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In vitro and in vivo efficacy of drugs against the protozoan parasite Azumiobodo hoyamushi that causes soft tunic syndrome in the edible ascidian Halocynthia roretzi (Drasche)
Authors:K H Park  S‐R Zeon  J‐G Lee  S‐H Choi  Y K Shin  K‐I Park
Institution:1. Department of Aquatic Life Medicine, Kunsan National University, , Gunsan City, Jeonbuk, Korea;2. Aquaculture Management Division, NFRDI, , Busan, Korea
Abstract:It was discovered recently that infection by a protozoan parasite, Azumiobodo hoyamushi, is the most probable cause for soft tunic syndrome in an edible ascidian, Halocynthia roretzi (Drasche). In an attempt to develop measures to eradicate the causative parasite, various drugs were tested for efficacy in vitro and in vivo. Of the 20 antiprotozoal drugs having different action mechanisms, five were found potent (24‐h EC50 < 10 mg L?1) in their parasite‐killing effects: formalin, H2O2, bithionol, ClO2 and bronopol. Moderately potent drugs (10 < 24‐h EC50 < 100 mg L?1) were quinine, fumagillin, amphotericin B, ketoconazole, povidone‐iodine, chloramine‐T and benzalkonium chloride. Seven compounds, metronidazole, albendazole, paromomycin, nalidixic acid, sulfamonomethoxine, KMnO4, potassium monopersulphate and citric acid, exhibited EC50 > 100 mg L?1. When ascidians were artificially infected with A. hoyamushi, treated using 40 mg L?1 formalin, bronopol, ClO2, or H2O2 for 1 h and then monitored for 24 h, very low mortality was observed. However, the number of surviving parasite cells in the ascidian tunic tissues was significantly reduced by treating with 40 mg L?1 formalin or ClO2 for 1 h. The data suggest that we might be able to develop a disinfection measure using a treatment regimen involving commonly available drugs.
Keywords:antiprotozoal drugs  ascidians     Azumiobodo hoyamushi     in vitro and vivo efficacy  soft tunic syndrome
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