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Oxadiazole-2-oxides may have other functional targets,in addition to SjTGR,through which they cause mortality in Schistosoma japonicum
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نویسنده
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song l.-j. ,luo h. ,fan w.-h. ,wang g.-p. ,yin x.-r. ,shen s. ,wang j. ,jin y. ,zhang w. ,gao h. ,liu q. ,wang w.-l. ,feng b. ,yu c.-x.
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منبع
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parasites and vectors - 2016 - دوره : 9 - شماره : 1
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چکیده
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Background: schistosomiasis is one of the world's major public health problems. besides praziquantel (pzq),there is currently no other effective treatment against schistosomiasis. the development of new antischistosomal agents to curb the emergence of pzq resistance should be a high priority. oxadiazole-2-oxides have been identified as potential antischistosomal reagents,with thioredoxin glutathione reductase (tgr) being one of their molecular targets. methods: to develop novel treatment reagents against schistosoma japonicum,30 novel oxadiazole-2-oxides were synthesised and their antischistosomal activities on juvenile and adult s. japonicum were evaluated in vitro and in vivo. their inhibitory activities against s. japonicum thioredoxin glutathione reductase (sjtgr) were also analysed. results: most of the oxadiazole-2-oxides showed good juvenile and adult s. japonica killing activities in vitro. however,the antischistosomal effects of these compounds were not positively correlated with either their inhibition of sjtgr,or with nitric oxide (no) release. compounds 4a,4b,7c,13,16 and 20 resulted in 87.7 %,83.1 %,87.1 %,84.6 %,90.8 % and 69.5 %,respectively,mortality in the adult worms,when used to treat infected mice at schistosomula stage. these mortality rates were similar to or higher than that of artemisinin. furthermore,compounds 4a and 16 resulted in 66.7 % and 69.4 % reductions in the worm burdens,respectively,when infected mice were treated at the adult worm stage. these treatment effects were similar to pzq. no differences in activity of the oxadiazole-2-oxides against female and male adult worms were observed. the toxicity of the oxadiazole-2-oxides on mammalian cells appeared to be similar to,or less than,that of pzq. conclusions: the antischistosomal activity of the oxadiazole-2-oxides does not depend on no production or the inhibition of sjtgr activity. there may be other functional targets of the oxadiazole-2-oxides in s. japonicum. several of the novel oxadiazole-2-oxides synthesised in this study could be used to develop novel antischistosomal drugs and explore potential molecular targets. © 2016 song et al.
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کلیدواژه
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Antischistosomal activity; Oxadiazole-2-oxide; Schistosoma japonicum; Structure-activity relationship (SAR)
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آدرس
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key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122, China, school of pharmaceutical science,jiangnan university,wuxi,214122, China, school of pharmaceutical science,jiangnan university,wuxi,214122, China, school of pharmaceutical science,jiangnan university,wuxi,214122, China, key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122, China, key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122, China, key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122, China, key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122, China, key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122, China, key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122, China, key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122, China, school of pharmaceutical science,jiangnan university,wuxi,214122, China, school of pharmaceutical science,jiangnan university,wuxi,214122, China, key laboratory on technology for disease prevention and control,ministry of health,jiangsu provincial key laboratory of parasite molecular biology,jiangsu institute of parasitic diseases,wuxi,jiangsu 214064,china,public health research center,jiangnan university,wuxi,214122,china,medical college,jiangnan university,wuxi,214122, China
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Authors
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