脑膜淋巴管转运功能障碍加重脂多糖诱导的小鼠中枢炎症
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江苏省自然科学基金青年基金(BK20171088)


Meningeal lymphatic vessel transport dysfunction exacerbates LPS⁃induced central inflam⁃ mation in mice
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    摘要:

    目的:探讨脑膜淋巴管(meningeal lymphatic vessel,mLV)转运功能障碍对脂多糖(lipopolysaccharide,LPS)诱导的小鼠中枢神经系统炎症的影响。方法:①16只C57BL/6雄性小鼠随机分为4组,Control组腹腔注射生理盐水,LPS组分别腹腔注射LPS(2 mg/kg)12、24、72 h,而后观察小鼠mLV转运功能、海马区小胶质细胞(microglial,MG)活化、白介素(interleukin,IL)-6 和IL-1β水平。②将8只小鼠随机分为2组,分别为Control组和VEGFR3抑制剂MAZ51组,观察MAZ51对mLV转运功能的影响。③将24只小鼠分为4组,分别为Control组、MAZ51组、LPS组、LPS+MAZ51组,对MAZ51组和LPS+MAZ51组预先腹腔注射 MAZ51(10 mg/kg),每周5 d,共30 d,6周后对LPS组和LPS+MAZ51组注射LPS,1 d后行为学实验评估小鼠的逃避恐惧能力;免疫组化检测MG 活化情况;ELISA 法检测IL-6、IL-1β的表达量。结果:小鼠腹腔注射LPS 24 h后脑膜LYVE-1面积和颈深淋巴结内OVA-647面积明显减少(P < 0.01),72 h内均低于基础水平(P < 0.01),24 h后海马MG活化、IL-6和IL-1β均明显增加 (P < 0.01)。与Control组相比,MAZ51组OVA-647荧光面积显著减少(P < 0.01)。LPS组小鼠海马区MG活化和IL-6、IL-1β的表达相对Control组均明显增加(P < 0.01)且小鼠僵直时间明显降低(P < 0.01);与LPS组相比,LPS+MAZ51组小鼠海马区MG 活化和炎症因子的表达均增加(P < 0.01)且僵直时间明显减少(P < 0.01)。结论:mLV转运障碍通过增加炎性介质聚积,活化 MG,加重LPS诱导的小鼠中枢炎症和认知功能障碍。

    Abstract:

    Objective:To explore the effects of meningeal lymphatic vessel transport dysfunction on lipopolysaccharide(LPS)-induced central nervous system inflammation in mice. Methods:Firstly,sixteen C57BL/6 mice were randomly divided into four groups, normal saline was injected intraperitoneally in the Control group. The LPS groups were injected intraperitoneally with LPS(2 mg/kg), and then the transport function of meningeal lymphatic vessels,activation of microglia and levels of interleukin-6(IL-6)and interleukin-1β (IL -1β)in the hippocampus were observed after 12 h,24 h and 72 h. Secondly,eight mice were randomly assigned to two groups: Control group and VEGFR3 inhibitor MAZ51 group,to observe the effects of MAZ51 on the transport function of meningeal lymphatic vessels. Finally,twenty-four mice were divided into four groups as follows:control group,MAZ51 group,LPS group,and LPS+MAZ51 group. MAZ51(10 mg/kg)was preinjected intraperitoneally into MAZ51 group and LPS+MAZ51 group for five days per week with a total of 30 days. After six weeks,LPS was injected into LPS group and LPS+MAZ51 group. A day later,behavioral experiments that assess the ability of mice to escape from fear were conducted;the activation of microglia in the hippocampus was measured by immunohistochemistry;the expression of IL-6 and IL-1β was evaluated by ELISA method. Results:The area of LYVE-1 in meninges and the area of OVA-647 in the deep cervical lymph nodes were significantly decreased 24 h after intraperitoneal injection of LPS(P < 0.01),and were lower than the basal level for 72 h(P < 0.01). The activation of microglia and levels of IL-6 and IL-1β in the hippocampus were significantly increased after 24 h(P < 0.01). Compared with the control group,the area of OVA-647 fluorescence in the MAZ51 group was significantly reduced(P < 0.01). The activation of microglia and the expression of inflammatory factors in the hippocampus of mice in the LPS+MAZ51 group were increased(P < 0.01)and the freezing time was significantly reduced(P < 0.01). Conclusion:The impairing transport function of meningeal lymphatic vessels aggravates LPS-induced central inflammation and cognitive dysfunction in mice by increasing inflammatory mediator accumulation and activating microglia.

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谢雯,董洪权,侍崇龙,金文杰.脑膜淋巴管转运功能障碍加重脂多糖诱导的小鼠中枢炎症[J].南京医科大学学报(自然科学版),2023,(7):927-933

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  • 收稿日期:2022-09-26
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  • 在线发布日期: 2023-07-16
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