AlphaFold2 可替代小蛋白质的溶液 NMR 结构测定:没那么快

IF 2 3区 化学 Q3 BIOCHEMICAL RESEARCH METHODS Journal of magnetic resonance Pub Date : 2024-07-01 DOI:10.1016/j.jmr.2024.107725
Jeffrey P. Bonin , James M. Aramini , Ying Dong , Hao Wu , Lewis E. Kay
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引用次数: 0

摘要

确定蛋白质的结构往往是从机理上理解其功能的第一步。近年来,计算蛋白质结构预测取得了长足的进步,AlphaFold2(AF2)成为研究人员用于这一目的的主要工具。虽然 AF2 通常能准确预测折叠蛋白质的结构,但我们在此提出一个案例,说明 AF2 以高度置信度错误地预测了一个折叠紧凑的小型蛋白质的结构。这种蛋白质即前白细胞介素-18(pro-IL-18),是细胞因子 IL-18 的前体。有趣的是,AF2 预测的前白细胞介素-18 的结构与成熟细胞因子的结构相吻合,而不是实验测定的前体蛋白的相应结构。因此,尽管计算结构预测在解决蛋白质生物物理问题方面大有可为,但仍然需要进行实验结构测定,即使是折叠良好的小型球状蛋白质也不例外。
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AlphaFold2 as a replacement for solution NMR structure determination of small proteins: Not so fast!

The determination of a protein’s structure is often a first step towards the development of a mechanistic understanding of its function. Considerable advances in computational protein structure prediction have been made in recent years, with AlphaFold2 (AF2) emerging as the primary tool used by researchers for this purpose. While AF2 generally predicts accurate structures of folded proteins, we present here a case where AF2 incorrectly predicts the structure of a small, folded and compact protein with high confidence. This protein, pro-interleukin-18 (pro-IL-18), is the precursor of the cytokine IL-18. Interestingly, the structure of pro-IL-18 predicted by AF2 matches that of the mature cytokine, and not the corresponding experimentally determined structure of the pro-form of the protein. Thus, while computational structure prediction holds immense promise for addressing problems in protein biophysics, there is still a need for experimental structure determination, even in the context of small well-folded, globular proteins.

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来源期刊
CiteScore
3.80
自引率
13.60%
发文量
150
审稿时长
69 days
期刊介绍: The Journal of Magnetic Resonance presents original technical and scientific papers in all aspects of magnetic resonance, including nuclear magnetic resonance spectroscopy (NMR) of solids and liquids, electron spin/paramagnetic resonance (EPR), in vivo magnetic resonance imaging (MRI) and spectroscopy (MRS), nuclear quadrupole resonance (NQR) and magnetic resonance phenomena at nearly zero fields or in combination with optics. The Journal''s main aims include deepening the physical principles underlying all these spectroscopies, publishing significant theoretical and experimental results leading to spectral and spatial progress in these areas, and opening new MR-based applications in chemistry, biology and medicine. The Journal also seeks descriptions of novel apparatuses, new experimental protocols, and new procedures of data analysis and interpretation - including computational and quantum-mechanical methods - capable of advancing MR spectroscopy and imaging.
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