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戊四氮与吗啡在状态依赖记忆模型中的相互作用:CREB信号通路的作用

Pentylenetetrazol and Morphine Interaction in a State-dependent Memory Model: Role of CREB Signaling.

作者信息

Tavassoli Marziyeh, Ardjmand Abolfazl

机构信息

Institute for Basic Sciences, Physiology Research Center, Kashan University of Medical Sciences, Kashan, Iran.

Department of Physiology, School of Medicine, Kashan University of Medical Sciences, Kashan, Iran.

出版信息

Basic Clin Neurosci. 2020 Jul-Aug;11(4):557-572. doi: 10.32598/bcn.11.4.1482.1. Epub 2020 Jul 1.

Abstract

INTRODUCTION

State-dependent (STD) memory is a process, in which the learned information can be optimally retrieved only when the subject is in the state similar to the encoding phase. This phenomenon has been widely studied with morphine. Several studies have reported that Pentylenetetrazole (PTZ) impairs memory in experimental animal models. Due to certain mechanistic interactions between morphine and PTZ, it is hypothesized that PTZ may interfere with the morphine-STD. The cyclic adenosine monophosphate Response Element-Binding (CREB) is considered as the main downstream marker for long-term memory. This study was designed to determine the possible interaction between PTZ and morphine STD and the presumable changes in CREB mRNA.

METHODS

In an Inhibitory Avoidance (IA) model, posttraining morphine (2.5, 5, and 7.5 mg/ kg-i.p.) was used. The pre-test morphine was evaluated for morphine-induced STD memory. Moreover, the effect of a pre-test PTZ (60 mg/kg-i.p.) was studied along with morphine STD. Locomotion testing was carried out using open-field. Eventually, using real-time-PCR, the CREB mRNA changes in the hippocampus were evaluated.

RESULTS

Posttraining MOR (7.5 mg/kg-i.p.) impaired IA memory (P<0.001). The pre-test injection of similar doses of morphine recovered the morphine-induced memory impairment (P<0.001). The pre-test PTZ impaired the IA memory recall (P<0.001); however, the pre-test PTZ along with morphine STD potentiated the morphine-induced STD (P<0.001). Alterations in CREB mRNA were observed in all groups. No difference was seen in the locomotor activity.

CONCLUSION

Presumably, the certain interactive effect of PTZ on morphine-induced STD is mediated through gamma-aminobutyric acid and opioid systems via CREB signaling.

摘要

引言

状态依赖(STD)记忆是一种过程,其中只有当主体处于与编码阶段相似的状态时,所学信息才能被最佳地检索出来。这种现象已通过吗啡进行了广泛研究。多项研究报告称,戊四氮(PTZ)会损害实验动物模型中的记忆。由于吗啡与PTZ之间存在某些机制相互作用,因此推测PTZ可能会干扰吗啡诱导的STD。环磷酸腺苷反应元件结合蛋白(CREB)被认为是长期记忆的主要下游标志物。本研究旨在确定PTZ与吗啡STD之间可能的相互作用以及CREB mRNA的推测性变化。

方法

在抑制性回避(IA)模型中,使用训练后吗啡(2.5、5和7.5毫克/千克腹腔注射)。对测试前吗啡进行评估,以研究吗啡诱导的STD记忆。此外,还研究了测试前PTZ(60毫克/千克腹腔注射)与吗啡STD的联合作用。使用旷场实验进行运动测试。最终,通过实时聚合酶链反应评估海马体中CREB mRNA的变化。

结果

训练后吗啡(7.5毫克/千克腹腔注射)损害了IA记忆(P<0.001)。测试前注射相似剂量的吗啡可恢复吗啡诱导的记忆损害(P<0.001)。测试前PTZ损害了IA记忆回忆(P<0.001);然而,测试前PTZ与吗啡STD联合使用可增强吗啡诱导的STD(P<0.001)。所有组均观察到CREB mRNA的变化。运动活性未见差异。

结论

推测PTZ对吗啡诱导的STD的特定交互作用是通过γ-氨基丁酸和阿片类系统经由CREB信号传导介导的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/520d/7878041/1f4afe558241/BCN-11-557-g001.jpg

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