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啮齿动物对声音惊吓的习惯化和前脉冲抑制

Habituation and prepulse inhibition of acoustic startle in rodents.

作者信息

Valsamis Bridget, Schmid Susanne

机构信息

Anatomy and Cell Biology, Schulich School of Medicine and Dentistry, University of Western Ontario.

出版信息

J Vis Exp. 2011 Sep 1(55):e3446. doi: 10.3791/3446.

Abstract

The acoustic startle response is a protective response, elicited by a sudden and intense acoustic stimulus. Facial and skeletal muscles are activated within a few milliseconds, leading to a whole body flinch in rodents(1). Although startle responses are reflexive responses that can be reliably elicited, they are not stereotypic. They can be modulated by emotions such as fear (fear potentiated startle) and joy (joy attenuated startle), by non-associative learning processes such as habituation and sensitization, and by other sensory stimuli through sensory gating processes (prepulse inhibition), turning startle responses into an excellent tool for assessing emotions, learning, and sensory gating, for review see( 2, 3). The primary pathway mediating startle responses is very short and well described, qualifying startle also as an excellent model for studying the underlying mechanisms for behavioural plasticity on a cellular/molecular level(3). We here describe a method for assessing short-term habituation, long-term habituation and prepulse inhibition of acoustic startle responses in rodents. Habituation describes the decrease of the startle response magnitude upon repeated presentation of the same stimulus. Habituation within a testing session is called short-term habituation (STH) and is reversible upon a period of several minutes without stimulation. Habituation between testing sessions is called long-term habituation (LTH)(4). Habituation is stimulus specific(5). Prepulse inhibition is the attenuation of a startle response by a preceding non-startling sensory stimulus(6). The interval between prepulse and startle stimulus can vary from 6 to up to 2000 ms. The prepulse can be any modality, however, acoustic prepulses are the most commonly used. Habituation is a form of non-associative learning. It can also be viewed as a form of sensory filtering, since it reduces the organisms' response to a non-threatening stimulus. Prepulse inhibition (PPI) was originally developed in human neuropsychiatric research as an operational measure for sensory gating(7). PPI deficits may represent the interface of "psychosis and cognition" as they seem to predict cognitive impairment(8-10). Both habituation and PPI are disrupted in patients suffering from schizophrenia(11), and PPI disruptions have shown to be, at least in some cases, amenable to treatment with mostly atypical antipsychotics(12, 13). However, other mental and neurodegenerative diseases are also accompanied by disruption in habituation and/or PPI, such as autism spectrum disorders (slower habituation), obsessive compulsive disorder, Tourette's syndrome, Huntington's disease, Parkinson's disease, and Alzheimer's Disease (PPI)(11, 14, 15) Dopamine induced PPI deficits are a commonly used animal model for the screening of antipsychotic drugs(16), but PPI deficits can also be induced by many other psychomimetic drugs, environmental modifications and surgical procedures.

摘要

听觉惊跳反应是一种保护性反应,由突然而强烈的听觉刺激引发。在啮齿动物中,面部和骨骼肌会在几毫秒内被激活,导致全身惊跳(1)。尽管惊跳反应是可被可靠诱发的反射性反应,但它们并非刻板不变。它们可被恐惧(恐惧增强惊跳)和喜悦(喜悦减弱惊跳)等情绪、习惯化和敏感化等非联想学习过程,以及通过感觉门控过程(前脉冲抑制)的其他感觉刺激所调节,从而使惊跳反应成为评估情绪、学习和感觉门控的绝佳工具,相关综述见(2, 3)。介导惊跳反应的主要通路非常短且已被充分描述,这也使惊跳成为在细胞/分子水平研究行为可塑性潜在机制的优秀模型(3)。我们在此描述一种评估啮齿动物听觉惊跳反应的短期习惯化、长期习惯化和前脉冲抑制的方法。习惯化描述了在重复呈现相同刺激时惊跳反应幅度的降低。在一次测试过程中的习惯化称为短期习惯化(STH),在几分钟无刺激的时间段后是可逆的。不同测试过程之间的习惯化称为长期习惯化(LTH)(4)。习惯化是刺激特异性的(5)。前脉冲抑制是由先前的非惊跳感觉刺激引起的惊跳反应减弱(6)。前脉冲与惊跳刺激之间的间隔可从6毫秒到2000毫秒不等。前脉冲可以是任何形式,然而,听觉前脉冲是最常用的。习惯化是一种非联想学习形式。它也可被视为一种感觉过滤形式,因为它减少了生物体对非威胁性刺激的反应。前脉冲抑制(PPI)最初是在人类神经精神研究中作为感觉门控的一种操作指标而开发出来的(7)。PPI缺陷可能代表“精神病与认知”的界面,因为它们似乎可预测认知障碍(8 - 10)。习惯化和PPI在精神分裂症患者中均受到破坏(11),并且PPI破坏已被证明,至少在某些情况下,大多可用非典型抗精神病药物进行治疗(12, 13)。然而,其他精神和神经退行性疾病也伴有习惯化和/或PPI的破坏,如自闭症谱系障碍(习惯化较慢)、强迫症、妥瑞氏症、亨廷顿舞蹈症、帕金森病和阿尔茨海默病(PPI)(11, 14, 15)。多巴胺诱导的PPI缺陷是用于筛选抗精神病药物的常用动物模型(16),但PPI缺陷也可由许多其他拟精神病药物、环境改变和外科手术诱发。

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