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促肾上腺皮质激素相关肽、点燃效应与癫痫症

ACTH-related peptides, kindling and seizure disorders.

作者信息

Goldman H, Berman R F, Murphy S

出版信息

Adv Biochem Psychopharmacol. 1987;43:317-27.

PMID:3035892
Abstract

Very small amounts of pituitary hormones and their peptide fragments can profoundly affect learning, memory and other behaviors in both rodents and humans. In addition, several potent pituitary hormone analogs have been developed (e.g. ORG-2766) which retain the behavioral but not the endocrine properties of the parent hormone. The abilities of these peptides to influence nervous system functions suggested that they also may be capable of modifying seizure activity. This possibility is supported by the fact that treatment with adrenocorticotropic hormone (ACTH) represents a major effective therapy for at least one clinical convulsive disorder, infantile spasm. This contention also is reinforced by our findings that ORG-2766 markedly reduces both the behavioral severity and the spread of seizure potentials in an animal model of epilepsy, the kindled rat. By contrast, arginine vasopressin and its non-endocrine desglycyl fragment (DGAVP) facilitates the seizure process in this animal model. Our research also suggests that the behavioral and physiological effects of certain anterior and posterior pituitary hormone fragments depend, in part, on their abilities to modulate permeability mechanisms in brain vasculature. In addition, and especially significant from the standpoint of etiology, is the observation that the kindling process itself appears to alter cerebrovascular permeability. In the kindled rat, "permanent" decreases in permeability (60-75%) are found selectively in the hypothalamic and hippocampal regions, weeks after the last seizure. Several lines of evidence indicate that disruption of normal cerebrovascular function occurs following epileptiform seizures. We propose that an immediate increase in cerebral blood flow and cerebrovascular permeability occurs following a single, acute seizure, and that repeated chronic seizures lead to damage to the cerebrovascular system. Sustained damage would be expected to contribute to the development and maintenance of a chronic seizure focus. Such observations suggest a link between important cerebrovascular disturbances associated with seizures and the existing known and proposed electrophysiological, metabolic and neuropathological substrates of epilepsy. They also point to new strategies for the treatment of seizure disorders by focusing on ways to reduce or prevent cerebrovascular damage.

摘要

极少量的垂体激素及其肽片段能够深刻影响啮齿动物和人类的学习、记忆及其他行为。此外,已经研发出了几种强效的垂体激素类似物(如ORG - 2766),它们保留了母体激素的行为特性,但不具备内分泌特性。这些肽影响神经系统功能的能力表明它们也可能能够改变癫痫活动。促肾上腺皮质激素(ACTH)治疗是至少一种临床惊厥性疾病——婴儿痉挛症的主要有效疗法,这一事实支持了这种可能性。我们的研究结果也强化了这一观点,即在癫痫动物模型——点燃大鼠中,ORG - 2766能显著降低行为严重程度和癫痫电位的扩散。相比之下,精氨酸加压素及其非内分泌去甘氨酰片段(DGAVP)在该动物模型中会促进癫痫发作过程。我们的研究还表明,某些垂体前叶和后叶激素片段的行为和生理效应部分取决于它们调节脑血管通透性机制的能力。此外,从病因学角度来看特别重要的是,观察到点燃过程本身似乎会改变脑血管通透性。在点燃大鼠中,在最后一次癫痫发作数周后,下丘脑和海马区域选择性地出现通透性“永久性”降低(60 - 75%)。几条证据表明,癫痫样发作后会出现正常脑血管功能的破坏。我们提出,单次急性癫痫发作后会立即出现脑血流量和脑血管通透性增加,而反复慢性癫痫发作会导致脑血管系统受损。持续的损伤预计会促进慢性癫痫病灶的形成和维持。这些观察结果表明,与癫痫相关的重要脑血管紊乱与现有的已知和提出的癫痫电生理、代谢及神经病理学基础之间存在联系。它们还指出了通过关注减少或预防脑血管损伤的方法来治疗癫痫疾病的新策略。

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