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通过直肠给予十一肽-hEGF 到小鼠脑内改善 Aβ 22-35 诱导的痴呆。

Amelioration of dementia induced by Aβ 22-35 through rectal delivery of undecapeptide-hEGF to mouse brain.

机构信息

Institute of Pharmacology and Toxicology, Academy of Military, Medical Sciences, Beijing 100850, China.

出版信息

Int J Pharm. 2011 Feb 28;405(1-2):1-8. doi: 10.1016/j.ijpharm.2010.11.018. Epub 2010 Nov 18.

DOI:10.1016/j.ijpharm.2010.11.018
PMID:21093564
Abstract

A group of growth factors have been shown to play important roles in amelioration of the malfunction of the neurodegenerative diseases. However, the proteins or polypeptides passing across the blood-brain barrier (BBB) to access the brain parenchyma are relatively few so that it hinders the therapies in clinic. Here a genetically reconstructed fusion peptide of human epidermal growth factor (hEGF) with an undecapeptide YGRKKRRQRRR (P11) was used to investigate the permeability between the cell membrane and the BBB via rectal administration. The efficiency to rescue the Aβ 22-35-induced dementia in mice was assessed after administration of P11-hEGF per rectal. Our results showed that P11-hEGF permeates across not only the 3T3 cell membrane in vitro, but also the endothelia of vessels after intravenous injection (IV), and the mucosa of the rectum after per rectal administration. Further results showed that the circulating P11-hEGF allowed penetrating through the blood-brain barrier and then getting into the brain manifesting biological responses. In the animal experiments, treatment with P11-hEGF not only ameliorated the dementia induced by Aβ 22-35 but also rescued the dementia of the aged mice, no matter how it was administrated (IV or per rectal). These results suggest that the rectal non-invasive delivery of the P11 polypeptide-conjugated growth factor is an efficient way for BBB transduction, thus raises the hope of real therapeutic progress against neurodegenerative diseases.

摘要

一组生长因子已被证明在改善神经退行性疾病的功能障碍方面发挥着重要作用。然而,能够穿过血脑屏障(BBB)进入脑实质的蛋白质或多肽相对较少,这阻碍了临床治疗。本文利用人表皮生长因子(hEGF)与人源十一肽 YGRKKRRQRRR(P11)的基因重组融合肽,通过直肠给药研究其穿过细胞膜和 BBB 的通透性。在经直肠给予 P11-hEGF 后,评估其对 Aβ22-35 诱导的痴呆小鼠的治疗效果。结果显示,P11-hEGF 不仅可以穿过体外 3T3 细胞膜,还可以穿过静脉注射(IV)后的血管内皮和直肠给药后的直肠黏膜。进一步的结果显示,循环中的 P11-hEGF 可以穿透血脑屏障进入大脑并发挥生物学反应。在动物实验中,P11-hEGF 的治疗不仅改善了 Aβ22-35 诱导的痴呆,还挽救了老年痴呆小鼠的痴呆,无论其是通过 IV 还是直肠给药。这些结果表明,P11 多肽偶联生长因子的直肠非侵入性给药是一种有效的 BBB 转导方法,为神经退行性疾病的治疗带来了新的希望。

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