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开发一种治疗非洲锥虫病的地美硝唑纳米制剂。

Development of a nanoparticulate formulation of diminazene to treat African trypanosomiasis.

机构信息

EA 4483, IFR 114 IMPRT, Faculté de Médecine, Pôle recherche, Département de Physiologie, 1 place de Verdun, 59045 Lille Cedex, France.

出版信息

Nanotechnology. 2010 Dec 17;21(50):505102. doi: 10.1088/0957-4484/21/50/505102. Epub 2010 Nov 22.

Abstract

There is a real need to develop new therapeutic strategies for African trypanosomiasis infections. In our study, we developed a new drug delivery system of diminazene (DMZ), a trypanocidal drug registered for veterinary use. This drug candidate presents a limited efficacy, a poor affinity for brain tissue and instability. The development of colloidal formulations based on a porous cationic nanoparticle with an oily core ((70)DGNP(+)), has potentially two advantages: stabilization of the drug and potential targeting of the parasite. We analyzed two processes of drug loading: in process (DMZ was added during the preparation of (70)DGNP(+) at 80 °C) and post-loading (DMZ was mixed with a (70)DGNP(+) solution at room temperature). Poor stability of the drug was observed using the in process technique. When using the post-loading technique over 80% drug entrapment efficiency was obtained at a ratio of DMZ:phospholipids (wt:wt) < 5%. Moreover, DMZ loaded into (70)DGNP(+) was found to be protected against oxidation and was stable for at least six months at 4 °C. Finally, in vitro tests on T.b. brucei showed an increased efficacy of DMZ loaded in (70)DGNP(+).

摘要

开发新的抗非洲锥虫病感染的治疗策略确实很有必要。在我们的研究中,我们开发了一种新的二脒那嗪(DMZ)药物传递系统,DMZ 是一种已注册用于兽医的杀锥虫药物。该候选药物疗效有限,对脑组织亲和力低,且不稳定。基于具有油芯的多孔阳离子纳米颗粒((70)DGNP(+))开发胶体制剂具有潜在的两个优势:稳定药物和潜在靶向寄生虫。我们分析了两种载药过程:过程中载药(在 80°C 时制备(70)DGNP(+)时加入 DMZ)和后载药(在室温下将 DMZ 与(70)DGNP(+)溶液混合)。使用过程中载药技术时,观察到药物稳定性差。当使用后载药技术时,在 DMZ:磷脂(wt:wt)<5%的比例下,获得了超过 80%的药物包封效率。此外,负载到(70)DGNP(+)中的 DMZ 被发现能够防止氧化,并且在 4°C 下至少稳定六个月。最后,对 T.b. brucei 的体外试验表明,负载到(70)DGNP(+)中的 DMZ 具有更高的疗效。

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