饱和酶编码基因(fat1)转基因斑马鱼,分别作为DHA内源合成缺陷和增强模型,系统研究了内源合成的DHA在调控脊椎动物卵母细胞成熟和卵子质量中的作用及其作用机制。研究发现,elovl2-/-突变雌性斑马鱼的繁殖力和卵子质量显著低于野生型(WT)斑马鱼,而fat1转基因雌性斑马鱼的繁殖力和卵子质量均高于WT斑马鱼。elovl2-/-胚胎因缺乏内源DHA导致卵子激活缺陷、微管稳定性较差和孕烯醇酮(pregnenolone, P5)水平降低。进一步研究发现,内源合成的DHA通过促进胆固醇侧链裂解酶编码基因cyp11a1的转录来促进P5的合成,从而在卵子发生过程中稳定微管组装和细胞骨架;DHA反过来则进一步促进了下丘脑-垂体-性腺(hypothalamic–pituitary–gonadal,HPG)轴的活性。总之,通过DHA合成缺陷和合成增强的斑马鱼模型,这项研究揭示了内源性合成的DHA在卵巢中通过对cyp11a1转录调节促进P5的产生,进而促进卵母细胞成熟并提升卵子质量的新机制。

     

    Abstract: Omega-3 polyunsaturated fatty acids (n-3 PUFAs), particularly docosahexaenoic acid (22:6n-3, DHA), play crucial roles in the reproductive health of vertebrates, including humans. Nevertheless, the underlying mechanism related to this phenomenon remains largely unknown. In this study, we employed two zebrafish genetic models, i.e., elovl2-/- mutant as an endogenous DHA-deficient model and fat1 (omega-3 desaturase encoding gene) transgenic zebrafish as an endogenous DHA-rich model, to investigate the effects of DHA on oocyte maturation and quality. Results show that the elovl2-/- mutants had much lower fecundity and poorer oocyte quality than the wild-type controls, while the fat1 zebrafish had higher fecundity and better oocyte quality than wild-type controls. DHA deficiency in elovl2-/- embryos led to defects in egg activation, poor microtubule stability, and reduced pregnenolone levels. Further study revealed that DHA promoted pregnenolone synthesis by enhancing transcription of cyp11a1, which encodes the cholesterol side-chain cleavage enzyme, thereby stabilizing microtubule assembly during oogenesis. In turn, the hypothalamic-pituitary-gonadal axis was enhanced by DHA. In conclusion, using two unique genetic models, our findings demonstrate that endogenously synthesized DHA promotes oocyte maturation and quality by promoting pregnenolone production via transcriptional regulation of cyp11a1.

     

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