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[蛋白激酶C与双相情感障碍锂盐治疗的相关性]

[On the relevance of protein kinase C to lithium therapy in bipolar disorder].

作者信息

Sela B

出版信息

Harefuah. 2004 Jun;143(6):414-6, 462.

PMID:15524097
Abstract

The discovery of lithium's efficacy as a mood-stabilizing agent revolutionized the treatment of patients with bipolar disorder and after 5 decades this drug continues to be the mainstay of treatment of this disorder. Valproate, which is dissimilar structurally to lithium, shares most of the effects of lithium at the level of protein kinase C (PKC). Both drugs reduce the activity of PKC, though via different mechanisms. In comparison to patients with major depressive disorder, schizophrenia, or healthy controls, PKC activity is significantly elevated in manic patients, suggesting that changes of PKC activity may be a central pathological trait of the illness. The precise physiological role of PKC activity in the regulation of mood is unclear. The enzyme modulates cellular responses via phosphorylation of numerous substrate proteins. Such substrates of PKC include cytoskeletal proteins, neurotransmitter and hormone receptors, G proteins, GAP-43, MARCKS etc. Further studies are required to clarify any causal role of CPK changes in bipolar-disorder.

摘要

锂作为一种情绪稳定剂的疗效的发现彻底改变了双相情感障碍患者的治疗方式,并且在50年后这种药物仍然是该疾病治疗的主要手段。丙戊酸盐在结构上与锂不同,但在蛋白激酶C(PKC)水平上具有锂的大部分作用。两种药物都降低PKC的活性,不过是通过不同的机制。与重度抑郁症患者、精神分裂症患者或健康对照相比,躁狂患者的PKC活性显著升高,这表明PKC活性的变化可能是该疾病的一个核心病理特征。PKC活性在情绪调节中的精确生理作用尚不清楚。该酶通过对众多底物蛋白进行磷酸化来调节细胞反应。PKC的此类底物包括细胞骨架蛋白、神经递质和激素受体、G蛋白、GAP - 43、MARCKS等。需要进一步研究来阐明PKC变化在双相情感障碍中的任何因果作用。

相似文献

1
[On the relevance of protein kinase C to lithium therapy in bipolar disorder].[蛋白激酶C与双相情感障碍锂盐治疗的相关性]
Harefuah. 2004 Jun;143(6):414-6, 462.
2
Modulation of CNS signal transduction pathways and gene expression by mood-stabilizing agents: therapeutic implications.心境稳定剂对中枢神经系统信号转导通路和基因表达的调节作用:治疗意义。
J Clin Psychiatry. 1999;60 Suppl 2:27-39; discussion 40-1, 113-6.
3
Myristoylated alanine-rich C kinase substrate (MARCKS): a molecular target for the therapeutic action of mood stabilizers in the brain?肉豆蔻酰化富含丙氨酸的蛋白激酶C底物(MARCKS):情绪稳定剂在大脑中治疗作用的分子靶点?
J Clin Psychiatry. 1996;57 Suppl 13:23-31; discussion 32-3.
4
Sodium valproate down-regulates the myristoylated alanine-rich C kinase substrate (MARCKS) in immortalized hippocampal cells: a property of protein kinase C-mediated mood stabilizers.丙戊酸钠下调永生化海马细胞中富含肉豆蔻酰化丙氨酸的蛋白激酶C底物(MARCKS):蛋白激酶C介导的情绪稳定剂的一种特性。
J Pharmacol Exp Ther. 1998 Apr;285(1):307-16.
5
[Possible involvement of protein kinase C in the pathophysiology and treatment of bipolar disorder].蛋白激酶C可能参与双相情感障碍的病理生理学及治疗
Harefuah. 2004 Jun;143(6):420-5, 462.
6
Neurobiology of lithium: an update.锂的神经生物学:最新进展
J Clin Psychiatry. 1998;59 Suppl 6:37-47.
7
Regulation of signal transduction pathways by mood-stabilizing agents: implications for the delayed onset of therapeutic efficacy.心境稳定剂对信号转导通路的调节作用:对治疗疗效延迟起效的影响
J Clin Psychiatry. 1996;57 Suppl 13:34-46; discussion 47-8.
8
Overview of the mechanism of action of lithium in the brain: fifty-year update.锂在大脑中的作用机制概述:五十年回顾
J Clin Psychiatry. 2000;61 Suppl 9:5-15.
9
Bipolar disorder: leads from the molecular and cellular mechanisms of action of mood stabilizers.双相情感障碍:源于心境稳定剂的分子和细胞作用机制。
Br J Psychiatry Suppl. 2001 Jun;41:s107-19.
10
Long-term action of lithium: a role for transcriptional and posttranscriptional factors regulated by protein kinase C.锂的长期作用:蛋白激酶C调控的转录和转录后因子的作用
Synapse. 1994 Jan;16(1):11-28. doi: 10.1002/syn.890160103.