Accessing a Medicinal-Chemistry-Relevant Chemical Space with sp2–sp3 Hybrid Heterocyclic Fragments

Raquel Mato; Colin Bournez; Quentin Lefebvre

doi:10.1055/s-0040-1720137

Synthesis, Inhaltsverzeichnis

Synthesis 2024; 56(22): 3450-3458
DOI: 10.1055/s-0040-1720137

paper

Special Topic Dedicated to Prof. Erick Carreira

Accessing a Medicinal-Chemistry-Relevant Chemical Space with sp²–sp³ Hybrid Heterocyclic Fragments

Raquel Mato

,

Colin Bournez

,

Quentin Lefebvre ∗

Abstract

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Dedicated to our co-founder Prof. Erick Carreira

Abstract

Target-first drug discovery relies heavily on protein structure information, which severely limits its application. In recent years, fragment-based drug Design (FBDD) has been identified as an alternative solution, where screening of smaller molecules for lower affinity allowed the use of focused libraries with a higher hit rate. It is shown that coupling an sp²-rich heteroaromatic group with a monofunctional sp³-rich core gives fragments (186 examples) with advantageous physical-chemical properties, covering a chemical space often neglected in traditional libraries.

Key words

fragment-based drug design - azetidine - oxetane - medicinal chemistry - aqueous solubility - logP

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Referenzen

References
1 Kansagra JJ, Raval KY, Ganatra TH. Curr. Trends Pharm. Pharm. Chem. 2022; 4: 120

2a Murray C, Rees D. Nat. Chem. 2009; 1: 187
2b Murray C, Rees D. Angew. Chem. Int. Ed. 2016; 2: 488
2c Kirsch P, Hartman AM, Hirsch AK. H, Empting M. Molecules 2019; 24: 4309

3a Erlanson DA, Fesik SW, Hubbard RE, Jahnke W, Jhoti H. Nat. Rev. Drug. Discov. 2016; 15: 605
3b Fuller N, Spadola L, Cowen S, Patel J, Schönherr H, Cao Q, McKenzie A, Edfeldt F, Rabow A, Goodnow R. Drug Discov. Today 2016; 21: 1272

4 Jhoti H, Williams G, Rees D, Murray CW. Nat. Rev. Drug. Discov. 2013; 12: 644
5 Carreira EM, Fessard TC. Chem. Rev. 2014; 114: 8257

For the importance of accessing 3D chemical space in drug discovery, see

6a Morley AD, Pugliese A, Birchall K, Bower J, Brennan P, Brown N, Chapman T, Drysdale M, Gilbert IH, Hoelder S, Jordan A, Ley SV, Merritt A, Miller D, Swarbrick ME, Wyatt PG. Drug Discov. Today 2013; 18: 1221
6b Prosser KE, Stokes RW, Cohen SM. ACS Med. Chem. Lett. 2020; 11: 1292
6c Silverstri IP, Colbon PJ. J. ACS Med. Chem. Lett. 2021; 12: 1220

7 Troelsen NS, Shanina E, Gonzalez-Romero D, Danková D, Jensen IS. A, Śniady KJ, Nami F, Zhang H, Rademacher C, Cuenda A, Gotfredsen CH, Clausen MH. Angew. Chem. Int. Ed. 2019; 59: 2204
8 Wood DJ, Lopez-Fernandez JD, Knight LE, Al-Khawaldeh I, Gai C, Lin S, Martin MP, Miller DC, Cano C, Endicott JA, Hardcastle IR, Noble ME. M, Waring MJ. J. Med Chem. 2019; 62: 3741

9a Sauer WH. B, Schwarz MK. J. Chem. Inf. Comput. Sci. 2003; 43: 987
9b Hung AW, Ramek A, Wang Y, Kaya T, Wilson JA, Clemons PA, Young DW. Proc. Natl. Acad. Sci. U. S. A. 2011; 108: 6799
9c Zhang R, McIntyre PJ, Collins PM, Foley DJ, Arter C, von Delft F, Bayliss R, Warriner S, Nelson A. Chem. Eur. J. 2019; 25: 6831

Fsp³ and shape are not necessarily correlated, see:

10a Jones SP, Firth JD, Wheldon MC, Atobe M, Hubbard RE, Blakemore DC, De Fusco C, Lucas SC. C, Roughley SD, Vidler LR, Whatton MA, Woolford AJ-A, Wrigley GL, O’Brien P. RSC Med. Chem. 2022; 13: 1614
10b Johnson JA, Nicolaou CA, Kirberger SE, Pandey AK, Hu H, Pomerantz WC. K. ACS Med. Chem. Lett. 2019; 10: 1648

11 Lovering F, Bikker J, Humblet C. J. Med. Chem. 2009; 52: 6752

12a Wermuth CG, Villoutreix B, Grisoni S, Olivier A, Rocher J.-P. In The Practice of Medicinal Chemistry . Wermuth C, Aldous D, Raboisson P, Rognan D. Academic Press; London: 2015: 73
12b Zheng Y.-J, Tice CM. Expert Opin. Drug Discovery 2016; 11: 831

13 ;https://scifinder-n.cas.org/ accessed on 29th July 2024

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