Structure of Leishmania major cysteine synthase.

Paul K Fyfe, Gareth D Westrop, Tania Ramos, Sylke Müller, Graham H Coombs, William N Hunter
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引用次数: 17

Abstract

Cysteine biosynthesis is a potential target for drug development against parasitic Leishmania species; these protozoa are responsible for a range of serious diseases. To improve understanding of this aspect of Leishmania biology, a crystallographic and biochemical study of L. major cysteine synthase has been undertaken, seeking to understand its structure, enzyme activity and modes of inhibition. Active enzyme was purified, assayed and crystallized in an orthorhombic form with a dimer in the asymmetric unit. Diffraction data extending to 1.8 Å resolution were measured and the structure was solved by molecular replacement. A fragment of γ-poly-D-glutamic acid, a constituent of the crystallization mixture, was bound in the enzyme active site. Although a D-glutamate tetrapeptide had insignificant inhibitory activity, the enzyme was competitively inhibited (K(i) = 4 µM) by DYVI, a peptide based on the C-terminus of the partner serine acetyltransferase with which the enzyme forms a complex. The structure surprisingly revealed that the cofactor pyridoxal phosphate had been lost during crystallization.

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利什曼原虫主要半胱氨酸合酶的结构。
半胱氨酸生物合成是开发抗寄生利什曼原虫药物的潜在靶点;这些原生动物是一系列严重疾病的罪魁祸首。为了提高对利什曼原虫生物学这方面的认识,对L.主要半胱氨酸合成酶进行了晶体学和生化研究,试图了解其结构、酶活性和抑制模式。活性酶被纯化,分析和结晶在一个不对称单元的二聚体的正交形式。测量了1.8 Å分辨率的衍射数据,并用分子置换法求解了结构。结晶混合物的组成成分γ-聚d -谷氨酸片段在酶活性位点结合。虽然d -谷氨酸四肽的抑制活性不明显,但该酶被DYVI竞争性抑制(K(i) = 4µM), DYVI是一种基于伙伴丝氨酸乙酰转移酶c端的肽,该酶与之形成复合物。该结构令人惊讶地揭示了在结晶过程中丢失的辅因子磷酸吡哆醛。
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期刊介绍: Acta Crystallographica Section F is a rapid structural biology communications journal. Articles on any aspect of structural biology, including structures determined using high-throughput methods or from iterative studies such as those used in the pharmaceutical industry, are welcomed by the journal. The journal offers the option of open access, and all communications benefit from unlimited free use of colour illustrations and no page charges. Authors are encouraged to submit multimedia content for publication with their articles. Acta Cryst. F has a dedicated online tool called publBio that is designed to make the preparation and submission of articles easier for authors.
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