Effect of Phlebotomus papatasi on the fitness, infectivity and antimony-resistance phenotype of antimony-resistant Leishmania major Mon-25

IF 4.1 2区医学 Q1 PARASITOLOGY International Journal for Parasitology: Drugs and Drug Resistance Pub Date : 2024-06-24 DOI:10.1016/j.ijpddr.2024.100554

Nalia Mekarnia , Kamal-Eddine Benallal , Jovana Sádlová , Barbora Vojtková , Aurélie Mauras , Nicolas Imbert , Maryline Longhitano , Zoubir Harrat , Petr Volf , Philippe M. Loiseau , Sandrine Cojean

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Abstract

Leishmania major is responsible for zoonotic cutaneous leishmaniasis. Therapy is mainly based on the use of antimony-based drugs; however, treatment failures and illness relapses were reported. Although studies were developed to understand mechanisms of drug resistance, the interactions of resistant parasites with their reservoir hosts and vectors remain poorly understood. Here we compared the development of two L. major MON-25 trivalent antimony-resistant lines, selected by a stepwise in vitro Sb(III)-drug pressure, to their wild-type parent line in the natural vector Phlebotomus papatasi. The intensity of infection, parasite location and morphological forms were compared by microscopy. Parasite growth curves and IC₅₀ values have been determined before and after the passage in Ph. papatasi. qPCR was used to assess the amplification rates of some antimony-resistance gene markers. In the digestive tract of sand flies, Sb(III)-resistant lines developed similar infection rates as the wild-type lines during the early-stage infections, but significant differences were observed during the late-stage of the infections. Thus, on day 7 p. i., resistant lines showed lower representation of heavy infections with colonization of the stomodeal valve and lower percentage of metacyclic promastigote forms in comparison to wild-type strains. Observed differences between both resistant lines suggest that the level of Sb(III)-resistance negatively correlates with the quality of the development in the vector. Nevertheless, both resistant lines developed mature infections with the presence of infective metacyclic forms in almost half of infected sandflies. The passage of parasites through the sand fly guts does not significantly influence their capacity to multiply in vitro. The IC₅₀ values and molecular analysis of antimony-resistance genes showed that the resistant phenotype of Sb(III)-resistant parasites is maintained after passage through the sand fly. Sb(III)-resistant lines of L. major MON-25 were able to produce mature infections in Ph. papatasi suggesting a possible circulation in the field using this vector.

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Phlebotomus papatasi 对抗锑利什曼原虫 Mon-25 的适应性、感染性和抗锑表型的影响。

大利什曼原虫是人畜共患皮肤利什曼病的罪魁祸首。治疗主要以使用锑基药物为主，但也有治疗失败和疾病复发的报道。虽然研究人员已经了解了抗药性的机制，但对抗药性寄生虫与其贮存宿主和载体之间的相互作用仍然知之甚少。在这里，我们比较了通过逐步体外Sb（III）-药物压力筛选出的两个L. major MON-25三价抗锑品系与其野生型亲本品系在自然载体Phlebotomus papatasi中的发展情况。通过显微镜比较了感染强度、寄生虫位置和形态。利用 qPCR 评估了一些抗锑基因标记的扩增率。在沙蝇的消化道中，Sb(III)抗性品系在感染初期的感染率与野生型品系相似，但在感染后期则出现了显著差异。因此，与野生型品系相比，抗性品系在第 7 天时表现出较低的重度感染率，并在气孔瓣膜上形成定殖，而中生原虫的比例也较低。两个抗性品系之间的差异表明，Sb(III)抗性水平与载体的发育质量呈负相关。尽管如此，两个抗性品系都发展出了成熟的感染，几乎一半的受感染沙蝇都出现了有感染力的元簇。寄生虫通过沙蝇内脏并不会对其体外繁殖能力产生重大影响。IC50 值和抗锑基因的分子分析表明，耐 Sb(III)寄生虫的抗锑表型在通过沙蝇后仍能保持。对 Sb(III)有抗性的 L. major MON-25 株系能够在 Ph. papatasi 中产生成熟的感染，这表明该病媒可能在田间流通。

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来源期刊

International Journal for Parasitology: Drugs and Drug Resistance PARASITOLOGY-PHARMACOLOGY & PHARMACY

CiteScore

7.90

自引率

7.50%

发文量

审稿时长

48 days

期刊介绍： The International Journal for Parasitology – Drugs and Drug Resistance is one of a series of specialist, open access journals launched by the International Journal for Parasitology. It publishes the results of original research in the area of anti-parasite drug identification, development and evaluation, and parasite drug resistance. The journal also covers research into natural products as anti-parasitic agents, and bioactive parasite products. Studies can be aimed at unicellular or multicellular parasites of human or veterinary importance.