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AlphaFold 加速了针对痕量胺相关受体 1 的精神药物激动剂的发现。

AlphaFold accelerated discovery of psychotropic agonists targeting the trace amine-associated receptor 1.

机构信息

Science for Life Laboratory, Department of Cell and Molecular Biology, Uppsala University, Box 596, SE-751 24 Uppsala, Sweden.

Neuro Svenningsson, Department of Clinical Neuroscience, Karolinska Institute, SE-171 76 Stockholm, Sweden.

出版信息

Sci Adv. 2024 Aug 9;10(32):eadn1524. doi: 10.1126/sciadv.adn1524. Epub 2024 Aug 7.

Abstract

Artificial intelligence is revolutionizing protein structure prediction, providing unprecedented opportunities for drug design. To assess the potential impact on ligand discovery, we compared virtual screens using protein structures generated by the AlphaFold machine learning method and traditional homology modeling. More than 16 million compounds were docked to models of the trace amine-associated receptor 1 (TAAR1), a G protein-coupled receptor of unknown structure and target for treating neuropsychiatric disorders. Sets of 30 and 32 highly ranked compounds from the AlphaFold and homology model screens, respectively, were experimentally evaluated. Of these, 25 were TAAR1 agonists with potencies ranging from 12 to 0.03 μM. The AlphaFold screen yielded a more than twofold higher hit rate (60%) than the homology model and discovered the most potent agonists. A TAAR1 agonist with a promising selectivity profile and drug-like properties showed physiological and antipsychotic-like effects in wild-type but not in TAAR1 knockout mice. These results demonstrate that AlphaFold structures can accelerate drug discovery.

摘要

人工智能正在彻底改变蛋白质结构预测,为药物设计提供了前所未有的机会。为了评估其对配体发现的潜在影响,我们比较了使用 AlphaFold 机器学习方法生成的蛋白质结构和传统同源建模进行虚拟筛选的结果。将超过 1600 万个化合物对接至痕迹胺相关受体 1(TAAR1)的模型上,该受体是一种未知结构的 G 蛋白偶联受体,也是治疗神经精神疾病的靶点。从 AlphaFold 和同源建模筛选中分别获得了 30 个和 32 个高排名化合物的集合,并进行了实验评估。其中,25 个是 TAAR1 激动剂,其效力范围为 12 至 0.03 μM。AlphaFold 筛选的命中率(60%)比同源建模高两倍以上,并且发现了最有效的激动剂。一种具有有前景的选择性特征和类药性的 TAAR1 激动剂在野生型小鼠中表现出生理和抗精神病样作用,但在 TAAR1 敲除小鼠中则没有。这些结果表明,AlphaFold 结构可以加速药物发现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d314/11305387/a557af83f0f4/sciadv.adn1524-f1.jpg

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