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大鼠齿状区强直后长期增强作用增加突触后411B免疫反应性。

Posttetanic long-term potentiation in rat dentate area increases postsynaptic 411B immunoreactivity.

作者信息

Bullock S, Lössner B, Krug M, Frey S, Rose S P, Matthies H

机构信息

Brain Research Group, Open University, Milton Keynes, England.

出版信息

J Neurochem. 1990 Aug;55(2):708-13. doi: 10.1111/j.1471-4159.1990.tb04190.x.

Abstract

411B is a monoclonal antibody raised to chick forebrain postsynaptic densities (PSDs) which also recognises an antigen in brain tissue from adult Wistar rats but not liver, heart, or lung. This antigen is enriched in the PSD fraction and appears to be a useful biochemical marker for plastic changes of postsynaptic structures in the rat brain. The aim of this study was to investigate whether 411B immunoreactivity is changed in various hippocampal subregions by post-tetanic long-term potentiation (LTP). LTP was elicited in freely moving rats by applying four trains of 300 square-wave pulses (frequency 200 Hz, pulse duration 0.2 ms, and intensity 300 mA) into the right perforant path; this included an increase in transmission efficacy at the ipsilateral perforant path-granular cell synapse of the dentate gyrus lasting several days. Eight hours after tetanisation, antigens recognised by monoclonal 411B and a polyclonal anti-actin antiserum were assayed in lysed homogenates of ipsi- and contralateral CA1. CA3, and CA4/dentate area hippocampal subfields as well as in visual cortex, cerebellum, and olfactory bulb dissected from LTP rats, and compared to passive controls. Under these experimental conditions, tetanisation of the perforant path resulted in a significant increase in the titre of 411B in the ipsilateral CA4/dentate area subfield (+34.0%; p less than 0.001) compared with passive controls, whereas in all other brain regions studied no differences between experimental and control rats were observed. In no region were anti-actin titres significantly different from controls.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

411B是一种针对鸡前脑突触后致密物(PSD)产生的单克隆抗体,它也能识别成年Wistar大鼠脑组织中的一种抗原,但不能识别肝脏、心脏或肺中的抗原。这种抗原在PSD组分中含量丰富,似乎是大鼠脑突触后结构可塑性变化的一种有用的生化标志物。本研究的目的是探讨强直后长期增强(LTP)是否会使411B免疫反应性在海马各亚区发生改变。通过向自由活动的大鼠右侧穿通路径施加四串300个方波脉冲(频率200Hz,脉冲持续时间0.2ms,强度300mA)来诱发LTP;这包括齿状回同侧穿通路径-颗粒细胞突触处的传递效能增加,持续数天。强直刺激8小时后,在同侧和对侧CA1、CA3以及CA4/齿状回区域海马亚区的裂解匀浆中,以及从接受LTP处理的大鼠分离出的视皮层、小脑和嗅球中,检测单克隆411B和多克隆抗肌动蛋白抗血清识别的抗原,并与被动对照组进行比较。在这些实验条件下,与被动对照组相比,穿通路径的强直刺激导致同侧CA4/齿状回区域亚区中411B的滴度显著增加(+34.0%;p小于0.001),而在所有其他研究的脑区中,未观察到实验大鼠和对照大鼠之间存在差异。在任何区域,抗肌动蛋白滴度与对照组均无显著差异。(摘要截断于250字)

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