volume 265 pages 108809

Antiparasitic activity of chalcones analogue against Trichomonas vaginalis: biochemical, molecular and in silico aspects

Bárbara Da Rocha Fonseca 1, 2
Raquel Nascimento Das Neves 1, 2
A. L. Strothmann 1, 2
Ângela Sena Lopes 1, 2
Caroline Carapina Da Silva 3, 4
Paloma Taborda Birmann 5, 6
Lucielli Savegnago 6
Cláudio Martin Pereira de Pereira 3
Claudio B. Pereira 4
Sibele Borsuk 2, 7
Publication typeJournal Article
Publication date2024-10-01
scimago Q3
wos Q3
SJR0.414
CiteScore2.8
Impact factor1.6
ISSN00144894, 10902449
Abstract
Trichomonas vaginalis is the etiologic agent of trichomoniasis, a worldwide distributed sexually transmitted infection (STI) that affects the genitourinary tract. Even though this disease already has a treatment in the prescription of drugs of the 5-nitroimidazole class, described low treatments adhesion, adverse side effects and cases of resistant isolates demonstrate the need for new formulations. With this in mind, chalcones emerge as a potential alternative to be tested, being compounds widely distributed in nature, easy to chemically synthesize and presenting several biological activities already reported. In this experiment, we evaluated the antiparasitic activity of 10 chalcone at a concentration of 100 μM against ATCC 30236 T. vaginalis isolates, considering negative (live trophozoites), positive (Metronidazole 100 μM) and vehicle (DMSO 0.6%) controls. Compounds 3a, 3c, 3g and 3i showed promising results, with MICs set at 70 μM, 80 μM, 90 μM and 90 μM, respectively (p<0,05). Cytotoxicity assays were performed on VERO and HMVII cell lines and revealed low inhibition rates at concentrations bellow 20 μM. To elucidate a possible mechanism of action for these molecules, the DPPH, ABTS and FRAP assays were performed, in which none of the four compounds presented antioxidant activity. Assays to verify ROS and lipid peroxidation in the parasite membrane were performed. None of the tested compounds identified ROS accumulation after incubation with trophozoites. 3g molecule promoted an increase in MDA production after incubation. Results presented in this paper demonstrate the promising trichomonicidal profile, although further tests are still needed to optimize their performance and better elucidate the mechanisms of action involved.
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Fonseca B. D. R. et al. Antiparasitic activity of chalcones analogue against Trichomonas vaginalis: biochemical, molecular and in silico aspects // Experimental Parasitology. 2024. Vol. 265. p. 108809.
GOST all authors (up to 50) Copy
Fonseca B. D. R., Das Neves R. N., Strothmann A. L., Sena Lopes Â., Da Silva C. C., Birmann P. T., Savegnago L., de Pereira C. M. P., Pereira C. B., Borsuk S. Antiparasitic activity of chalcones analogue against Trichomonas vaginalis: biochemical, molecular and in silico aspects // Experimental Parasitology. 2024. Vol. 265. p. 108809.
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TY - JOUR
DO - 10.1016/j.exppara.2024.108809
UR - https://linkinghub.elsevier.com/retrieve/pii/S0014489424001127
TI - Antiparasitic activity of chalcones analogue against Trichomonas vaginalis: biochemical, molecular and in silico aspects
T2 - Experimental Parasitology
AU - Fonseca, Bárbara Da Rocha
AU - Das Neves, Raquel Nascimento
AU - Strothmann, A. L.
AU - Sena Lopes, Ângela
AU - Da Silva, Caroline Carapina
AU - Birmann, Paloma Taborda
AU - Savegnago, Lucielli
AU - de Pereira, Cláudio Martin Pereira
AU - Pereira, Claudio B.
AU - Borsuk, Sibele
PY - 2024
DA - 2024/10/01
PB - Elsevier
SP - 108809
VL - 265
PMID - 39094997
SN - 0014-4894
SN - 1090-2449
ER -
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@article{2024_Fonseca,
author = {Bárbara Da Rocha Fonseca and Raquel Nascimento Das Neves and A. L. Strothmann and Ângela Sena Lopes and Caroline Carapina Da Silva and Paloma Taborda Birmann and Lucielli Savegnago and Cláudio Martin Pereira de Pereira and Claudio B. Pereira and Sibele Borsuk},
title = {Antiparasitic activity of chalcones analogue against Trichomonas vaginalis: biochemical, molecular and in silico aspects},
journal = {Experimental Parasitology},
year = {2024},
volume = {265},
publisher = {Elsevier},
month = {oct},
url = {https://linkinghub.elsevier.com/retrieve/pii/S0014489424001127},
pages = {108809},
doi = {10.1016/j.exppara.2024.108809}
}