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Structures of type 2 peroxisomal targeting signals in two trypanosomatid aldolases.

机译:2种锥虫性醛缩酶中2型过氧化物酶体靶向信号的结构。

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摘要

Trypanosomatids, unicellular organisms responsible for several global diseases, contain unique organelles called glycosomes in which the first seven glycolytic enzymes are sequestered. We report the crystal structures of glycosomal fructose-1,6-bisphosphate aldolase from two major tropical pathogens, Trypanosoma brucei and Leishmania mexicana, the causative agents of African sleeping sickness and one form of leishmaniasis, respectively. Unlike mammalian aldolases, the T. brucei and L. mexicana aldolases contain nonameric N-terminal type 2 peroxisomal targeting signals (PTS2s) to direct their import into the glycosome. In both tetrameric trypanosomatid aldolases, the PTS2s from two different subunits form two closely intertwined structures. These "PTS2 dimers", which have very similar conformations in the two aldolase structures, are the first reported conformations of a glycosomal or peroxisomal PTS2, and provide opportunities for the design of trypanocidal compounds. Copyright 2000 Academic Press.
机译:锥虫病是造成几种全球性疾病的单细胞生物,含有称为糖体的独特细胞器,其中前七个糖酵解酶被隔离。我们报告了来自两个主要的热带病原体,布鲁氏锥虫和墨西哥利什曼原虫,非洲昏睡病的病原体和利什曼病的一种形式的糖体果糖-1,6-二磷酸醛缩酶的晶体结构。与哺乳动物的醛缩酶不同,布鲁氏菌和墨西哥乳杆菌的醛缩酶含有非异构的N端2型过氧化物酶体靶向信号(PTS2s),以指导其导入糖体中。在两个四聚体锥虫醛糖醛缩酶中,来自两个不同亚基的PTS2形成两个紧密缠绕的结构。这些“ PTS2二聚体”在两个醛缩酶结构中具有非常相似的构象,是糖体或过氧化物酶体PTS2的第一个报道构象,为锥虫杀虫剂化合物的设计提供了机会。版权所有2000学术出版社。

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