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成年猴子在海马体、杏仁核和眶额皮质的新生损伤后存在听觉惊跳和前脉冲抑制缺陷。

Acoustic startle and prepulse inhibition deficits in adult monkeys with neonatal lesions of the hippocampus, amygdala and orbital frontal cortex.

机构信息

Psychology Department, University of Hawaii at Hilo, Hilo, HI 96720.

Emory National Primate Research Center Emory University, Atlanta, GA, United States.

出版信息

Behav Brain Res. 2023 Feb 13;438:114170. doi: 10.1016/j.bbr.2022.114170. Epub 2022 Oct 22.

Abstract

Sensory-motor gating, the process of filtering sensory stimuli to modulate motor responses, is impaired in many psychiatric diseases but especially schizophrenia. Sensory-motor gating assessed with the prepulse inhibition paradigm (PPI) measures startle in response to preceding acoustic stimuli. PPI studies in rodents have consistently found that neonatal hippocampal lesions impair sensory-motor gating in adult animals, but its applicability to primates has yet to be tested. The study examined acoustic startle responses and PPI in adult rhesus monkeys with neonatal lesions of the hippocampus (Neo-Hibo), amygdala (Neo-Aibo), and orbital frontal cortex areas 11 and 13 (Neo-Oasp) and with sham-operations (Neo-C). All monkeys were initially habituated to the startle apparatus and assayed for acoustic startle response curves. Subsequently, PPI was measured with the prepulse occurring at 60, 120, 240, 480, 1000 and 5000 msec prior to the pulse onset. No significant group differences in baseline startle were found. Compared to Neo-C monkeys, Neo-Hibo monkeys showed normal startle curves as well as normal PPI at short prepulse delays but prepulse facilitation (PPF) at longer prepulse intervals. Neo-Aibo monkeys displayed enhanced startle responses with only minor changes in PPI, whereas Neo-Oasp monkeys had severe dampening of startle responses and impaired PPI at shorter prepulse intervals. These results support prior evidence from rodent literature of the involvement of each of these areas in the development of the complex cortico-limbic circuit modulating sensory-motor gating and may shade light on the specific neural structures associated with deficits in PPI reported in neuropsychiatric disorders, such as schizophrenia, autism spectrum disorders, and post-traumatic disorders.

摘要

感觉运动门控,即过滤感觉刺激以调节运动反应的过程,在许多精神疾病中受到损害,尤其是精神分裂症。使用前脉冲抑制范式 (PPI) 评估的感觉运动门控测量对先前的声音刺激的惊跳反应。啮齿动物的 PPI 研究一致发现,新生海马损伤会损害成年动物的感觉运动门控,但尚未对灵长类动物进行测试。该研究检查了患有新生海马 (Neo-Hibo)、杏仁核 (Neo-Aibo) 和眶额皮质区域 11 和 13 (Neo-Oasp) 损伤以及假手术 (Neo-C) 的成年恒河猴的听觉惊跳反应和 PPI。所有猴子最初都适应了惊跳装置,并对听觉惊跳反应曲线进行了测定。随后,在脉冲开始前 60、120、240、480、1000 和 5000 毫秒时发生的预备脉冲测量 PPI。基线惊跳无显著组间差异。与 Neo-C 猴子相比,Neo-Hibo 猴子表现出正常的惊跳曲线和正常的短预备脉冲延迟时的 PPI,但在较长的预备脉冲间隔时出现预备脉冲促进 (PPF)。Neo-Aibo 猴子表现出增强的惊跳反应,仅有 PPI 的微小变化,而 Neo-Oasp 猴子的惊跳反应严重减弱,在较短的预备脉冲间隔时 PPI 受损。这些结果支持来自啮齿动物文献的先前证据,即这些区域中的每一个都参与了调节感觉运动门控的复杂皮质-边缘回路的发育,并且可能阐明与精神分裂症、自闭症谱系障碍和创伤后障碍等神经精神障碍中报道的 PPI 缺陷相关的特定神经结构。

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