人类丝虫 Loa loa、涡虫 Onchocerca volvulus 和 Mansonella perstans 在免疫受损小鼠品系中的发育比较

V. C. Chunda, Fanny F. Fombad, Chi A Kien, Rene Ebai, Frederick Esofi, Anna Ning Ntuh, Emmanuel Ouam, N. V. Gandjui, Relindis Ekanya, Franck Nietcho, Lucy Cho Nchang, Chefor Magha, A. Njouendou, P. Enyong, Achim Hoerauf, S. Wanji, M. Ritter
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Methods Therefore, we aim to establish experimental M. perstans infections using the immunocompromised mouse strains RAG2IL-2Rγ−/− (lack B, T and natural killer cells), IL-4Rα/IL-5−/− (impaired IL-4/5 signalling and eosinophil activation) and NOD.Cg-PrkdcscidIl2rgtm1Wj l/SzJ (NOD scid gamma, NSG) BALB/c mice (lack mature lymphocytes) through subcutaneous (s.c.) or intraperitoneal (i.p.) inoculation of infective stage 3 larvae (L3) isolated from engorged vectors. Results In total, 145 immunocompromised mice have been inoculated with 3,250 M. perstans, 3,337 O. volvulus, and 2,720 Loa loa L3 to comparatively analyse which immunocompromised mouse strain is susceptible to human filarial infections. Whereas, no M. perstans and O. volvulus L3 could be recovered upon 2-63 days post-inoculation, a 62-66% Loa loa L3 recovery rate could be achieved in the different mouse strains. 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引用次数: 0

摘要

导言:人类丝虫感染的小鼠模型不仅是研究线虫生物学及其对宿主免疫力调节的迫切需要,而且也将为筛选和测试新型抗丝虫药物提供一个平台。最近,利用免疫功能低下的小鼠品系建立了小鼠 Loa loa 感染模型,而小鼠 Mansonella perstans 感染模型至今尚未建立。因此,我们利用免疫受损的小鼠品系 RAG2IL-2Rγ-/-(缺乏 B、T 和自然杀伤细胞)、IL-4Rα/IL-5-/-(IL-4/5 信号传导和嗜酸性粒细胞活化受损)和 NOD.Cg-Prkdcsc-/- (IL-4/5 信号传导和嗜酸性粒细胞活化受损)来建立实验性 M. perstans 感染模型。Cg-PrkdcscidIl2rgtm1Wj l/SzJ(NOD scid gamma,NSG)BALB/c小鼠(缺乏成熟淋巴细胞)通过皮下注射或腹腔注射从吞食载体中分离出的感染性3期幼虫(L3)。结果 共有145只免疫力低下的小鼠接种了3,250条M. perstans、3,337条O. volvulus和2,720条Loa loa L3,以比较分析哪种免疫力低下的小鼠品系易受人类丝虫感染。不同品系的小鼠在接种后 2-63 天内均无法恢复 M. perstans 和 O. volvulus L3,而 Loa loa L3 的恢复率为 62-66%。小鼠的性别、接种类型(静脉注射或皮下注射)或分析时间点(接种后 2-63 天)都不会影响 L3 的成功恢复。此外,使用免疫抑制剂氢化可的松、泼尼松龙和环磷酰胺也不能恢复 M. perstans L3 的恢复率。讨论 这些研究结果表明,RAG2IL-2Rg-/-BALB/c和C57BL/6、IL-4Rα/IL-5-/-BALB/c和NSG小鼠在使用应用方法时对M. perstans和O. volvulus L3接种不敏感,而Loa loa感染可以维持。进一步的研究应探讨人源化免疫缺陷小鼠是否可能对M. perstans.
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Comparative development of human filariae Loa loa, Onchocerca volvulus and Mansonella perstans in immunocompromised mouse strains
Introduction Mouse models of human filarial infections are not only urgently needed to investigate the biology of the nematodes and their modulation of the host’s immunity, but will also provide a platform to screen and test novel anti-filarial drugs. Recently, murine Loa loa infection models have been stablished using immunocompromised mouse strains, whereas murine Mansonella perstans infections have not been implemented until now. Methods Therefore, we aim to establish experimental M. perstans infections using the immunocompromised mouse strains RAG2IL-2Rγ−/− (lack B, T and natural killer cells), IL-4Rα/IL-5−/− (impaired IL-4/5 signalling and eosinophil activation) and NOD.Cg-PrkdcscidIl2rgtm1Wj l/SzJ (NOD scid gamma, NSG) BALB/c mice (lack mature lymphocytes) through subcutaneous (s.c.) or intraperitoneal (i.p.) inoculation of infective stage 3 larvae (L3) isolated from engorged vectors. Results In total, 145 immunocompromised mice have been inoculated with 3,250 M. perstans, 3,337 O. volvulus, and 2,720 Loa loa L3 to comparatively analyse which immunocompromised mouse strain is susceptible to human filarial infections. Whereas, no M. perstans and O. volvulus L3 could be recovered upon 2-63 days post-inoculation, a 62-66% Loa loa L3 recovery rate could be achieved in the different mouse strains. Gender of mice, type of inoculation (s.c. or i.p.) or time point of analysis (2-63 days post inoculation) did not interfere with the success of L3 recovery. In addition, administration of the immune suppressants hydrocortisone, prednisolone and cyclophosphamide did not restore M. perstans L3 recovery rates. Discussion These findings show that RAG2IL-2Rg−/−BALB/c and C57BL/6, IL-4Rα/IL-5−/− BALB/c and NSG mice were not susceptible to M. perstans and O. volvulus L3 inoculation using the applied methods, whereas Loa loa infection could be maintained. Further studies should investigate if humanized immunocompromised mice might be susceptible to M. perstans. and O. volvulus.
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