凝结魏茨曼氏菌通过调节脂代谢通路改善高糖饮食诱导对秀丽线虫的损伤

韩龙飞; 吴影; 樊秋霞; 曹力; 牛华伟; 李璇; 赵丽娜; 古绍彬

doi:10.13386/j.issn1002-0306.2024080122

凝结魏茨曼氏菌通过调节脂代谢通路改善高糖饮食诱导对秀丽线虫的损伤

Weizmannia coagulans Ameliorate High-sucrose Diet-Induced Damage in Caenorhabditis elegans by Regulating Lipid Metabolism Pathways

摘要

摘要: 目的：探究凝结魏茨曼氏菌CGMCC 9951对高糖饮食线虫所致机体损伤的改善作用，明确其对脂代谢通路调控作用的靶点。方法：通过在培养基中添加100 mmol/L蔗糖构建线虫的高糖饮食模型，研究凝结魏茨曼氏菌CGMCC 9951对高糖饮食线虫体长、体宽、运动和产卵数的影响，以及体内氧化应激和脂肪积累的变化。结果：CGMCC 9951使高糖线虫的寿命最高延长了27.36%（P<0.05），摆头频率和身体弯曲频率最高分别提高了64.01%和101.91%（P<0.05），产卵数最高增加了77.14%（P<0.05），体宽都有明显缩小（P<0.05），但对高糖线虫的体长无显著影响（P>0.05）；CGMCC 9951使高糖线虫体内过氧化氢酶活性和谷胱甘肽含量最高分别提高了123.34%和55.63%（P<0.05），且丙二醛积累最高降低了74.88%（P<0.05）；CGMCC 9951使高糖线虫体内甘油三酯含量最大减少了56.25%（P<0.05），并且油红O染色显示出其脂肪积累明显降低。实时荧光定量PCR结果表明CGMCC 9951使高糖线虫SREBP信号通路相关基因的表达显著降低（P<0.05），而NHR-49和5-HT信号通路相关基因表达显著增加（P<0.05）。此外，在胰岛素信号通路中daf-2表达下调，daf-16表达上调（P<0.05）。相比于daf-16，daf-2在CGMCC 9951调节高糖线虫脂肪积累过程中发挥着关键作用。最后，CGMCC 9951能够降低DAF-16核转位。结论：凝结魏茨曼氏菌CGMCC 9951能够修复高糖饮食对秀丽隐杆线虫的损伤，并通过调节脂代谢途径减少脂肪在线虫体内的积累。

Abstract: To investigate the ameliorative effects of Weizmannia coagulans (W. coagulans) CGMCC 9951 on the damage induced by a high-sucrose diet in Caenorhabditis elegans (C. elegans) and to elucidate the target pathways involved in the regulation of lipid metabolism. Methods: A high-sucrose diet model of C. elegans was established by supplementing the culture medium with 100 mmol/L sucrose. The effects of W. coagulans CGMCC 9951 on the body length, body width, locomotor activity, and egg production of C. elegans were assessed, along with changes in oxidative stress and lipid accumulation. Results: The lifespan of C. elegans on a high-sucrose diet was extended by up to 27.36% (P<0.05) by CGMCC 9951. Head thrashing frequency was significantly increased by 64.01%, and body bending frequency by 101.91% (P<0.05). Egg production was increased by up to 77.14% (P<0.05). Body width was significantly reduced (P<0.05), but no significant changes were observed in body length (P>0.05). Catalase activity and glutathione levels were enhanced by up to 123.34% and 55.63%, respectively (P<0.05), while malondialdehyde accumulation was reduced by up to 74.88% (P<0.05) by CGMCC 9951. Additionally, triglyceride levels were decreased by up to 56.25% (P<0.05) by CGMCC 9951, and a significant reduction in lipid accumulation was revealed by Oil Red O staining. Real-time quantitative PCR showed that the expression of genes related to the SREBP signaling pathway was significantly downregulated (P<0.05) by CGMCC 9951, while the genes related to the NHR-49 and 5-HT signaling pathways were upregulated (P<0.05). Moreover, in the insulin signaling pathway, daf-2 expression was downregulated, and daf-16 expression was upregulated (P<0.05). Compared to daf-16, a pivotal role in the regulation of lipid accumulation in C. elegans on a high-sucrose diet was played by daf-2 under the treatment of CGMCC 9951. Finally, the nuclear translocation of DAF-16 was reduced by CGMCC 9951. Conclusion: High-sucrose diet-induced damage in C. elegans can be mitigated and lipid accumulation reduced through modulation of lipid metabolism pathways by W. coagulans CGMCC 9951.

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