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首页> 外文期刊>Journal of neuroinflammation >The enteric bacterial metabolite propionic acid alters brain and plasma phospholipid molecular species: further development of a rodent model of autism spectrum disorders
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The enteric bacterial metabolite propionic acid alters brain and plasma phospholipid molecular species: further development of a rodent model of autism spectrum disorders

机译:肠细菌代谢产物丙酸改变大脑和血浆磷脂分子种类:自闭症谱系障碍的啮齿动物模型的进一步发展

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Gastrointestinal symptoms and altered blood phospholipid profiles have been reported in patients with autism spectrum disorders (ASD). Most of the phospholipid analyses have been conducted on the fatty acid composition of isolated phospholipid classes following hydrolysis. A paucity of information exists on how the intact phospholipid molecular species are altered in ASD. We applied ESI/MS to determine how brain and blood intact phospholipid species were altered during the induction of ASD-like behaviors in rats following intraventricular infusions with the enteric bacterial metabolite propionic acid. Animals were infused daily for 8?days, locomotor activity assessed, and animals killed during the induced behaviors. Propionic acid infusions increased locomotor activity. Lipid analysis revealed treatment altered 21 brain and 30 blood phospholipid molecular species. Notable alterations were observed in the composition of brain SM, diacyl mono and polyunsaturated PC, PI, PS, PE, and plasmalogen PC and PE molecular species. These alterations suggest that the propionic acid rat model is a useful tool to study aberrations in lipid metabolism known to affect membrane fluidity, peroxisomal function, gap junction coupling capacity, signaling, and neuroinflammation, all of which may be associated with the pathogenesis of ASD.
机译:据报道自闭症谱系障碍(ASD)患者的胃肠道症状和血液磷脂谱改变。水解后,大多数磷脂分析都是针对分离的磷脂类别的脂肪酸组成进行的。关于如何在ASD中改变完整磷脂分子种类的信息很少。我们应用ESI / MS确定脑室内输注肠内细菌代谢产物丙酸后,在诱导ASD样行为的过程中大脑和血液完整的磷脂种类是如何变化的。每天给动物输注8天,评估运动能力,并在诱发行为期间处死动物。丙酸输注可增强运动活性。脂质分析显示治疗改变了21种大脑和30种血液磷脂分子种类。观察到大脑SM,二酰基单和多不饱和PC,PI,PS,PE和缩醛磷脂PC和PE分子种类的组成发生了显着变化。这些改变表明,丙酸大鼠模型是研究脂质代谢异常的有用工具,已知这些异常会影响膜流动性,过氧化物酶体功能,间隙连接偶联能力,信号传导和神经炎症,所有这些都可能与ASD的发病机理有关。

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