首页> 外文期刊>Acta crystallographica. Section F, Structural biology communications >Cruzain structures: apocruzain and cruzain bound to S-methyl thiomethanesulfonate and implications for drug design
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Cruzain structures: apocruzain and cruzain bound to S-methyl thiomethanesulfonate and implications for drug design

机译:Cruzain结构:ApoCruzain和Cruzain与S-甲基甲磺酸甲磺酸盐结合并对药物设计的影响

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摘要

Chagas disease, which is caused by Trypanosoma cruzi, affects more than six million people worldwide. Cruzain is the major cysteine protease involved in the survival of this parasite. Here, the expression, purification and crystallization of this enzyme are reported. The cruzain crystals diffracted to 1.2 A ° resolution, yielding two novel cruzain structures: apocruzain and cruzain bound to the reversible covalent inhibitor S-methyl thiomethanesulfonate.Mass-spectrometric experiments confirmed the presence of a methylthiol group attached to the catalytic cysteine. Comparison of these structures with previously published structures indicates the rigidity of the cruzain structure. These results provide further structural information about the enzyme and may help in new in silico studies to identify or optimize novel prototypes of cruzain inhibitors.
机译:Chagas疾病是由Trypanosoma Cruzi引起的,影响全世界超过600万人。 Cruzain是涉及该寄生虫存活的主要半胱氨酸蛋白酶。 这里,报道了该酶的表达,纯化和结晶。 克鲁松晶体衍射至1.2°分辨率,产生两种新的裂解结构:ApOrtuzain和裂解粘附到可逆的共价抑制剂S-甲基甲磺酸甲基磺酸盐。光谱测定实验证实了附着于催化半胱氨酸的甲基硫基基团的存在。 这些结构与先前公布的结构的比较表明了克鲁松结构的刚性。 这些结果提供了有关酶的进一步结构信息,并且可以帮助硅研究中的新型,以识别或优化克鲁松抑制剂的新型原型。

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