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成纤维细胞生长因子 2 增强条件性恐惧的消退并减少其更新。

Fibroblast growth factor-2 enhances extinction and reduces renewal of conditioned fear.

机构信息

School of Psychology, The University of New South Wales, Sydney, NSW, Australia.

出版信息

Neuropsychopharmacology. 2010 May;35(6):1348-55. doi: 10.1038/npp.2010.3. Epub 2010 Feb 3.

Abstract

Anxiety disorders are increasingly prevalent in society; hence, there is a need to improve on existing treatments for such disorders. Fibroblast growth factor-2 (FGF2), a mitogen that is involved in brain development and regeneration, has been shown to both facilitate long-term extinction of fear and reduce stress-precipitated relapse in rats. Extinction is the laboratory analog of exposure-based therapies in humans. In this study, we continued to investigate the clinical potential of FGF2 as a pharmacological enhancer of extinction by examining its effect on renewal, a common type of relapse. In all experiments, rats were trained to fear a white noise-conditioned stimulus, and then this learned fear was extinguished the following day. Rats received systemic injections of FGF2 or vehicle immediately after extinction training. At test, on the day after extinction training, levels of freezing elicited by the white noise in either the extinction context or the original training context were measured. FGF2-treated rats showed less renewal of fear when tested in the original training context than did vehicle-treated rats. This pattern occurred even when vehicle rats were given double the amount of extinction training, and when FGF2-treated rats were given equivalent exposure to the extinction context. These results show that FGF2 facilitates long-term extinction and attenuates relapse, and thus highlight its potential as a novel pharmacological adjunct to exposure therapy.

摘要

焦虑症在社会中越来越普遍;因此,有必要改进现有的此类疾病治疗方法。成纤维细胞生长因子 2(FGF2)是一种参与大脑发育和再生的有丝分裂原,已被证明既能促进恐惧的长期消退,又能减少大鼠应激引发的复发。消退是人类暴露疗法的实验室模拟。在这项研究中,我们通过检查其对恢复的影响,继续研究 FGF2 作为一种增强消退的药理学增强剂的临床潜力,恢复是一种常见的复发类型。在所有实验中,大鼠被训练对一种白噪声条件刺激产生恐惧,然后在第二天进行这种习得的恐惧消退。在消退训练后,大鼠立即接受系统注射 FGF2 或载体。在测试中,在消退训练后的第二天,通过测量大鼠在原始训练环境或原始训练环境中听到白噪声时的冻结水平来测量恐惧的恢复程度。与接受载体治疗的大鼠相比,接受 FGF2 治疗的大鼠在原始训练环境中恐惧的恢复程度较低。即使给载体大鼠进行两倍的消退训练,并且给 FGF2 治疗的大鼠进行相同的消退环境暴露时,也会出现这种模式。这些结果表明 FGF2 促进了长期消退并减轻了复发,因此突出了其作为暴露疗法的新型药理学辅助手段的潜力。

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