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无鞭毛体利什曼原虫作为体外研究合适模型。

Axenic amastigotes of Leishmania species as a suitable model for in vitro studies.

机构信息

Fundação Oswaldo Cruz, Instituto Oswaldo Cruz, Laboratório de Biologia Molecular e Doenças Endêmicas, Rio de Janeiro, RJ, Brazil.

Fundação Oswaldo Cruz, Centro de Desenvolvimento Tecnológico em Saúde, Rio de Janeiro, RJ, Brazil; Universidade Iguaçu, Faculdade de Ciências Biológicas e da Saúde, Rio de Janeiro, RJ, Brazil.

出版信息

Acta Trop. 2021 Aug;220:105956. doi: 10.1016/j.actatropica.2021.105956. Epub 2021 May 9.

Abstract

Leishmania spp. are etiological agents of infection diseases, which in some cases can be fatal. The main forms of their biological cycle, promastigotes and amastigotes, can be maintained in vitro. While promastigotes are easier to maintain, amastigotes are more complex and can be obtained through different ways, including infection assays of tissues or in vitro cells, and differentiation from promastigotes to axenic amastigotes. Several protocols have been proposed for in vitro differentiation for at least 12 Leishmania spp. of both subgenera, Leishmania and Viannia. In this review we propose a critical summary of axenic amastigotes induction, as well as the impact of these strategies on metabolic pathways and regulatory networks analyzed by omics approaches. The parameters used by different research groups show considerable variations in temperature, pH and induction stages, as highlighted here for Leishmania (Viannia) braziliensis. Therefore, a consensus on strategies for inducing amastigogenesis is necessary to improve accuracy and even define stage-specific biomarkers. In fact, the axenic amastigote model has contributed to elucidate several aspects of the parasite cycle, however, since it does not reproduce the intracellular environment, its use requires several precautions. In addition, we present a discussion about using axenic amastigotes for drug screening, suggesting the need of a more sensitive methodology to verify cell viability in these tests. Collectively, this review explores the advantages and limitations found in studies with axenic amastigotes, done for more than 30 years, and discuss the gaps that impair their use as a suitable model for in vitro studies.

摘要

利什曼原虫属是感染性疾病的病原体,在某些情况下可能是致命的。其生物周期的主要形式,即前鞭毛体和无鞭毛体,可以在体外维持。虽然前鞭毛体更容易维持,但无鞭毛体更为复杂,可以通过不同的方法获得,包括组织或体外细胞的感染测定,以及从前鞭毛体到无鞭毛体的分化。已经提出了至少 12 种利什曼原虫属(Leishmania 和 Viannia)亚种的体外分化的方案。在这篇综述中,我们提出了对无鞭毛体诱导的批判性总结,以及这些策略对通过组学方法分析的代谢途径和调控网络的影响。不同研究小组使用的参数在温度、pH 和诱导阶段上有很大的差异,这里以利什曼(Viannia)巴西利ensis 为例进行了强调。因此,有必要就诱导无鞭毛体形成的策略达成共识,以提高准确性,甚至定义阶段特异性生物标志物。事实上,无鞭毛体模型有助于阐明寄生虫周期的几个方面,然而,由于它不能复制细胞内环境,因此其使用需要一些预防措施。此外,我们还对使用无鞭毛体进行药物筛选进行了讨论,建议需要一种更灵敏的方法来验证这些测试中的细胞活力。总的来说,这篇综述探讨了 30 多年来无鞭毛体研究中发现的优势和局限性,并讨论了影响其作为体外研究合适模型的使用的差距。

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