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Structural modelling and comparative analysis of homologous analogous and specific proteins from Trypanosoma cruzi versus Homo sapiens: putative drug targets for chagas disease treatment

机译:克鲁氏锥虫与智人的同源类似和特异蛋白质的结构建模和比较分析:南美锥虫病治疗的推定药物靶标

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摘要

BackgroundTrypanosoma cruzi is the etiological agent of Chagas' disease, an endemic infection that causes thousands of deaths every year in Latin America. Therapeutic options remain inefficient, demanding the search for new drugs and/or new molecular targets. Such efforts can focus on proteins that are specific to the parasite, but analogous enzymes and enzymes with a three-dimensional (3D) structure sufficiently different from the corresponding host proteins may represent equally interesting targets. In order to find these targets we used the workflows MHOLline and AnEnΠ obtaining 3D models from homologous, analogous and specific proteins of Trypanosoma cruzi versus Homo sapiens.
机译:背景克鲁氏锥虫是恰加斯氏病的病原体,查加斯氏病是一种地方性感染,每年在拉丁美洲造成数千人死亡。治疗选择仍然无效,要求寻找新药和/或新的分子靶标。这样的努力可以集中于对寄生虫特异的蛋白质,但是类似的酶和具有与相应宿主蛋白充分不同的三维(3D)结构的酶可能代表同样有趣的靶标。为了找到这些目标,我们使用了MHOLline和AnEnΠ工作流程,从克氏锥虫与智人的同源,相似和特定蛋白质中获得了3D模型。

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