首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Substance P is expressed in hippocampal principal neurons during status epilepticus and plays a critical role in the maintenance of status epilepticus
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Substance P is expressed in hippocampal principal neurons during status epilepticus and plays a critical role in the maintenance of status epilepticus

机译:P物质在癫痫持续状态期间在海马主要神经元中表达在维持癫痫持续状态中起关键作用

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摘要

Substance P (SP), a member of the tachykinin family, is widely distributed in the central nervous system and is involved in a variety of physiological processes including cardiovascular function, inflammatory responses, and nociception. We show here that intrahippocampal administration of SP triggers self-sustaining status epilepticus (SSSE) in response to stimulation of the perforant path for periods too brief to have any effect in control rats, and this SSSE generates a pattern of acute hippocampal damage resembling that known to occur in human epilepsy. The SP receptor (SPR) antagonists, spantide II and RP-67,580, block both the initiation of SSSE and SSSE-induced hippocampal damage and terminate established anticonvulsant-resistant SSSE. SSSE results in a rapid and dramatic increase in the expression of preprotachykinin A (a precursor of SP) mRNA and SP in principal neurons in CA3, CA1, and the dentate gyrus as well as in hippocampal mossy fibers. SP also increases glutamate release from hippocampal slices. Enhanced expression of SP during SSSE may modulate hippocampal excitability and contribute to the maintenance of SSSE. Thus, SPR antagonists may constitute a novel category of drugs in antiepileptic therapy.
机译:P(SP)是速激肽家族的一员,广泛分布于中枢神经系统,并参与多种生理过程,包括心血管功能,炎症反应和伤害感受。我们在这里显示,海马内注射SP会触发自我维持性癫痫持续状态(SSSE),以刺激穿孔路径持续太短的时间以至于对对照组大鼠没有任何作用,并且这种SSSE会产生类似于已知的急性海马损伤模式发生在人类癫痫病中。 SP受体(SPR)拮抗剂,Spantide II和RP-67,580,可阻止SSSE和SSSE诱导的海马损伤的发作,并终止已建立的抗惊厥性SSSE。 SSSE导致CA3,CA1和齿状回以及海马生苔纤维中主要神经元中前激肽原A(SP的前体)mRNA和SP的表达急剧增加。 SP还增加了海马片中谷氨酸的释放。 SSSE期间SP表达的增强可能会调节海马兴奋性并有助于维持SSSE。因此,在抗癫痫治疗中,SPR拮抗剂可构成一类新的药物。

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