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使用介孔硅微粒进行肽类胃饥饿素拮抗剂的体内递送。

In vivo delivery of a peptide, ghrelin antagonist, with mesoporous silicon microparticles.

作者信息

Kilpeläinen M, Riikonen J, Vlasova M A, Huotari A, Lehto V P, Salonen J, Herzig K H, Järvinen K

机构信息

A.I. Virtanen Institute, University of Kuopio, 70211 Kuopio, Finland.

出版信息

J Control Release. 2009 Jul 20;137(2):166-70. doi: 10.1016/j.jconrel.2009.03.017. Epub 2009 Apr 2.

Abstract

Peptides may represent potential treatment options for many severe illnesses. However, they need an effective delivery system to overcome rapid degradation after their administration. One possible way to prolong peptide action is to use particulate drug delivery systems. In the present study, thermally hydrocarbonized mesoporous silicon (THCPSi) microparticles (38-53 microm) were studied as a peptide delivery system in vivo. D-lys-GHRP6 (ghrelin antagonist, GhA) was used as a model peptide. The effects of GhA-loaded THCPSi microparticles on food intake (s.c., GhA dose 14 mg/kg) and on blood pressure (s.c., GhA dose 4 mg/kg) were examined in mice and rats, respectively. In addition, the effects of THCPSi microparticles (2 mg) on cytokine secretion in mice after single s.c. administration were examined by determining several cytokine plasma concentrations. The present results demonstrate that GhA can be loaded into THCPSi microparticles with a high loading degree (20% w/w). GhA loaded THCPSi microparticles inhibited food intake for a prolonged time, and increased blood pressure more slowly than encountered with a GhA solution. Furthermore, THCPSi microparticles did not increase cytokine activity. The present results suggest that THCPSi might be used as a drug delivery system for peptides.

摘要

肽可能是许多严重疾病的潜在治疗选择。然而,它们需要一种有效的递送系统来克服给药后迅速降解的问题。延长肽作用的一种可能方法是使用颗粒药物递送系统。在本研究中,热碳化介孔硅(THCPSi)微粒(38 - 53微米)作为一种肽体内递送系统进行了研究。D - 赖氨酸 - GHRP6(生长激素释放肽拮抗剂,GhA)被用作模型肽。分别在小鼠和大鼠中研究了负载GhA的THCPSi微粒对食物摄入量(皮下注射,GhA剂量14毫克/千克)和血压(皮下注射,GhA剂量4毫克/千克)的影响。此外,通过测定几种细胞因子的血浆浓度,研究了单次皮下注射后THCPSi微粒(2毫克)对小鼠细胞因子分泌的影响。目前的结果表明,GhA可以以高负载度(20% w/w)负载到THCPSi微粒中。负载GhA的THCPSi微粒能长时间抑制食物摄入,且升高血压的速度比GhA溶液慢。此外,THCPSi微粒不会增加细胞因子活性。目前的结果表明,THCPSi可能用作肽的药物递送系统。

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