David A. Delgadillo, Lin Wu, Caroline Wang, Yalong Zhang, Kunal K. Jha, Jessica E. Burch, Lygia Silva de Moraes, Isabel Hernandez Rodriguez, Melody J. Tang, Gerald F. Bills, Benjamin P. Tu, Yi Tang, Hosea M. Nelson
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引用次数: 0
摘要
自然界仍然是一个巨大的复杂和功能性代谢物储存库,其结构特征继续推动着制药、农用化学品和材料科学的创新。低温电子显微镜(cryogenic electron microscopy, cryoEM)方法,微晶体电子衍射(microED,一种3D ED技术),已经成为一种强大的工具,以结构表征小分子。尽管微ed在结构化学中扮演着新兴的角色,但其成本和产量限制了其在天然产物(NPs)发现中的应用。虽然样品制备(如阵列)的最新进展为解决这些挑战提供了一个概念性框架,但它们仍未得到证实。在此,我们报告了阵列驱动发现的结构前所未有的NPs家族(zopalides a - e), muurolane型倍半萜苷(rhytidoside a),曲霉毒素类似物(曲霉毒素H和I),以及先前报道的真菌代谢物的四种晶体结构。最后,这是首次在没有其他方法的情况下,仅用少量样品直接用微能谱法测定了新发现的NPs的绝对立体构型
Microcrystal Electron Diffraction-Guided Discovery of Fungal Metabolites
Nature remains a vast repository of complex and functional metabolites whose structural characterization continues to drive innovations in pharmaceuticals, agrochemicals, and materials science. The cryogenic electron microscopy (cryoEM) method, microcrystal electron diffraction (microED, a 3D ED technique), has emerged as a powerful tool to structurally characterize small molecules. Despite this emerging role in structural chemistry, the cost and throughput of microED have limited its application in the discovery of natural products (NPs). While recent advances in sample preparation (e.g., arrayED) have provided a conceptual framework to address these challenges, they have remained unproven. Herein, we report the arrayED-driven discovery of a structurally unprecedented family of NPs (zopalides A–E), a muurolane-type sesquiterpene glycoside (rhytidoside A), aspergillicin analogs (aspergillicins H and I), and four crystal structures of previously reported fungal metabolites. Lastly, this the first time that the absolute stereo configuration of newly discovered NPs has been determined directly by microED alone without other methods using a small amount of sample
期刊介绍:
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