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纳米给药增强脊髓损伤的神经保护作用。

Nanowired drug delivery to enhance neuroprotection in spinal cord injury.

机构信息

Department of Chemistry and Biochemistry, University of Arkansas Fayetteville, Fayetteville, AR 72701, USA.

出版信息

CNS Neurol Disord Drug Targets. 2012 Feb;11(1):86-95. doi: 10.2174/187152712799960727.

Abstract

Spinal cord injury (SCI) is a serious clinical situation for which no suitable drug therapy exists. SCI often results in paraplegia or quadriplegia and, apart from the personal trauma leads to huge costs to society for rehabilitation or day-to-day life support. Sensory motor dysfunction following SCI is mainly a consequence of the slowly progressing cord pathology after primary injury that worsens over tine. Thus, almost all sensory and motor nerve control and pathways passing through spinal cord and reflexes are compromised in SCI patients. As a result their peripheral nervous system, autonomic nervous function and central nervous system regulations are adversely affected. Experiments carried out in our laboratory show that various therapeutic agents, if given within 10 to 30 minutes after primary SCI could correct morphological changes to a certain extent. In these rat models of SCI reduction in cord pathology, e.g., bloodspinal cord barrier (BSCB) breakdown, edema formation and cell injury by the neuroprotective agents that also limited sensory motor dysfunction and improved functional behavior. However, these drugs if given beyond 30 minutes after SCI showed a markedly reduced neuroprotective efficacy. Thus, new strategies are needed to enhance neuroprotection in SCI to prevent structural and functional changes over longer periods of time. To that end our laboratory has initiated a series of investigations in which nanowired delivery of various neurotherapeutic agents are applied after different time periods of SCI, that resulted in a much better outcome than with the parent compounds under identical conditions. The superior neuroprotective activity of nanowired compound delivery could be due to a reduced metabolism of active compounds in the central nervous system (CNS) or by sustained release of the drug for longer times. In addition, nanowired drugs may penetrate the CNS faster and could reach widespread areas once entering the spinal cord. Thus, nanowired drug delivery to treat SCI may have potential therapeutic value. These aspects of nanowired drug delivery to enhance neuroprotection in SCI are discussed in this review based on our own investigations.

摘要

脊髓损伤 (SCI) 是一种严重的临床情况,目前尚无合适的药物治疗方法。SCI 常导致截瘫或四肢瘫痪,除了个人创伤外,还会给社会带来巨大的康复或日常生活支持成本。SCI 后的感觉运动功能障碍主要是原发性损伤后脊髓病理学缓慢进展导致的,随着时间的推移而恶化。因此,SCI 患者几乎所有的感觉和运动神经控制以及穿过脊髓的通路和反射都受到了损害。结果,他们的周围神经系统、自主神经系统功能和中枢神经系统调节受到了不利影响。我们实验室进行的实验表明,如果在原发性 SCI 后 10 至 30 分钟内给予各种治疗剂,可以在一定程度上纠正形态学变化。在这些 SCI 大鼠模型中,神经保护剂减少了脊髓病理学变化,例如血脊髓屏障 (BSCB) 破裂、水肿形成和细胞损伤,同时也限制了感觉运动功能障碍并改善了功能行为。然而,如果在 SCI 后 30 分钟以上给予这些药物,则神经保护效果明显降低。因此,需要新的策略来增强 SCI 中的神经保护,以防止更长时间内的结构和功能变化。为此,我们实验室已经启动了一系列研究,在这些研究中,在不同的 SCI 后时间段内应用各种神经治疗剂的纳米线输送,与相同条件下的母体化合物相比,结果要好得多。纳米线化合物输送的优越神经保护活性可能是由于中枢神经系统 (CNS) 中活性化合物的代谢减少,或者药物的持续释放时间更长。此外,纳米线药物可能更快地穿透 CNS,并在进入脊髓后可以到达广泛的区域。因此,纳米线药物输送治疗 SCI 可能具有潜在的治疗价值。本文基于我们自己的研究,讨论了纳米线药物输送增强 SCI 中神经保护的这些方面。

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