三七总皂苷下调CD36信号通路对高脂饲料喂养小鼠血小板高反应性的抑制作用
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1大理大学公共卫生学院实验教学中心,2营养与食品卫生学教研室,云南 大理 671000

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国家自然科学基金(82260638);云南省基础研究专项面上项目(202401AT070081)


Total saponins of Panax notoginseng attenuate platelet hyperreactivity through down ⁃ regulating CD36 signalling pathway in mice fed a high⁃fat diet
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1Department of Laboratory Teaching Center,2Department of Nutrition,School of Public Health,Dali University,Dali 671000 ,China

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    摘要:

    目的:探讨膳食补充三七总皂苷(total saponins of Panax notoginseng,PNS)对高脂血症模型小鼠血小板高反应性的影响及其可能的分子机制。方法:将8周龄健康雄性C57BL/6J小鼠随机分为4组,即低脂饲料(low-fat diet,LFD)喂饲组(LFD 组)、LFD+PNS 组(LFD中添加PNS 200 mg/kg饲料)、高脂饲料(high-fat diet,HFD)喂饲组(HFD组)、HFD+PNS 组(HFD中添加 PNS 200 mg/kg饲料),实验干预12 周后处死小鼠,分离血浆和提取纯化血小板,使用试剂盒检测血脂水平,血小板聚集仪测定血小板最大聚集率,流式细胞术和酶联免疫吸附法检测血小板活化指标,实时定量PCR技术检测血小板CD36 mRNA表达水平,Western blot免疫印迹实验检测血小板CD36蛋白表达、Src和p47phox的磷酸化水平。结果:与LFD组相比,HFD组小鼠血浆总胆固醇、甘油三酯和低密度脂蛋白胆固醇显著升高,膳食补充PNS可显著降低小鼠的血脂水平。在激动剂凝血酶的刺激下, 膳食补充PNS显著降低由HFD诱导的小鼠血小板聚集和活化,如抑制血小板表面CD62P的表达和血小板因子4(platelet factor 4, PF4)及趋化因子配体5(chemokine ligand 5,CCL5)的释放,提示PNS可降低HFD诱导的小鼠血小板高反应性。机制上,膳食补充PNS显著降低由HFD诱导的小鼠血小板CD36 mRNA 和蛋白表达,并且显著抑制由HFD诱导血小板CD36下游信号通路的活化,包括下调Src和p47phox的磷酸化水平。此外,膳食补充 PNS 可显著抑制由HFD组小鼠血浆诱导的血小板表面CD62P的表达,在CD36 分子的中和性抗体FA6-152的作用下,PNS的抑制作用被消除。结论:膳食补充PNS对高脂饲料喂养小鼠的血小板高反应性具有抑制作用,其作用机制可能是下调CD36信号通路,本研究为PNS改善高脂血症及其相关慢性代谢性疾病中血栓形成提供参考价值。

    Abstract:

    Objective:The current study aims to assess the efficacy of total saponins of Panax notoginseng(PNS)supplementation on platelet hyperreactivity in hyperlipidemic mice as well as to clarify the underlying mechanisms in vivo. Methods:Healthy male C57BL/6J mice(aged 8 weeks)were randomly divided into four groups and fed either a low-fat diet(LFD group),a LFD supplemented with PNS(200 mg/kg diet,LFD+PNS group),a high-fat diet(HFD group),or a HFD supplemented with PNS(200 mg/kg diet,HFD+ PNS group)for 12 weeks. After that all mice were killed,and the plasma and purified platelets were prepared,followed by measurement levels of plasma lipid profile using commercial assay kits. A platelet aggregometer was used to measure maximal aggregation ratio. Platelet activation was determined by flow cytometry and enzyme - linked immunosorbent assays. Real - time PCR technique was used to detect CD36 mRNA expression,and Western blot was used to measure protein expression levels of CD36 and phosphorylation of Src and p47phox. Results:When compared with those in LFD group,the plasma levels of total cholesterol,triglyceride and low density lipoprotein cholesterol were significantly increased in HFD group,which were greatly decreased by PNS supplementation. Moreover,PNS supplementation favorably attenuated HFD-induced platelet aggregation and activation in response to an agonist thrombin,including inhibiting platelet surface CD62P expression,and platelet factor 4(PF4)and chemokine ligand 5 (CCL5)release,indicating a potent inhibitory effect of PNS on HFD-induced platelet hyperreactivity. Mechanistically,CD36 mRNA and protein expression increased by HFD were significantly down-regulated by PNS supplementation. Moreover,PNS supplementation also greatly attenuated HFD-induced activation of downstream signalling pathways mediated by CD36,including down-regulating Src and p47phox phosphorylation. Furthermore,it is found that platelet surface CD62P expression isolated from LFD mice in response to adenosine diphosphate were increased by adding hyperlipidemic plasma from HFD mice,which was greatly decreased in LFD+PNS group. This significant difference was abolished when pretreated with an anti-CD36 monoclonal antibody FA6-152. Conclusions:PNS supplementation attenuates platelet hyperreactivity in mice fed a high - fat diet possibly through down - regulating CD36 signalling pathway. The current study may provide potential value for PNS to improve thrombosis in hyperlipemia and the related chronic metabolic diseases.

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张春梅,胡锦秋,毕晓艳,马军羽,李梦瑶,李荣,牙甫礼.三七总皂苷下调CD36信号通路对高脂饲料喂养小鼠血小板高反应性的抑制作用[J].南京医科大学学报(自然科学版),2025,(8):1092-1100

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  • 收稿日期:2024-12-02
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  • 在线发布日期: 2025-08-13
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