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纳米技术在克氏锥虫病防治中的应用。

Nanotechnological approaches against Chagas disease.

机构信息

Programa de Nanomedicinas, Universidad Nacional de Quilmes, Bernal, Buenos Aires, Argentina.

出版信息

Adv Drug Deliv Rev. 2010 Mar 18;62(4-5):576-88. doi: 10.1016/j.addr.2009.11.025. Epub 2009 Nov 23.

DOI:10.1016/j.addr.2009.11.025
PMID:19941920
Abstract

Over several thousand years, the flagellated Trypanosome cruzi-causative agent of Chagas disease-developed a complex life cycle between the reduviidae vectors and its human hosts. Due to their silent and hidden location, the intracellular amastigotes are mainly responsible for the nearly 50,000 annual deaths caused by the chronic chagasic cardiomyopathy. Chagas disease is the most important parasitic disease in the Americas, though treatments have not evolved towards a more efficient pharmacotherapy that (i) eradicates the scarce amastigotes present at the indeterminate/chronic form and (ii) employs less toxic drugs than benznidazole or nifurtimox. Nano-drug delivery systems (nanoDDS) represent useful means to selectively deliver the drug to intracellular targets. However, preclinical research in Chagas must be extended in order to improve the chances of a clinical implementation. The stages involved in this process are (i) selection of the appropriate drug for a specific parasite, (ii) development of a drug-loaded nanoDDS structure that displays the adequate pharmacokinetics, biodistribution and intracellular transit and (iii) selection of the right parasite form to target and the right stage of the disease for the treatment to be started. In this review we will critically overview the few research works published in the last 20years in the context of nanotechnology and Chagas diseases and highlight the gaps in knowledge towards the design of more efficient medicines to address this endemic.

摘要

在几千年的时间里,引起恰加斯病的鞭毛原生动物克氏锥虫在吸血蝽媒介和人类宿主之间发展出了一种复杂的生命周期。由于其潜伏和隐匿的位置,细胞内的无鞭毛体主要负责每年近 50,000 例由慢性恰加斯心肌病引起的死亡。尽管治疗方法并未朝着更有效的药物治疗方向发展(i)消除无症状/慢性期罕见的无鞭毛体,(ii)使用比苯硝唑或硝呋替莫毒性更小的药物,但恰加斯病仍是美洲最重要的寄生虫病。纳米药物递送系统(nanoDDS)代表了向细胞内靶点选择性递送药物的有用手段。然而,为了提高临床实施的机会,必须扩展恰加斯病的临床前研究。这个过程涉及(i)为特定寄生虫选择合适的药物,(ii)开发具有适当药代动力学、生物分布和细胞内转运的载药 nanoDDS 结构,以及(iii)选择合适的寄生虫形式作为靶标和治疗开始的疾病阶段。在这篇综述中,我们将批判性地回顾过去 20 年在纳米技术和恰加斯病背景下发表的少数研究工作,并强调在设计更有效的药物以解决这种地方病方面存在的知识差距。

相似文献

1
Nanotechnological approaches against Chagas disease.纳米技术在克氏锥虫病防治中的应用。
Adv Drug Deliv Rev. 2010 Mar 18;62(4-5):576-88. doi: 10.1016/j.addr.2009.11.025. Epub 2009 Nov 23.
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Side effects of benznidazole as treatment in chronic Chagas disease: fears and realities.苄硝唑作为慢性恰加斯病治疗药物的副作用:恐惧与现实
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[Treatment of Chagas disease].[恰加斯病的治疗]
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Potential new clinical therapies for Chagas disease.治疗恰加斯病的新临床疗法。
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Nanomedicines against Chagas disease: an update on therapeutics, prophylaxis and diagnosis.抗恰加斯病的纳米药物:治疗、预防和诊断的最新进展
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[Treatment of Trypanosoma cruzi infection in the indeterminate phase: experience and current guidelines in Argentina].[恰加斯病不确定期克氏锥虫感染的治疗:阿根廷的经验与现行指南]
Medicina (B Aires). 1999;59 Suppl 2:166-70.

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