Article
In vitro effects of bis(N-[4-(hydroxyphenyl)methyl]-2-pyridinemethamine) zinc perchlorate monohydrate 4 on the physiology and interaction process of Leishmania amazonensis
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SANGENITO, Leandro S. et al. In vitro effects of bis(N-[4-(hydroxyphenyl)methyl]-2-pyridinemethamine) zinc perchlorate monohydrate 4 on the physiology and interaction process of Leishmania amazonensis. Parasitology International, v. 84, 102376, p. 1-6, May 2021.
1383-5769
10.1016/j.parint.2021.102376
Autor
Sangenito, Leandro S.
Rodrigues, Hallana D.
Santiago, Simone O.
Bombaça, Ana Cristina S.
Menna-Barreto, Rubem F.S.
Reddy, Andrew
Branquinha, Marta H.
Velasco-Torrijos, Trinidad
Santos, André L.S.
Resumen
Despite the high morbidity, mortality and socio-economic impact, few therapeutic options are available for this
disease. To make matters worse, the available molecules have several limitations such as limited efficacy, high
cost, side effects and increased resistance. In this context, our group previously synthesized new compounds with
anti-leishmania potential being the bis(N-[4-(hydroxyphenyl)methyl]-2-pyridinemethamine)zinc perchlorate
monohydrate 4 (complex 4) the most promising one. Therefore, this present work revealed some morphological
and physiological changes promoted by complex 4 on Leishmania amazonensis promastigotes as well as it was
evidenced its potential against intramacrophage amastigotes. Complex 4 promoted a progressive reduction on
the promastigotes size and a remarkable increase on the granularity/complexity as judged by flow cytometry.
Transmission electron microscopy (TEM) analysis revealed extensive mitochondrial and plasma membrane alterations,
although plasma membrane integrity remained. The mitochondrial changes observed by TEM were
accompanied by a decrease in the activity of mitochondrial dehydrogenases with increased production of
reactive oxygen species. Interestingly, promastigotes also showed changes in lipid metabolism. Besides the very
low toxicity to macrophages, complex 4 had a great effect on intramacrophage amastigotes, displaying an IC50 of
3.91 μM. Collectively, the data presented here reinforce the potential of aminopyridyl compounds complexed to
zinc against L. amazonensis. Thus, our work serves as a basis for in vivo assays to be designed or even the synthesis
of more selective/effective compounds with lower cost. 2023
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