AlphaFold accelerates artificial intelligence powered drug discovery: efficient discovery of a novel CDK20 small molecule inhibitor

Feng Ren; Xiao Ding; Min Zheng; Mikhail Korzinkin; Xin Cai; Wei Zhu; Alexey Mantsyzov; Alex Aliper; Vladimir Aladinskiy; Zhongying Cao; Shanshan Kong; Xi Long; Bonnie Hei Man Liu; Yingtao Liu; Vladimir Naumov; Anastasia Shneyderman; Ivan V Ozerov; Ju Wang; Frank W Pun; Daniil A Polykovskiy; Chong Sun; Michael Levitt; Alán Aspuru-Guzik; Alex Zhavoronkov

doi:10.1039/d2sc05709c

AlphaFold accelerates artificial intelligence powered drug discovery: efficient discovery of a novel CDK20 small molecule inhibitor

Chem Sci. 2023 Jan 10;14(6):1443-1452. doi: 10.1039/d2sc05709c. eCollection 2023 Feb 8.

Authors

Feng Ren¹, Xiao Ding¹, Min Zheng¹, Mikhail Korzinkin², Xin Cai¹, Wei Zhu¹, Alexey Mantsyzov², Alex Aliper², Vladimir Aladinskiy², Zhongying Cao¹, Shanshan Kong¹, Xi Long², Bonnie Hei Man Liu², Yingtao Liu¹, Vladimir Naumov², Anastasia Shneyderman², Ivan V Ozerov², Ju Wang¹, Frank W Pun², Daniil A Polykovskiy², Chong Sun³, Michael Levitt⁴, Alán Aspuru-Guzik³, Alex Zhavoronkov^{1

2}

Affiliations

¹ Insilico Medicine Shanghai Ltd Suite 901, Tower C, Changtai Plaza, 2889 Jinke Road. Pudong New District Shanghai 201203 China alex@insilico.com.
² Insilico Medicine Kong Kong Ltd Unit 310, 3/F, Building 8W, Phase 2, Hong Kong Science Park, Pak Shek Kok Hong Kong China.
³ Department of Chemistry, Department of Computer Science, University of Toronto, Vector Institute for Artificial Intelligence, Canadian Institute for Advanced Research Toronto Ontario Canada alan@aspuru.com.
⁴ Department of Structural Biology, Stanford University Palo Alto CA USA.

Abstract

The application of artificial intelligence (AI) has been considered a revolutionary change in drug discovery and development. In 2020, the AlphaFold computer program predicted protein structures for the whole human genome, which has been considered a remarkable breakthrough in both AI applications and structural biology. Despite the varying confidence levels, these predicted structures could still significantly contribute to structure-based drug design of novel targets, especially the ones with no or limited structural information. In this work, we successfully applied AlphaFold to our end-to-end AI-powered drug discovery engines, including a biocomputational platform PandaOmics and a generative chemistry platform Chemistry42. A novel hit molecule against a novel target without an experimental structure was identified, starting from target selection towards hit identification, in a cost- and time-efficient manner. PandaOmics provided the protein of interest for the treatment of hepatocellular carcinoma (HCC) and Chemistry42 generated the molecules based on the structure predicted by AlphaFold, and the selected molecules were synthesized and tested in biological assays. Through this approach, we identified a small molecule hit compound for cyclin-dependent kinase 20 (CDK20) with a binding constant Kd value of 9.2 ± 0.5 μM (n = 3) within 30 days from target selection and after only synthesizing 7 compounds. Based on the available data, a second round of AI-powered compound generation was conducted and through this, a more potent hit molecule, ISM042-2-048, was discovered with an average Kd value of 566.7 ± 256.2 nM (n = 3). Compound ISM042-2-048 also showed good CDK20 inhibitory activity with an IC₅₀ value of 33.4 ± 22.6 nM (n = 3). In addition, ISM042-2-048 demonstrated selective anti-proliferation activity in an HCC cell line with CDK20 overexpression, Huh7, with an IC₅₀ of 208.7 ± 3.3 nM, compared to a counter screen cell line HEK293 (IC₅₀ = 1706.7 ± 670.0 nM). This work is the first demonstration of applying AlphaFold to the hit identification process in drug discovery.

Grants and funding

R35 GM122543/GM/NIGMS NIH HHS/United States