Leishmania tarentolae novel responses to Bi3+-doped strontium aluminum oxyfluorides

Novel therapeutics for the treatment of leishmaniasis are of interest as the disease not only is becoming more prevalent, but drug resistance is increasing in certain regions of the world. Reported here is the use of Bi3+-doped strontium aluminum oxyfluoride phosphors and protease inhibitors to test...

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Published inHeliyon Vol. 7; no. 9; p. e07896
Main Authors Apuzzo, C. Fiore, Sullivan, Eirin C., Platt, David C., Seger-Held, Ian, Jones, Marjorie A.
Format Journal Article
LanguageEnglish
Published Elsevier Ltd 01.09.2021
Elsevier
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Summary:Novel therapeutics for the treatment of leishmaniasis are of interest as the disease not only is becoming more prevalent, but drug resistance is increasing in certain regions of the world. Reported here is the use of Bi3+-doped strontium aluminum oxyfluoride phosphors and protease inhibitors to test in vitro inhibitory activity against cultured promastigote Leishmania tarentolae and effects on L. tarentolae secreted acid phosphatase (SAP) activity. Cell viability did not significantly decrease in the presence of 50 μM anti-perovskite compounds, implying limited cytotoxicity. Yet SAP activity did increase in the cell free preparations with time in the presence of strontium compounds. Of interest was the observation that cell free SAP activity did not increase in the presence of protease inhibitors with or without added strontium compounds. Since secreted proteases may play a role in the maturation of Leishmania SAP and thus be involved with parasite-host infection establishment, this is in further need of evaluation. Nitric oxide production on day 4 post-addition of the strontium compounds was evaluated and showed an approximately 50% decrease in NO production in the presence of two test compounds relative to DMSO control cells. This is the first report of anti-perovskite compound inhibition of NO production by Leishmania. Leishmania, Leishmaniasis, Anti-perovskites, Strontium, Oxyfluorides, Secreted acid phosphatases, Leishmania secreted proteases, Nitric oxide.
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ISSN:2405-8440
2405-8440
DOI:10.1016/j.heliyon.2021.e07896