Biochemistry and Molecular Biology, Interdisciplinary Research Center, Justus Liebig University, Giessen, Germany.
Max Planck Institute for Medical Research, Heidelberg, Germany.
Commun Biol. 2022 Dec 9;5(1):1353. doi: 10.1038/s42003-022-04307-7.
Since unicellular parasites highly depend on NADPH as a source for reducing equivalents, the pentose phosphate pathway, especially the first and rate-limiting NADPH-producing enzyme glucose 6-phosphate dehydrogenase (G6PD), is considered an excellent antitrypanosomatid drug target. Here we present the crystal structure of Leishmania donovani G6PD (LdG6PD) elucidating the unique N-terminal domain of Kinetoplastida G6PDs. Our investigations on the function of the N-domain suggest its involvement in the formation of a tetramer that is completely different from related Trypanosoma G6PDs. Structural and functional investigations further provide interesting insights into the binding mode of LdG6PD, following an ordered mechanism, which is confirmed by a G6P-induced domain shift and rotation of the helical N-domain. Taken together, these insights into LdG6PD contribute to the understanding of G6PDs' molecular mechanisms and provide an excellent basis for further drug discovery approaches.
由于单细胞寄生虫高度依赖 NADPH 作为还原当量的来源,因此戊糖磷酸途径,特别是第一个限速 NADPH 产生酶葡萄糖 6-磷酸脱氢酶(G6PD),被认为是一个很好的抗利什曼原虫药物靶点。在这里,我们展示了莱什曼原虫 G6PD(LdG6PD)的晶体结构,阐明了动基体目 G6PD 独特的 N 端结构域。我们对 N 结构域功能的研究表明,它参与形成一个四聚体,这与相关的锥虫 G6PD 完全不同。结构和功能研究进一步提供了有趣的见解,了解 LdG6PD 的结合模式,遵循有序的机制,这通过 G6P 诱导的结构域位移和螺旋 N 结构域的旋转得到证实。总之,这些对 LdG6PD 的见解有助于理解 G6PD 的分子机制,并为进一步的药物发现方法提供了极好的基础。
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