Novel Heterocyclic DPP-4 Inhibitors for the Treatment of Type 2 Diabetes
Overview
Authors
Affiliations
Novel deazaxanthine-based DPP-4 inhibitors have been identified that are potent (IC(50) <10nM) and highly selective versus other dipeptidyl peptidases. Their synthesis and SAR are reported, along with initial efforts to improve the PK profile through decoration of the deazaxanthine core. Optimisation of compound 3a resulted in the identification of compound (S)-4i, which displayed an improved in vitro and ADME profile. Further enhancements to the PK profile were possible by changing from the deazahypoxanthine to the deazaxanthine template, culminating in compound 12g, which displayed good ex vivo DPP-4 inhibition and a superior PK profile in rat, suggestive of once daily dosing in man.
Enhancing Drug Design across Multiple Therapeutic Targets with CVAE Generative Models.
Romanelli V, Annunziata D, Cerchia C, Cerciello D, Piccialli F, Lavecchia A ACS Omega. 2024; 9(43):43963-43976.
PMID: 39493989 PMC: 11525747. DOI: 10.1021/acsomega.4c08027.
Nag S, Stany B, Mishra S, Kumar S, Mohanto S, Ahmed M Endocrinol Diabetes Metab. 2024; 7(4):e509.
PMID: 38982323 PMC: 11233261. DOI: 10.1002/edm2.509.
Hossain A, Rahman M, Faruqe M, Saif A, Suhi S, Zaman R Pharmaceutics. 2024; 16(4).
PMID: 38675143 PMC: 11053753. DOI: 10.3390/pharmaceutics16040483.
Heterocyclic compounds as a magic bullet for diabetes mellitus: a review.
Farwa U, Raza M RSC Adv. 2022; 12(35):22951-22973.
PMID: 36105949 PMC: 9379558. DOI: 10.1039/d2ra02697j.
Sajal H, Patil S, Raj R, Shbeer A, Ageel M, Ramu R Molecules. 2022; 27(16).
PMID: 36014373 PMC: 9415412. DOI: 10.3390/molecules27165133.