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D-氨基酸在精神分裂症中的影响。

Impact of D-Amino Acids in Schizophrenia.

作者信息

Dursun Serdar M, Dursun Leman H, Baker Glen B

机构信息

Department of Psychiatry (Neurochemical Research Unit and Bebensee Schizophrenia Research Unit) and Neuroscience and Mental Health Institute, University of Alberta, Edmonton, AB T6G 2B7, Canada.

出版信息

Biomolecules. 2025 Sep 2;15(9):1270. doi: 10.3390/biom15091270.

Abstract

Most amino acids contain a chiral center and thus, can exist as L- and D-isomers. For many years, it was thought that only the L-isomers were present in mammals. However, in recent decades it has been demonstrated that D-isomers are also present. Three of these amino acids, namely D-serine, D-aspartate, and D-alanine, have been proposed to play a role in the etiology of schizophrenia via interactions with glutamate receptors. D-Serine and D-alanine act at the glycine modulatory site on the NMDA receptor, while D-aspartate acts at the glutamate site on the same receptor. D-aspartate also acts on the mGlu5 receptor and can stimulate glutamate release presynaptically. Preclinical studies have reported that manipulations to reduce brain levels of D-serine, D-aspartate, or D-alanine lead to schizophrenia-relevant behaviors, and clinical studies have reported reduced levels of these D-amino acids in the brain tissue (postmortem) and/or body fluids from schizophrenia patients compared to those noted in controls, although there are some contradictory findings. The possible use of these amino acids and/or the manipulation of their relevant enzymes in the treatment of schizophrenia are described. D-Cysteine has been identified recently in human brain tissue, with the highest values in white matter; demonstration of its involvement in brain development has led to speculation that it could be involved in the etiology of schizophrenia, identifying it as a potential therapy in combination with antipsychotics. Future directions and potential problems that should be considered in studies on D-amino acids and their relevant enzymes in schizophrenia are discussed.

摘要

大多数氨基酸都含有一个手性中心,因此可以以L-异构体和D-异构体的形式存在。多年来,人们一直认为哺乳动物体内只存在L-异构体。然而,近几十年来已证实D-异构体也存在。其中三种氨基酸,即D-丝氨酸、D-天冬氨酸和D-丙氨酸,被认为通过与谷氨酸受体相互作用在精神分裂症的病因学中发挥作用。D-丝氨酸和D-丙氨酸作用于NMDA受体上的甘氨酸调节位点,而D-天冬氨酸作用于同一受体上的谷氨酸位点。D-天冬氨酸还作用于mGlu5受体,并能在突触前刺激谷氨酸释放。临床前研究报告称,降低大脑中D-丝氨酸、D-天冬氨酸或D-丙氨酸水平的操作会导致与精神分裂症相关的行为,临床研究报告称,与对照组相比,精神分裂症患者脑组织(死后)和/或体液中这些D-氨基酸的水平降低,尽管也有一些相互矛盾的发现。本文描述了这些氨基酸和/或其相关酶在精神分裂症治疗中的可能用途。最近在人类脑组织中发现了D-半胱氨酸,在白质中含量最高;其参与大脑发育的证据引发了人们的猜测,即它可能与精神分裂症的病因有关,这表明它可作为与抗精神病药物联合使用的潜在疗法。本文还讨论了在精神分裂症研究中关于D-氨基酸及其相关酶应考虑的未来方向和潜在问题。

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