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氧化石墨烯可预防外侧杏仁核功能障碍性突触可塑性,并逆转大鼠的长期焦虑行为。

Graphene oxide prevents lateral amygdala dysfunctional synaptic plasticity and reverts long lasting anxiety behavior in rats.

机构信息

Neuron Physiology and Technology Lab, International School for Advanced Studies (SISSA), Neuroscience, Via Bonomea 265, 34136, Trieste, Italy.

Catalan Institute of Nanoscience and Nanotechnology (ICN2), CSIC and BIST, Campus UAB, Bellaterra, 08193, Barcelona, Spain.

出版信息

Biomaterials. 2021 Apr;271:120749. doi: 10.1016/j.biomaterials.2021.120749. Epub 2021 Mar 4.

Abstract

Engineered small graphene oxide (s-GO) sheets were previously shown to reversibly down-regulate glutamatergic synapses in the hippocampus of juvenile rats, disclosing an unexpected translational potential of these nanomaterials to target selective synapses in vivo. Synapses are anatomical specializations acting in the Central Nervous System (CNS) as functional interfaces among neurons. Dynamic changes in synaptic function, named synaptic plasticity, are crucial to learning and memory. More recently, pathological mechanisms involving dysfunctional synaptic plasticity were implicated in several brain diseases, from dementia to anxiety disorders. Hyper-excitability of glutamatergic neurons in the lateral nucleus of the amygdala complex (LA) is substantially involved in the storage of aversive memory induced by stressful events enabling post-traumatic stress disorder (PTSD). Here we translated in PTSD animal model the ability of s-GO, when stereotaxically administered to hamper LA glutamatergic transmission and to prevent the behavioral response featured in long-term aversive memory. We propose that s-GO, by interference with glutamatergic plasticity, impair LA-dependent memory retrieval related to PTSD.

摘要

先前的研究表明,工程化小石墨烯氧化物(s-GO)片能够可逆地下调幼年大鼠海马中的谷氨酸能突触,揭示了这些纳米材料在体内靶向选择性突触的意外转化潜力。突触是中枢神经系统(CNS)中的解剖学特化结构,作为神经元之间的功能接口。突触功能的动态变化,称为突触可塑性,对于学习和记忆至关重要。最近,涉及突触可塑性功能障碍的病理机制被牵涉到多种脑疾病,从痴呆症到焦虑症。杏仁核复合体(LA)外侧核中谷氨酸能神经元的过度兴奋与由应激事件引起的厌恶记忆的储存密切相关,使创伤后应激障碍(PTSD)成为可能。在这里,我们在 PTSD 动物模型中转化了 s-GO 的能力,当立体定向给予 s-GO 以阻碍 LA 谷氨酸能传递并防止与 PTSD 相关的长期厌恶记忆的行为反应。我们提出,s-GO 通过干扰谷氨酸能可塑性,损害与 PTSD 相关的 LA 依赖性记忆检索。

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