Virtual screening and molecular dynamic simulations of the antimalarial derivatives of 2-anilino 4-amino substituted quinazolines docked against a Pf -DHODH protein target.
Zakari Ya'u IbrahimAdamu UzairuGideon Adamu ShallangwaStephen Eyije AbechiSulaiman IsyakuPublished in: The Egyptian journal of medical human genetics (2022)
The ability of these ligands to form hydrogen bonds, as well as various other interactions, was cited as a factor responsible for their better binding affinity. These findings could aid further the development of enhanced antimalarial drugs.