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齿状回中配对脉冲反应的调制:产前蛋白质营养不良的影响。

Modulation of paired-pulse responses in the dentate gyrus: effects of prenatal protein malnutrition.

作者信息

Bronzino J D, Blaise J H, Mokler D J, Galler J R, Morgane P J

机构信息

Department of Engineering, Trinity College, 300 Summit Street, Hartford, CT, USA.

出版信息

Brain Res. 1999 Dec 4;849(1-2):45-57. doi: 10.1016/s0006-8993(99)02071-5.

Abstract

Since our major hypothesis is that prenatal protein malnutrition significantly affects hippocampal neuroplasticity, this study examined the effects of prenatal protein malnutrition on the modulation of dentate granule cell excitability in freely moving rats at 15, 30 and 90 days of age across the vigilance states of quiet waking (QW), slow-wave sleep (SWS) and rapid eye movement (REM) sleep. Using paired-pulse stimulation, the paired-pulse index (PPI), a measure of the type and degree of modulation of dentate granule cell excitability elicited by stimulation of the medial perforant path, was obtained for each vigilance state at each stage of development. Four specific measures of granule cell excitability were computed, namely, PPI using both population spike amplitude (PSA) and EPSP slope measures, absolute values of PSA(1) and EPSP(1) slope. PPI values obtained at 15, 30 and 90 days of age, however, were altered during normal ontogenetic development, but not by vigilance state. At 15 days of age, the malnourished group exhibits greater early inhibition of the PPI using the PSA measure at IPIs between 20 and 30 ms regardless of vigilance state, while at 30 days of age, the malnourished group exhibits greater facilitation at IPIs between 50 and 70 ms during QW and SWS, but not during REM sleep. In the control adult (PND90) and juvenile (PND30) animal, PSA(1) values are significantly higher during SWS than in QW or REM sleep. However, for the younger malnourished animals (PND15 and PND30), PSA(1) values were found to be significantly greater during REM sleep rather than SWS. Therefore, as the animal matures, there appears to be a shift in vigilance state dependent synaptic transmission through the hippocampal trisynaptic circuit from REM sleep to SWS in both control and malnourished animals, with the change occurring later in malnourished animals when compared to control ones. Furthermore, our findings suggests that prenatal protein malnutrition significantly alters modulation of dentate granule cell excitability (i.e., PPI values using the PSA measure) during the earlier stages of development but not in adulthood.

摘要

由于我们的主要假设是产前蛋白质营养不良会显著影响海马体神经可塑性,本研究考察了产前蛋白质营养不良对15日龄、30日龄和90日龄自由活动大鼠在安静觉醒(QW)、慢波睡眠(SWS)和快速眼动(REM)睡眠等警觉状态下齿状颗粒细胞兴奋性调节的影响。使用配对脉冲刺激,在发育的每个阶段,针对每种警觉状态获取配对脉冲指数(PPI),它是通过刺激内侧穿通路径引发的齿状颗粒细胞兴奋性调节的类型和程度的一种度量。计算了颗粒细胞兴奋性的四个具体指标,即使用群体峰电位幅度(PSA)和兴奋性突触后电位(EPSP)斜率测量的PPI、PSA(1)的绝对值和EPSP(1)斜率。然而,在正常个体发育过程中,15日龄、30日龄和90日龄时获得的PPI值会发生改变,但不受警觉状态影响。在15日龄时,无论警觉状态如何,营养不良组在20至30毫秒的脉冲间隔(IPI)下使用PSA测量时对PPI表现出更大的早期抑制,而在30日龄时,营养不良组在QW和SWS期间,在50至70毫秒的IPI下表现出更大的易化作用,但在REM睡眠期间则不然。在对照成年(出生后第90天,PND90)和幼年(出生后第30天,PND30)动物中,SWS期间的PSA(1)值显著高于QW或REM睡眠期间。然而,对于较年幼的营养不良动物(PND15和PND30),发现REM睡眠期间的PSA(1)值显著大于SWS期间。因此,随着动物成熟,在对照和营养不良动物中,通过海马三突触回路的警觉状态依赖性突触传递似乎从REM睡眠转变为SWS,与对照动物相比,营养不良动物的这种变化发生得更晚。此外,我们的研究结果表明,产前蛋白质营养不良在发育的早期阶段会显著改变齿状颗粒细胞兴奋性的调节(即使用PSA测量的PPI值),但在成年期则不会。

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