Microglial Dystrophy and Spatial Learning Impairments Following Exposure to Multiple Early-life Stressors in Rats.

IF 2.4 Q4 NEUROSCIENCES
Syed Mujtaba, Nisha Patro, Ishan Kumar Patro
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引用次数: 0

Abstract

Background: Adversities during perinatal critical windows act as a major risk factor for several psychopathologies during adolescence and adulthood. Protein malnutrition, infections, neurotoxicant exposure and social stressors are significant adverse factors encountered by neonates born to socio-economically compromised societies.

Purpose: The purpose of this study is to understand how the cumulative exposure to multiple perinatal stressors can result in conditions that mimic various neurological disorders in affected individuals later in life. The present study aimed to understand the involvement of microglia, their activation, priming and dystrophy due to multi-hit exposure in severe spatial learning and memory impairments.

Methods: Naïve female Wistar rats (n = 32; 140-150 gm) were divided into control and low protein (LP) groups and fed with 20% and 8% protein diets, respectively, starting from 15 days prior to breeding, followed by mating with healthy males. Pups from both control and LP groups, with their respective mothers, were maintained on their respective diets throughout the experimental regime. Both control and LP F1 Pups were injected intraperitoneally either with deltamethrin (DLT; 0.7 mg/kg body weight) from postnatal day (PND) 1-7 or lipopolysaccharide (LPS; 0.3 mg/kg body weight) at PND3 then a booster on PND5 or both in combination on specified days, forming eight groups: Control, Control+DLT, Control+LPS, Control+DLT+LPS, LP, LP+LPS, LP+DLT and LP+DLT+LPS (Multi-hit). Microglial priming was studied using immunohistochemical procedures, and spatial learning and memory were estimated by the Morris water maze test in F1 rats (1, 3, 6 months).

Results: Results revealed that LP F1-treated rats were more susceptible to stressors with reduced brain weight, long-term microglial activation specifying primed states with enhanced expression of CD11b/CR3, MHC-II/OX-6 and ED2.

Conclusion: Multi-hit exposure induced dystrophic changes in a large population of microglia, causing severe learning and memory impairments, suggesting that perinatal multi-hit exposure might become a significant risk factor for developmental disorders in adulthood.

暴露于多种早期生活应激源后的小胶质细胞营养不良和空间学习障碍。
背景:围产期关键窗口期的逆境是青春期和成年期几种精神病理的主要危险因素。蛋白质营养不良、感染、神经毒物暴露和社会压力是出生在社会经济受损社会的新生儿遇到的重要不利因素。目的:本研究的目的是了解累积暴露于多种围产期应激源如何导致受影响个体在以后的生活中模仿各种神经系统疾病。本研究旨在了解小胶质细胞在严重空间学习和记忆障碍中的参与、激活、启动和营养不良。方法:Naïve雌性Wistar大鼠(n = 32;140 ~ 150 gm),分为对照组和低蛋白组,分别饲喂蛋白质含量为20%和8%的饲粮,于繁殖前15 d开始饲喂,随后与健康雄鼠交配。对照组和LP组的幼崽及其各自的母亲在整个实验过程中保持各自的饮食。对照组和LP F1幼崽分别腹腔注射溴氰菊酯(DLT);0.7 mg/kg体重)从出生日后(PND) 1-7或脂多糖(LPS;(0.3 mg/kg体重),然后在指定的日子给予PND5增强剂或两者结合,形成8组:对照组,对照组+DLT,对照组+LPS,对照组+DLT+LPS, LP, LP+LPS, LP+DLT和LP+DLT+LPS(多击)。采用免疫组织化学方法研究F1大鼠(1,3,6个月)的小胶质细胞启动,并通过Morris水迷宫测试评估空间学习和记忆。结果:结果显示LP f1处理的大鼠更易受到应激源的影响,脑重量减轻,长期小胶质细胞激活指定启动状态,CD11b/CR3, MHC-II/OX-6和ED2的表达增强。结论:多击暴露导致大量小胶质细胞营养不良改变,导致严重的学习和记忆障碍,提示围产期多击暴露可能成为成年期发育障碍的重要危险因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Annals of Neurosciences
Annals of Neurosciences NEUROSCIENCES-
CiteScore
2.40
自引率
0.00%
发文量
39
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