Long Qianfa, Upadhya Dinesh, Hattiangady Bharathi, Kim Dong-Ki, An Su Yeon, Shuai Bing, Prockop Darwin J, Shetty Ashok K
Institute for Regenerative Medicine, Texas A&M Health Science Center College of Medicine, Temple, TX 76502.
Olin E. Teague Veterans' Medical Center, Central Texas Veterans Health Care System, Temple, TX 76502.
Proc Natl Acad Sci U S A. 2017 Apr 25;114(17):E3536-E3545. doi: 10.1073/pnas.1703920114. Epub 2017 Apr 10.
Status epilepticus (SE), a medical emergency that is typically terminated through antiepileptic drug treatment, leads to hippocampus dysfunction typified by neurodegeneration, inflammation, altered neurogenesis, as well as cognitive and memory deficits. Here, we examined the effects of intranasal (IN) administration of extracellular vesicles (EVs) secreted from human bone marrow-derived mesenchymal stem cells (MSCs) on SE-induced adverse changes. The EVs used in this study are referred to as A1-exosomes because of their robust antiinflammatory properties. We subjected young mice to pilocarpine-induced SE for 2 h and then administered A1-exosomes or vehicle IN twice over 24 h. The A1-exosomes reached the hippocampus within 6 h of administration, and animals receiving them exhibited diminished loss of glutamatergic and GABAergic neurons and greatly reduced inflammation in the hippocampus. Moreover, the neuroprotective and antiinflammatory effects of A1-exosomes were coupled with long-term preservation of normal hippocampal neurogenesis and cognitive and memory function, in contrast to waned and abnormal neurogenesis, persistent inflammation, and functional deficits in animals receiving vehicle. These results provide evidence that IN administration of A1-exosomes is efficient for minimizing the adverse effects of SE in the hippocampus and preventing SE-induced cognitive and memory impairments.
癫痫持续状态(SE)是一种医疗急症,通常通过抗癫痫药物治疗来终止,它会导致海马体功能障碍,其特征为神经退行性变、炎症、神经发生改变以及认知和记忆缺陷。在此,我们研究了经鼻(IN)给予人骨髓间充质干细胞(MSC)分泌的细胞外囊泡(EV)对SE诱导的不良变化的影响。本研究中使用的EV因其强大的抗炎特性而被称为A1-外泌体。我们使幼鼠接受匹鲁卡品诱导的SE 2小时,然后在24小时内分两次经鼻给予A1-外泌体或赋形剂。A1-外泌体在给药后6小时内到达海马体,接受它们的动物海马体中谷氨酸能和γ-氨基丁酸能神经元的损失减少,炎症也大大减轻。此外,与接受赋形剂的动物中减弱和异常的神经发生、持续的炎症以及功能缺陷相比,A1-外泌体的神经保护和抗炎作用与正常海马体神经发生以及认知和记忆功能的长期保存相关。这些结果证明,经鼻给予A1-外泌体可有效减轻SE对海马体的不良影响,并预防SE诱导的认知和记忆损害。