胆囊收缩素-8通过一种涉及CCK(A)和CCK(B)受体的机制调节成年小鼠大脑中的神经生长因子浓度。

Cholecystokinin-8 regulation of NGF concentrations in adult mouse brain through a mechanism involving CCK(A) and CCK(B) receptors.

作者信息

Tirassa P, Stenfors C, Lundeberg T, Aloe L

机构信息

Institute of Neurobiology (CNR), Rome, Italy.

出版信息

Br J Pharmacol. 1998 Mar;123(6):1230-6. doi: 10.1038/sj.bjp.0701718.

DOI:10.1038/sj.bjp.0701718

PMID:9559909

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565271/

Abstract

Nerve growth factor (NGF), a powerful agent for the growth, differentiation and regeneration of lesioned cells of the central and peripheral nervous systems, has in recent years been indicated as a potential therapeutic agent capable of reversing the processes of cell damage in neurodegenerative events in man. Since NGF does not cross the blood-brain barrier and central NGF administration requires invasive surgical procedures, the discovery of substances modulating in vivo NGF synthesis in the brain will be extremely useful for a possible clinical use of NGF. 2. The aim of the present study to analyse if the content of NGF in the brain of adult mice can be affected by peripheral administration of cholecystokinin-8 (CCK-8), a well known neuropeptide which has stimulant actions on neurons in the brain and promotes a variety of neurobehavioural effects both in man and rodents. 3. The dose-response and time course effects of an i.p. injection of CCK-8 on the NGF concentrations in the hippocampus, cortex, hypothalamus and pituitary of adult male mice were analysed by use of a sensitive immunoenzymatic assay for NGF. The effects of pretreatment with selective CCK(A) and CCK(B) receptor antagonists and atropine on the NGF response to CCK injection were also studied. 4. The effects of CCK-8 were dose- and time-dependent and the injection of 8 nmol kg(-1) resulted in a 3 fold increase of NGF levels in the hypothalamus and pituitary, and about a 60% increase in the hippocampus. No effects were observed in the cortex. Pretreatment with a selective CCK(A) receptor antagonist blocked the CCK-induced NGF increase in the hypothalamus and pituitary. In the hippocampus the same effect was obtained with a CCK(B) receptor antagonist. Pretreatment with atropine suppressed the CCK-induced effects on NGF levels in all the brain regions examined. 5. Our results showing that i.p. injection with CCK-8 can modulate NGF levels in the brain through a mechanism which seems, in part, to be mediated via the vagal afferents, indicate that this neuropeptide may represent a useful pharmacological approach to enhance endogenous NGF levels in neuropathologies associated with a neurotrophin deficit.

摘要

神经生长因子（NGF）是一种对中枢和外周神经系统受损细胞的生长、分化及再生具有强大作用的因子，近年来已被视为一种潜在的治疗剂，能够逆转人类神经退行性病变中的细胞损伤过程。由于NGF不能穿过血脑屏障，且向中枢给予NGF需要侵入性手术操作，因此发现能够调节脑内NGF体内合成的物质对于NGF的临床应用可能极为有用。2. 本研究的目的是分析成年小鼠脑内NGF的含量是否会受到胆囊收缩素-8（CCK-8）外周给药的影响，CCK-8是一种著名的神经肽，对脑内神经元具有刺激作用，并在人类和啮齿动物中促进多种神经行为效应。3. 通过使用一种灵敏的NGF免疫酶测定法，分析腹腔注射CCK-8对成年雄性小鼠海马、皮质、下丘脑和垂体中NGF浓度的剂量反应和时间进程效应。还研究了用选择性CCK(A)和CCK(B)受体拮抗剂以及阿托品预处理对NGF对CCK注射反应的影响。4. CCK-8的作用呈剂量和时间依赖性，注射8 nmol·kg⁻¹可使下丘脑和垂体中的NGF水平增加3倍，海马中的NGF水平增加约60%。在皮质中未观察到影响。用选择性CCK(A)受体拮抗剂预处理可阻断CCK诱导的下丘脑和垂体中NGF的增加。在海马中，用CCK(B)受体拮抗剂也得到了相同的效果。用阿托品预处理可抑制CCK对所有检测脑区中NGF水平的诱导作用。5. 我们的结果表明，腹腔注射CCK-8可通过一种似乎部分由迷走神经传入介导的机制调节脑内NGF水平，这表明该神经肽可能是一种有用的药理学方法，可提高与神经营养因子缺乏相关的神经病理学中内源性NGF水平。