Discovery of a Biologically Active Bromodomain Inhibitor by Target-Directed Dynamic Combinatorial Chemistry

GARCÍA, PAULA; ALONSO, VICTORIA L.; SERRA, ESTEBAN; ESCALANTE, ANDREA M.; FURLAN, RICARDO L. E.

ACS Medicinal Chemistry Letters

American Chemical Society

Año: 2018

1948-5875

Target-directed dynamic combinatorial chemistry (DCC) has emerged as a strategy for the identification of inhibitors of relevant therapeutic targets. In this contribution, we use this strategy for the identification of a high-affinity binder of a parasite target, the Trypanosoma cruzi bromodomain-containing protein TcBDF3. This protein is essential for viability of T. cruzi, the protozoan parasite that causes Chagas disease. A small dynamic library of acylhydrazones was prepared from aldehydes and acylhydrazides at neutral pH in presence of aniline. The most amplified library member shows: (a) high affinity for the template, (b) interesting antiparasitic activity against different parasite forms and (c) low toxicity against Vero cells. In addition, parasites are rescued from the compound toxicity by TcBDF3 overexpression, suggesting that the toxicity of this compound is due to the TcBDF3 inhibition i.e. the binding event that initially drives the molecular amplification, is reproduced in the parasite leading to selective toxicity.