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TiO2 纳米载体递送 DL-3-正丁基苯酞(DL-NBP)减轻震荡性颅脑损伤后血脑屏障破坏、脑水肿形成和神经元损伤。

TiO-Nanowired Delivery of DL-3-n-butylphthalide (DL-NBP) Attenuates Blood-Brain Barrier Disruption, Brain Edema Formation, and Neuronal Damages Following Concussive Head Injury.

机构信息

Department of Neurology, Bethune International Peace Hospital, Zhongshan Road (West), Shijiazhuang, Hebei Province, China.

Cerebrovascular Research Laboratory, Department of Surgical Sciences, Anesthesiology & Intensive Care Medicine, Uppsala University Hospital, SE-751 85, Uppsala, Sweden.

出版信息

Mol Neurobiol. 2018 Jan;55(1):350-358. doi: 10.1007/s12035-017-0746-5.

DOI:10.1007/s12035-017-0746-5
PMID:28856586
Abstract

DL-3-n-butylphthalide (DL-NBP) is one of the constituents of Chinese celery extract that is used to treat stroke, dementia, and ischemic diseases. However, its role in traumatic brain injury is less well known. In this investigation, neuroprotective effects of DL-NBP in concussive head injury (CHI) on brain pathology were explored in a rat model. CHI was inflicted in anesthetized rats by dropping a weight of 114.6 g from a height of 20 cm through a guide tube on the exposed right parietal bone inducing an impact of 0.224 N and allowed them to survive 4 to 24 h after the primary insult. DL-NBP was administered (40 or 60 mg/kg, i.p.) 2 and 4 h after injury in 8-h survival group and 8 and 12 h after trauma in 24-h survival group. In addition, TiO-nanowired delivery of DL-NBP (20 or 40 mg/kg, i.p.) in 8 and 24 h CHI rats was also examined. Untreated CHI showed a progressive increase in blood-brain barrier (BBB) breakdown to Evans blue albumin (EBA) and radioiodine (I), edema formation, and neuronal injuries. The magnitude and intensity of these pathological changes were most marked in the left hemisphere. Treatment with DL-NBP significantly reduced brain pathology in CHI following 8 to 12 h at 40-mg dose. However, 60-mg dose is needed to thwart brain pathology at 24 h following CHI. On the other hand, TiO-DL-NBP was effective in reducing brain damage up to 8 or 12 h using a 20-mg dose and only 40-mg dose was needed for neuroprotection in CHI at 24 h. These observations are the first to suggest that (i) DL-NBP is quite effective in reducing brain pathology and (ii) nanodelivery of DL-NBP has far more superior effects in CHI, not reported earlier.

摘要

DL-3-正丁基苯酞(DL-NBP)是中国芹菜提取物的成分之一,用于治疗中风、痴呆和缺血性疾病。然而,其在创伤性脑损伤中的作用知之甚少。在这项研究中,我们在大鼠模型中探讨了 DL-NBP 在震荡性颅脑损伤(CHI)中的神经保护作用。在麻醉大鼠中,通过引导管从 20cm 高处将 114.6g 的重量落在暴露的右顶骨上,造成 0.224N 的冲击,使它们在原发性损伤后 4 至 24 小时存活。在 8 小时存活组中,在损伤后 2 小时和 4 小时给予 DL-NBP(40 或 60mg/kg,ip),在 24 小时存活组中在创伤后 8 小时和 12 小时给予 DL-NBP。此外,还检查了 TiO 纳米递药的 DL-NBP(20 或 40mg/kg,ip)在 8 小时和 24 小时 CHI 大鼠中的作用。未治疗的 CHI 显示血脑屏障(BBB)对 Evans 蓝白蛋白(EBA)和放射性碘(I)的通透性逐渐增加,水肿形成和神经元损伤。这些病理变化的幅度和强度在左半球最为明显。在 40mg 剂量下,DL-NBP 在 CHI 后 8 至 12 小时可显著减轻脑病理学变化。然而,在 CHI 后 24 小时需要 60mg 剂量才能阻止脑病理学变化。另一方面,TiO-DL-NBP 在使用 20mg 剂量时可有效减少 8 或 12 小时的脑损伤,而在 CHI 中 24 小时神经保护仅需 40mg 剂量。这些观察结果首次表明:(i)DL-NBP 非常有效地减轻脑病理学变化;(ii)DL-NBP 的纳米递药在 CHI 中具有更好的效果,这在以前的研究中尚未报道。

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