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大鼠实验性变态反应性脑脊髓炎中脂质体脑定位的早期检测

Early detection of liposome brain localization in rat experimental allergic encephalomyelitis.

作者信息

Rousseau V, Denizot B, Le Jeune J J, Jallet P

机构信息

UPRES-EA 2169 Vectorisation Particulaire, Angers, France.

出版信息

Exp Brain Res. 1999 Apr;125(3):255-64. doi: 10.1007/s002210050681.

Abstract

Blood-brain barrier (BBB) permeability increases prior to the development of clinical signs in early-stage multiple sclerosis (MS). Detection of subtle changes would thus be helpful for diagnostic purposes and rapid therapeutic decisions before new episodes. Since multiple sclerosis and experimental allergic encephalomyelitis (EAE) have numerous common features, in particular BBB-permeability characteristics, and since we have previously shown that BBB localization is disturbed by tumors, embolism, and mannitol injection, we investigated BBB-liposome permeability in an EAE rat model. Twenty young male Lewis rats received a single intradermal inoculation of guinea-pig spinal cord. The effect of the Freund's adjuvant and spinal cord alone on brain permeability were also assessed. In order to compare solution permeability and liposome localization, radioactive liposomes and, 1 h later, 99mTc-DTPA were injected intravenously. Scintigraphic acquisitions were obtained to follow the biodistribution of radioactivity in the whole body. Each rat was subjected to a first examination before inoculation and then every two days until completion and may be considered as its own control. EAE induced a previously unreported increase in global-body permeability, probably due to inflammation. Liposome brain localization and brain/heart ratio were significantly different between normal animals and those with early-stage EAE (before appearance of clinical signs) and distinguished between different disease stages in clinically patent EAE. The index of disease progression was modified earlier than with 99mTc-DTPA injection. One explanation may be particle pick-up by circulating macrophages, which cross the BBB during this pathology. For clinical applications, experiments must be confirmed on models more reliable for human multiple sclerosis.

摘要

在早期多发性硬化症(MS)出现临床症状之前,血脑屏障(BBB)通透性会增加。因此,检测细微变化将有助于诊断,并在新发作前做出快速治疗决策。由于多发性硬化症和实验性变应性脑脊髓炎(EAE)有许多共同特征,特别是血脑屏障通透性特征,而且我们之前已经表明肿瘤、栓塞和甘露醇注射会扰乱血脑屏障定位,所以我们在EAE大鼠模型中研究了血脑屏障-脂质体通透性。20只年轻雄性Lewis大鼠接受了单次豚鼠脊髓皮内接种。还评估了弗氏佐剂和单独脊髓对脑通透性的影响。为了比较溶液通透性和脂质体定位,静脉注射放射性脂质体,1小时后注射99mTc-DTPA。进行闪烁扫描采集以跟踪全身放射性的生物分布。每只大鼠在接种前进行首次检查,然后每两天检查一次,直至实验结束,可将其视为自身对照。EAE导致全身通透性出现此前未报道的增加,可能是由于炎症所致。正常动物与早期EAE(临床症状出现前)动物之间的脂质体脑定位和脑/心比值存在显著差异,且在临床明显的EAE中能区分不同疾病阶段。疾病进展指数比注射99mTc-DTPA更早出现变化。一种解释可能是循环巨噬细胞摄取颗粒,这些巨噬细胞在这种病理过程中穿过血脑屏障。对于临床应用,必须在对人类多发性硬化症更可靠的模型上证实这些实验。

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