6 research outputs found
Hydroxamic acid derivatives: a promising scaffold for rational compound optimization in Chagas disease.
This work describes the antitrypanocidal activity of two hydroxamic acid derivatives containing o-ethoxy (HAD1) and p-ethoxy (HAD2) as substituent in the aromatic ring linked to the isoxazoline ring. HAD1 and HAD2 induced a significant reduction in the number of intracellular parasites and consequently showed activity on the multiplication of the parasite. Treatment of cardiomyocytes and macrophages with the compounds revealed no significant loss in cell viability. Ultrastructural alterations after treatment of cardiomyocytes or macrophages infected by Trypanosoma cruzi with the IC50 value of HAD1 revealed alterations to amastigotes, showing initial damage seen as swelling of the kinetoplast. This gave a good indication of the ability of the drug to permeate through the host cell membrane as well as its selectivity to the parasite target. Both compounds HAD1 and 2 were able to reduce the cysteine peptidases and decrease the activity of metallopeptidases
Hydroxamic acid derivatives: a promising scaffold for rational compound optimization in Chagas disease
This work describes the antitrypanocidal activity of two hydroxamic acid derivatives containing o-ethoxy (HAD1) and p-ethoxy (HAD2) as substituent in the aromatic ring linked to the isoxazoline ring. HAD1 and HAD2 induced a significant reduction in the number of intracellular parasites and consequently showed activity on the multiplication of the parasite. Treatment of cardiomyocytes and macrophages with the compounds revealed no significant loss in cell viability. Ultrastructural alterations after treatment of cardiomyocytes or macrophages infected by Trypanosoma cruzi with the IC50 value of HAD1 revealed alterations to amastigotes, showing initial damage seen as swelling of the kinetoplast. This gave a good indication of the ability of the drug to permeate through the host cell membrane as well as its selectivity to the parasite target. Both compounds HAD1 and 2 were able to reduce the cysteine peptidases and decrease the activity of metallopeptidases
Cloning, Characterization, and Sulfonamide and Thiol Inhibition Studies of an α‑Carbonic Anhydrase from <i>Trypanosoma cruzi</i>, the Causative Agent of Chagas Disease
An α-carbonic anhydrase (CA,
EC 4.2.1.1) has been identified,
cloned, and characterized from the unicellular protozoan <i>Trypanosoma
cruzi</i>, the causative agent of Chagas disease. The enzyme
(TcCA) has a very high catalytic activity for the CO<sub>2</sub> hydration
reaction, being similar kinetically to the human (h) isoform hCA II,
although it is devoid of the His64 proton shuttle. A large number
of aromatic/heterocyclic sulfonamides and some 5-mercapto-1,3,4-thiadiazoles
were investigated as TcCA inhibitors. The aromatic sulfonamides were
weak inhibitors (<i>K</i><sub>I</sub> values of 192 nM to
84 ÎĽM), whereas some heterocyclic compounds inhibited the enzyme
with <i>K</i><sub>I</sub> values in the range 61.6–93.6
nM. The thiols were the most potent in vitro inhibitors (<i>K</i><sub>I</sub> values of 21.1–79.0 nM), and some of them also
inhibited the epimastigotes growth of two <i>T. cruzi</i> strains in vivo