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对吡哆醛激酶作为非洲锥虫药物靶点的化学、遗传和结构评估。

Chemical, genetic and structural assessment of pyridoxal kinase as a drug target in the African trypanosome.

机构信息

Division of Biological Chemistry & Drug Discovery, College of Life Sciences, University of Dundee, Dundee, UK.

出版信息

Mol Microbiol. 2012 Oct;86(1):51-64. doi: 10.1111/j.1365-2958.2012.08189.x. Epub 2012 Aug 16.

Abstract

Pyridoxal-5'-phosphate (vitamin B(6) ) is an essential cofactor for many important enzymatic reactions such as transamination and decarboxylation. African trypanosomes are unable to synthesise vitamin B(6) de novo and rely on uptake of B(6) vitamers such as pyridoxal and pyridoxamine from their hosts, which are subsequently phosphorylated by pyridoxal kinase (PdxK). A conditional null mutant of PdxK was generated in Trypanosoma brucei bloodstream forms showing that this enzyme is essential for growth of the parasite in vitro and for infectivity in mice. Activity of recombinant T. brucei PdxK was comparable to previously published work having a specific activity of 327 ± 13 mU mg(-1) and a K(m)(app) with respect to pyridoxal of 29.6 ± 3.9 µM. A coupled assay was developed demonstrating that the enzyme has equivalent catalytic efficiency with pyridoxal, pyridoxamine and pyridoxine, and that ginkgotoxin is an effective pseudo substrate. A high resolution structure of PdxK in complex with ATP revealed important structural differences with the human enzyme. These findings suggest that pyridoxal kinase is an essential and druggable target that could lead to much needed alternative treatments for this devastating disease.

摘要

磷酸吡哆醛(维生素 B6)是许多重要酶促反应的必需辅助因子,如转氨基和脱羧作用。非洲锥虫不能从头合成维生素 B6,依赖于从宿主摄取 B6 维生素,如吡哆醛和吡哆胺,随后由吡哆醛激酶(PdxK)磷酸化。在布氏锥虫血液期形成体中生成了条件性 null 突变体 PdxK,表明该酶对于寄生虫在体外生长和在小鼠中的感染性是必需的。重组 T. brucei PdxK 的活性与之前发表的工作相当,比活为 327 ± 13 mU mg(-1),相对于吡哆醛的 K(m)(app)为 29.6 ± 3.9 µM。开发了一种偶联测定法,证明该酶与吡哆醛、吡哆胺和吡哆醇具有等效的催化效率,而银杏内酯是一种有效的伪底物。与 ATP 结合的 PdxK 的高分辨率结构揭示了与人类酶的重要结构差异。这些发现表明,吡哆醛激酶是一个必需的、可成药的靶点,可以为这种毁灭性疾病带来急需的替代治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bbb6/3470933/3ca9794dadf3/mmi0086-0051-f1.jpg

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