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内源性士的宁、尼古丁和吗啡——与神经精神疾病相关的低士的宁能、高士的宁能、烟碱能和吗啡能状态的描述。

Endogenous strychnine, nicotine, and morphine--description of hypo and hyper-strychninergic, nicotinergic and morphinergic state in relation to neuropsychiatric diseases.

作者信息

Ravikumar A, Arun P, Devi K V, Kurup P A

机构信息

Department of Neurology, Medical College Hospital, Trivandrum 695011, India.

出版信息

Indian J Exp Biol. 2000 Jun;38(6):559-66.

Abstract

Previous work from this laboratory had demonstrated the presence of endogenous morphine, strychnine and nicotine in the mammalian brain and human serum samples. Morphine is synthesised from tyrosine and strychnine and nicotine from tryptophan. This study examines the role of strychnine, nicotine and morphine in neuropsychiatric disorders. The blood levels of tyrosine, tryptophan, strychnine, nicotine and morphine were studied as also RBC membrane Na(+)-K+ ATPase activity. It was found that serum tyrosine levels were reduced and tryptophan levels elevated in all neuropsychiatric disorders studied with a reduction in RBC Na(+)-K+ ATPase activity. Nicotine was present in significant amounts in serum of patients with schizophrenia, CNS glioma and syndrome X with multiple lacunar state. Morphine was present in significant amounts only in the serum of patients with multiple sclerosis and MDP. Strychnine was present in significant amounts in the serum of patients with epilepsy, Parkinson's disease and MDP. The presence of nicotine and strychnine in significant amounts could be related to elevated tryptophan levels suggesting the synthesis of these alkaloids from tryptophan. Morphine was not detected in most of the disorders owing to low tyrosine levels noted in them. Na(+)-K+ ATPase inhibition noticed in most of the disorders could be related to decreased hyperpolarising morphinergic transmission and increased depolarising nicotinergic and strychinergic transmission. The role of morphine, strychnine and nicotine in the pathogenesis of these disorders in the setting of membrane Na(+)-K+ ATPase inhibition is discussed.

摘要

该实验室之前的研究已经证明,哺乳动物大脑和人类血清样本中存在内源性吗啡、士的宁和尼古丁。吗啡由酪氨酸合成,士的宁和尼古丁由色氨酸合成。本研究探讨了士的宁、尼古丁和吗啡在神经精神疾病中的作用。研究了酪氨酸、色氨酸、士的宁、尼古丁和吗啡的血药浓度以及红细胞膜钠钾ATP酶活性。结果发现,在所研究的所有神经精神疾病中,血清酪氨酸水平降低,色氨酸水平升高,同时红细胞钠钾ATP酶活性降低。在精神分裂症、中枢神经系统胶质瘤和伴有多发性腔隙状态的X综合征患者的血清中,尼古丁含量显著。吗啡仅在多发性硬化症和MDP患者的血清中含量显著。士的宁在癫痫、帕金森病和MDP患者的血清中含量显著。尼古丁和士的宁的大量存在可能与色氨酸水平升高有关,提示这些生物碱由色氨酸合成。由于大多数疾病中酪氨酸水平较低,因此未检测到吗啡。在大多数疾病中观察到的钠钾ATP酶抑制可能与超极化吗啡能传递减少以及去极化烟碱能和士的宁能传递增加有关。本文讨论了在膜钠钾ATP酶抑制情况下,吗啡、士的宁和尼古丁在这些疾病发病机制中的作用。

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