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恩诺沙星和托曲珠利能够抑制人妊娠晚期BeWo滋养层细胞和绒毛外植体的生长。

Enrofloxacin and Toltrazuril Are Able to Reduce Growth in Human BeWo Trophoblastic Cells and Villous Explants from Human Third Trimester Pregnancy.

作者信息

da Silva Rafaela J, Gomes Angelica O, Franco Priscila S, Pereira Ariane S, Milian Iliana C B, Ribeiro Mayara, Fiorenzani Paolo, Dos Santos Maria C, Mineo José R, da Silva Neide M, Ferro Eloisa A V, de Freitas Barbosa Bellisa

机构信息

Laboratory of Immunophysiology of Reproduction, Institute of Biomedical Science, Federal University of UberlândiaUberlândia, Brazil.

Departament of Morphology, Federal University of Triângulo MineiroUberaba, Brazil.

出版信息

Front Cell Infect Microbiol. 2017 Jul 26;7:340. doi: 10.3389/fcimb.2017.00340. eCollection 2017.

Abstract

Classical treatment for congenital toxoplasmosis is based on combination of sulfadiazine and pyrimethamine plus folinic acid. Due to teratogenic effects and bone marrow suppression caused by pyrimethamine, the establishment of new therapeutic strategies is indispensable to minimize the side effects and improve the control of infection. Previous studies demonstrated that enrofloxacin and toltrazuril reduced the incidence of and infection. The aim of the present study was to evaluate the efficacy of enrofloxacin and toltrazuril in the control of infection in human trophoblast cells (BeWo line) and in human villous explants from the third trimester. BeWo cells and villous were treated with several concentrations of enrofloxacin, toltrazuril, sulfadiazine, pyrimethamine, or combination of sulfadiazine+pyrimethamine, and the cellular or tissue viability was verified. Next, BeWo cells were infected by (2F1 clone or the ME49 strain), whereas villous samples were only infected by the 2F1 clone. Then, infected cells and villous were treated with all antibiotics and the intracellular proliferation as well as the cytokine production were analyzed. Finally, we evaluated the direct effect of enrofloxacin and toltrazuril in tachyzoites to verify possible changes in parasite structure. Enrofloxacin and toltrazuril did not decrease the viability of cells and villous in lower concentrations. Both drugs were able to significantly reduce the parasite intracellular proliferation in BeWo cells and villous explants when compared to untreated conditions. Regardless of the strain, BeWo cells infected and treated with enrofloxacin or toltrazuril induced high levels of IL-6 and MIF. In villous explants, enrofloxacin induced high MIF production. Finally, the drugs increased the number of unviable parasites and triggered damage to tachyzoite structure. Taken together, it can be concluded that enrofloxacin and toltrazuril are able to control infection in BeWo cells and villous explants, probably by a direct action on the host cells and parasites, which leads to modifications of cytokine release and tachyzoite structure.

摘要

先天性弓形虫病的传统治疗方法是基于磺胺嘧啶和乙胺嘧啶加亚叶酸的联合使用。由于乙胺嘧啶会产生致畸作用并抑制骨髓,因此建立新的治疗策略对于将副作用降至最低并改善感染控制至关重要。先前的研究表明,恩诺沙星和托曲珠利可降低[此处原文缺失相关感染信息]感染的发生率。本研究的目的是评估恩诺沙星和托曲珠利在控制人滋养层细胞(BeWo系)和孕晚期人绒毛外植体中[此处原文缺失相关感染信息]感染方面的疗效。用几种浓度的恩诺沙星、托曲珠利、磺胺嘧啶、乙胺嘧啶或磺胺嘧啶 + 乙胺嘧啶组合处理BeWo细胞和绒毛,并验证细胞或组织活力。接下来,用[此处原文缺失相关感染信息](2F1克隆株或ME49株)感染BeWo细胞,而绒毛样本仅用2F1克隆株感染。然后,用所有抗生素处理感染的细胞和绒毛,并分析[此处原文缺失相关感染信息]细胞内增殖以及细胞因子产生情况。最后,我们评估了恩诺沙星和托曲珠利对速殖子的直接作用,以验证寄生虫结构可能发生的变化。低浓度的恩诺沙星和托曲珠利不会降低细胞和绒毛的活力。与未处理的情况相比,这两种药物均能显著降低BeWo细胞和绒毛外植体中寄生虫的细胞内增殖。无论[此处原文缺失相关感染信息]菌株如何,用恩诺沙星或托曲珠利感染并处理的BeWo细胞都会诱导高水平的IL - 6和MIF。在绒毛外植体中,恩诺沙星诱导产生高水平的MIF。最后,这些药物增加了无活力寄生虫的数量,并引发速殖子结构的损伤。综上所述,可以得出结论,恩诺沙星和托曲珠利能够控制BeWo细胞和绒毛外植体中的[此处原文缺失相关感染信息]感染,可能是通过对宿主细胞和寄生虫的直接作用,从而导致细胞因子释放和速殖子结构的改变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1101/5526852/8f192ee25505/fcimb-07-00340-g0001.jpg

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