Article
作者: Silva Duarte, Lovaine ; Bizarro, Cristiano Valim ; Galina, Luiza ; Delgado Paz, Josiane ; Sperotto, Nathalia ; Scheibler Rambo, Raoní ; Basso, Luiz Augusto ; Abbadi, Bruno Lopes ; Borsoi, Ana Flávia ; Neves Muniz, Mauro ; Machado, Pablo ; Silveira Grams, Estevão ; Calle González, Laura ; Fries da Silva, Fernanda ; Pissinate, Kenia ; Silva Ramos, Alessandro ; Alberton Perelló, Marcia ; de Matos Czeczot, Alexia ; da Silva Dadda, Adilio ; Souza Macchi Hopf, Fernanda
Utilizing a scaffold-hopping strategy from the drug candidate telacebec, a novel series of 2-(quinolin-4-yloxy)acetamides was synthesized and evaluated as inhibitors of Mycobacterium tuberculosis (Mtb) growth. These compounds demonstrated potent activity against drug-sensitive and multidrug-resistant strains (MIC ≤ 0.02 μM). Leading compounds were evaluated against a known qcrB resistant strain (T313A), and their loss in activity suggested that the cytochrome bc1 complex is the likely target. Additionally, these structures showed high selectivity regarding mammalian cells (selectivity index > 500) and stability across different aqueous media. Furthermore, some of the synthesized quinolines demonstrated aqueous solubility values that exceeded those of telacebec, while maintaining low rates of metabolism. Finally, a selected compound prevented Mtb growth by more than 1.7 log10 colony forming units in a macrophage model of tuberculosis (TB) infection. These findings validate the proposed design and introduce new 2-(quinolin-4-yloxy)acetamides with potential for development in TB drug discovery campaigns.