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由于连续传代导致的恰加斯利什曼原虫前鞭毛体发育阶段的种群变化。

Population changes in Leishmania chagasi promastigote developmental stages due to serial passage.

作者信息

Lei Soi Meng, Romine Nathan M, Beetham Jeffrey K

机构信息

Department of Veterinary Pathology, Iowa State University, Ames, Iowa 50011, USA.

出版信息

J Parasitol. 2010 Dec;96(6):1134-8. doi: 10.1645/GE-2566.1. Epub 2010 Aug 13.

Abstract

Leishmania chagasi causes visceral leishmaniasis, a potentially fatal disease of humans. Within the sand fly vector, L. chagasi replicates as promastigotes which undergo complex changes in morphology as they progress from early stage procyclic promastigotes, to intermediate stage leptomonad and nectomonad promastigotes, and ultimately to terminal stage metacyclic promastigotes that are highly infective to vertebrates. This developmental progression is largely recapitulated in vitro using axenic promastigote cultures that have been passaged only a few times. Within a single passage (which takes about a week), axenic cultures progress from logarithmic to stationary growth phases; parasites within those growth phases progress from stages that do not have metacyclic cell properties to ones that do. Interestingly, repeated serial passage of promastigote cultures will result in cell populations that exhibit perturbations in developmental progression, in expression levels of surface macromolecules (major surface protease, MSP, and promastigote surface antigen, PSA), and in virulence properties, including resistance to serum lysis. Experiments were performed to determine whether there exists a direct relationship between promastigote developmental form and perturbations associated with repeated serial passage. Passage 2 to passage 4 L. chagasi cultures at stationary growth phase were predominately (>85%) comprised of metacyclic promastigotes and exhibited high resistance to serum lysis and high levels of MSP and PSA. Serial passaging 8, or more, times resulted in a stationary phase population that was largely (>85%) comprised of nectomonad promastigotes, almost completely devoid (<2%) of metacyclic promastigotes, and that exhibited low resistance to serum lysis and low levels of MSP and PSA. The study suggests that the loss of particular cell properties seen in cells from serially passaged cultures is principally due to a dramatic reduction in the proportion of metacyclic promastigotes. Additionally, the study suggests that serially passaged cultures may be a highly enriched source of nectomonad-stage promastigotes, a stage that has largely been characterized only in mixtures containing other promastigote forms.

摘要

恰加斯利什曼原虫可引发内脏利什曼病,这是一种对人类有潜在致命性的疾病。在白蛉传播媒介体内,恰加斯利什曼原虫以前鞭毛体形式进行繁殖,从前鞭毛体早期的前循环型,发展到中期的细滴虫型和游动滴虫型前鞭毛体,最终成为对脊椎动物具有高度感染性的终末型后循环型前鞭毛体,其形态会发生复杂变化。这种发育进程在很大程度上可在体外通过仅传代几次的无菌前鞭毛体培养物得以重现。在单次传代(约需一周时间)内,无菌培养物从对数生长期进入稳定生长期;处于这些生长阶段的寄生虫从没有后循环细胞特性的阶段发展到具有该特性的阶段。有趣的是,前鞭毛体培养物的反复连续传代将导致细胞群体在发育进程、表面大分子(主要表面蛋白酶、MSP和前鞭毛体表面抗原、PSA)的表达水平以及毒力特性(包括对血清溶解的抗性)方面出现扰动。进行了实验以确定前鞭毛体发育形式与反复连续传代相关的扰动之间是否存在直接关系。处于稳定生长期的第2代至第4代恰加斯利什曼原虫培养物主要(>85%)由后循环型前鞭毛体组成,对血清溶解具有高抗性,且MSP和PSA水平较高。连续传代8次或更多次会导致稳定期群体主要(>85%)由游动滴虫型前鞭毛体组成,几乎完全没有(<2%)后循环型前鞭毛体,且对血清溶解的抗性较低,MSP和PSA水平也较低。该研究表明,在连续传代培养的细胞中观察到的特定细胞特性丧失主要是由于后循环型前鞭毛体比例的大幅降低。此外,该研究表明连续传代培养物可能是游动滴虫阶段前鞭毛体的高度富集来源,该阶段在很大程度上仅在含有其他前鞭毛体形式的混合物中得到表征。

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