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肼屈嗪在大鼠脊髓损伤中的神经保护作用-减轻丙烯醛介导的损伤。

Neuroprotective role of hydralazine in rat spinal cord injury-attenuation of acrolein-mediated damage.

机构信息

Department of Basic Medical Sciences, College of Veterinary Medicine, Purdue University, West Lafayette, Indiana, USA; Weldon School of Biomedical Engineering, Purdue University, West Lafayette, Indiana, USA.

出版信息

J Neurochem. 2014 Apr;129(2):339-49. doi: 10.1111/jnc.12628. Epub 2013 Dec 15.

Abstract

Acrolein, an α,β-unsaturated aldehyde and a reactive product of lipid peroxidation, has been suggested as a key factor in neural post-traumatic secondary injury in spinal cord injury (SCI), mainly based on in vitro and ex vivo evidence. Here, we demonstrate an increase of acrolein up to 300%; the elevation lasted at least 2 weeks in a rat SCI model. More importantly, hydralazine, a known acrolein scavenger can provide neuroprotection when applied systemically. Besides effectively reducing acrolein, hydralazine treatment also resulted in significant amelioration of tissue damage, motor deficits, and neuropathic pain. This effect was further supported by demonstrating the ability of hydralazine to reach spinal cord tissue at a therapeutic level following intraperitoneal application. This suggests that hydralazine is an effective neuroprotective agent not only in vitro, but in a live animal model of SCI as well. Finally, the role of acrolein in SCI was further validated by the fact that acrolein injection into the spinal cord caused significant SCI-like tissue damage and motor deficits. Taken together, available evidence strongly suggests a critical causal role of acrolein in the pathogenesis of spinal cord trauma. Since acrolein has been linked to a variety of illness and conditions, we believe that acrolein-scavenging measures have the potential to be expanded significantly ensuring a broad impact on human health.

摘要

丙烯醛,一种α,β-不饱和醛和脂质过氧化的反应产物,被认为是脊髓损伤(SCI)中神经创伤后二次损伤的关键因素,主要基于体外和离体证据。在这里,我们在大鼠 SCI 模型中证明丙烯醛增加了 300%;这种升高至少持续了 2 周。更重要的是,肼屈嗪,一种已知的丙烯醛清除剂,当全身应用时可以提供神经保护。肼屈嗪治疗不仅能有效降低丙烯醛,还能显著改善组织损伤、运动功能障碍和神经病理性疼痛。这一效应通过证明腹腔内应用肼屈嗪能够达到治疗水平,从而进一步得到证实。这表明肼屈嗪不仅在体外,而且在 SCI 的活体动物模型中也是一种有效的神经保护剂。最后,丙烯醛在 SCI 中的作用进一步通过将丙烯醛注射到脊髓中引起类似 SCI 的组织损伤和运动功能障碍这一事实得到验证。综上所述,现有证据强烈表明丙烯醛在脊髓创伤发病机制中起着关键的因果作用。由于丙烯醛与多种疾病和状况有关,我们相信丙烯醛清除措施有可能得到显著扩展,从而对人类健康产生广泛影响。

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