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用于抗利什曼病疫苗的微/纳米颗粒佐剂:现状和未来趋势。

Micro/nanoparticle adjuvants for antileishmanial vaccines: present and future trends.

机构信息

Nanotechnology Research Center, School of Pharmacy, Mashhad University of Medical Sciences, Mashhad, Iran.

出版信息

Vaccine. 2013 Jan 21;31(5):735-49. doi: 10.1016/j.vaccine.2012.11.068. Epub 2012 Dec 7.

Abstract

Leishmania infection continues to have a major impact on public health inducing significant morbidity and mortality mostly in the poorest populations. Drug resistance, toxicity and side effects associated with expensive chemotherapeutic treatments and difficult reservoir control emphasize the need for a safe and effective vaccine which is not available yet. Although, Leishmanization (LZ) was shown to be effective against cutaneous leishmaniasis, standardization and safety are the main problems of LZ. First generation killed parasites demonstrated limited efficacy in phase 3 trials and moreover well defined molecules have not reached to phase 3 yet. Limited efficacy in vaccines against leishmaniasis is partly due to lack of an appropriate adjuvant. Hence, the use of particulate delivery systems as carriers for antigen and/or immunostimulatory adjuvants for effective delivery to the antigen-presenting cells (APCs) is a valuable strategy to enhance vaccine efficacies. Particle-based delivery systems such as emulsions, liposomes, virosomes, and polymeric microspheres have the potential for successfully delivering antigens, which can then be further improved via incorporation of additional antigenic or immustimulatory adjuvant components in or onto the particle carrier system. In this review, we have attempted to provide a list of particulate vaccine delivery systems involved in the production of candidate leishmaniasis vaccines and introduced some potentially useful vaccine delivery systems for leishmaniasis in future experiments. In conclusion, combination vaccines (adjuvant systems) composed of candidate antigens and more importantly well-developed particulate delivery systems, such as lipid-based particles containing immunostimulatory adjuvants, have a chance to succeed as antileishmanial vaccines.

摘要

利什曼原虫感染继续对公共卫生造成重大影响,主要在最贫困人群中导致发病率和死亡率显著增加。与昂贵的化疗药物治疗相关的耐药性、毒性和副作用以及难以控制的储存库,强调了需要一种安全有效的疫苗,但目前还没有。尽管利什曼化(LZ)已被证明对皮肤利什曼病有效,但标准化和安全性是 LZ 的主要问题。第一代杀死寄生虫的疗效在 3 期试验中有限,而且尚未达到 3 期的明确分子。针对利什曼病的疫苗疗效有限,部分原因是缺乏适当的佐剂。因此,使用颗粒递送系统作为载体将抗原和/或免疫刺激性佐剂有效递送至抗原呈递细胞(APC)是增强疫苗效力的一种有价值的策略。基于颗粒的递送系统,如乳液、脂质体、病毒体和聚合物微球,具有成功递送抗原的潜力,通过将额外的抗原或免疫刺激性佐剂成分掺入或结合到颗粒载体系统中,可以进一步提高其效果。在这篇综述中,我们试图提供参与生产候选利什曼病疫苗的颗粒疫苗递送系统的列表,并介绍了一些未来实验中可能有用的利什曼病疫苗递送系统。总之,由候选抗原和更重要的经过充分开发的颗粒递送系统(如含有免疫刺激性佐剂的脂质基颗粒)组成的联合疫苗(佐剂系统)有机会成功作为抗利什曼病疫苗。

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