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免疫组织化学研究罗 13-3978、吡喹酮、奥沙米酮和甲氟喹治疗感染曼氏血吸虫小鼠的效果。

Immunohistochemical Investigations of Treatment with Ro 13-3978, Praziquantel, Oxamniquine, and Mefloquine in Schistosoma mansoni-Infected Mice.

机构信息

Swiss Tropical and Public Health Institute, Basel, Switzerland, and University of Basel, Basel Switzerland.

Swiss Tropical and Public Health Institute, Basel, Switzerland, and University of Basel, Basel Switzerland

出版信息

Antimicrob Agents Chemother. 2017 Nov 22;61(12). doi: 10.1128/AAC.01142-17. Print 2017 Dec.

Abstract

To date, there is only one drug in use, praziquantel, to treat more than 250 million people afflicted with schistosomiasis, a debilitating parasitic disease. The aryl hydantoin Ro 13-3978 is a promising drug candidate with activity superior to that of praziquantel against both adult and juvenile organisms. Given the drug's contrasting low activity and the timing of its onset of action , it was postulated that immune-assisted parasite clearance could contribute to the drug's activity. We undertook histopathological studies to investigate this hypothesis. Infected mice were treated with an effective dose of Ro 13-3978 (100 mg/kg of body weight) and were dissected before and after the drug's onset of action. The veins and livers were excised, paraffin-embedded, and sectioned, and macrophages (IBA-1), neutrophils (Neutro), B cells (CD45R), and T cells (CD3) were stained by immunohistochemistry. For comparison, samples from infected untreated mice and mice treated with effective doses of praziquantel (400 mg/kg), oxamniquine (200 mg/kg), and mefloquine (200 mg/kg) were examined. At 24 h after treatment with Ro 13-3978, significant macrophage recruitment to the veins was observed, along with a modest increase in circulating B cells, and at 48 h, neutrophils and T cells are also present. Treatment with praziquantel and oxamniquine showed similar patterns of recruitment but with comparatively higher cellular levels, whereas mefloquine treatment resulted in minimal cell recruitment until 3 days posttreatment. Our study sheds light on the immediate immune responses to antischistosomal treatment in mice and provides further insight into immune effector mechanisms of schistosome clearance.

摘要

迄今为止,仅有一种药物——吡喹酮被用于治疗超过 2.5 亿名感染血吸虫病的患者,这是一种使人虚弱的寄生虫病。芳基海因 Ro 13-3978 是一种很有前途的候选药物,其活性优于吡喹酮,对成虫和幼虫均有效。鉴于该药物的活性对比低,且作用开始时间晚,人们推测免疫辅助寄生虫清除可能有助于该药物的活性。我们进行了组织病理学研究来验证这一假说。将感染的小鼠用有效剂量的 Ro 13-3978(100mg/kg 体重)治疗,并在药物作用开始前后进行解剖。取出静脉和肝脏,石蜡包埋,切片,用免疫组织化学法对巨噬细胞(IBA-1)、中性粒细胞(Neutro)、B 细胞(CD45R)和 T 细胞(CD3)进行染色。为了进行比较,还检查了未经处理的感染小鼠、用有效剂量吡喹酮(400mg/kg)、奥沙米酮(200mg/kg)和甲氟喹(200mg/kg)治疗的小鼠的样本。在用 Ro 13-3978 治疗 24 小时后,观察到巨噬细胞向静脉大量募集,同时循环 B 细胞略有增加,48 小时后,中性粒细胞和 T 细胞也存在。用吡喹酮和奥沙米酮治疗显示出类似的募集模式,但细胞水平相对较高,而用甲氟喹治疗直到治疗后 3 天,细胞募集才很少。我们的研究阐明了小鼠抗血吸虫治疗的即时免疫反应,并进一步深入了解了血吸虫清除的免疫效应机制。

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