Heterocyclization vs Coupling Reactions: A DNA-Encoded Libraries Case

Author:

Oksiuta Oleksandr V.1ORCID,Pashenko Alexander E.2ORCID,Smalii Radomyr V.3ORCID,Volochnyuk Dmitry M.2ORCID,Ryabukhin Serhii V.2ORCID

Affiliation:

1. Institute of Organic Chemistry of the National Academy of Sciences of Ukraine; Chemspace LLC, Ukraine

2. Institute of Organic Chemistry of the National Academy of Sciences of Ukraine; Enamine Ltd.; Taras Shevchenko National University of Kyiv, Ukraine

3. Enamine Ltd., Ukraine

Abstract

Aim. DNA-encoded libraries technologies (DELT) are gradually becoming an important part of standard drug discovery toolbox. DELT is looking to find its place between classic low-molecular-weight drug candidates on the one hand, and high-molecular-weight antibodies and peptides on the other hand. On its natural path to overcoming the “childhood diseases” typical for every novel technology, DELT has reached a point where the chemical diversity of DNA-encoded libraries (DELs) becomes an important factor to look out for. In this paper, we aim to take a closer look at the chemical diversity of DELs in their present state and find the ways to improve it.Results and discussion. We have identified the DEL-viable building blocks from the Enamine Ltd. stock collection, as well as from Chemspace Ltd. virtual collection, using the SMARTS set, which takes into account all the necessary structural restrictions. Using modern cheminformatics tools, such as Synt-On, we have analyzed the scaffold diversity of both stock and virtual core bi- and tri-functional building blocks (BBs) suitable for DNA-tolerant reactions. The identification of scaffolds from the most recently published on-DNA heterocyclization reactions and analysis of their inclusion into the existing BBs space have shown that novel DNA-tolerant heterocyclizations are extremely useful for expanding chemical diversity in DEL technologies.Conclusions. The analysis performed allowed us to recognize which functional groups should be prioritized as the most impactful when the new BBs are designed. It is also made clear that the development of new DNA-tolerant reactions, including heterocyclizations, have a significant potential to further expand DEL molecular diversity.

Publisher

National University of Pharmacy

Subject

General Medicine

Cited by 3 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Meta-GTM: Visualization and Analysis of the Chemical Library Space;Journal of Chemical Information and Modeling;2023-08-21

2. Assessment of the Commercially Available Chemical Space for Using in the 19F NMR FAXS Method: a Enamine Ltd. Case;Journal of Organic and Pharmaceutical Chemistry;2023-08-21

3. Chemical Library Space: Definition and DNA-Encoded Library Comparison Study Case;Journal of Chemical Information and Modeling;2023-06-27

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