Nanostructures for Improved Antimonial Therapy of Leishmaniasis

“…The mechanism of action of pentavalent antimonials has remained essentially unknown. Evidence suggests that pentavalent antimony Sb(V) is a prodrug which is reduced in vivo into trivalent antimony Sb(III) [63,64]. Sb(III) is the active/toxic form that exhibits antileishmanial activity.…”

“…The reduction of Sb(V) to Sb(III) is favored by slightly elevated temperature and acidic pH. This suggests that Sb(V) drugs may act as a molecular carrier releasing the active Sb(III) form in the acidic intracellular compartments where the Leishmania parasites reside [64,65]. The antileishmanial activity of Sb(III) involves multiple pathways, such as: interaction with thiol metabolism of parasites resulting in deoxyribonucleic acid (DNA) fragmentation; inhibition of Leishmania type I DNA topoisomerase which promote adenosine triphosphate (ATP) and guanosine triphosphate (GTP) depletion resulting in the reduction or depletion of parasites energy; promotion the production of proinflammatory cytokines that can increase the release of reactive oxygen species [63].…”

“…Even though pentavalent antimonial drugs are still the first-line medication in several developing countries, they have several limitations due to the toxicity of Sb(III) [64]. These drugs require daily parenteral administration which causes local pain.…”

“…Systemic side effects such as hepatotoxicity, nephrotoxicity, pancreatitis, cardiac toxicity, myalgia, abdominal colic, nausea, vomiting, diarrhea are common during treatment [63,64]. In addition, the development of drug resistance decreases the effectiveness of these compounds [63,64,65]. The use of pentamidine is limited due to toxicity and drug resistance [47].…”

Future Prospects in the Treatment of Parasitic Diseases: 2-Amino-1,3,4-Thiadiazoles in Leishmaniasis

“…The mechanism of action of pentavalent antimonials has remained essentially unknown. Evidence suggests that pentavalent antimony Sb(V) is a prodrug which is reduced in vivo into trivalent antimony Sb(III) [63,64]. Sb(III) is the active/toxic form that exhibits antileishmanial activity.…”

“…The reduction of Sb(V) to Sb(III) is favored by slightly elevated temperature and acidic pH. This suggests that Sb(V) drugs may act as a molecular carrier releasing the active Sb(III) form in the acidic intracellular compartments where the Leishmania parasites reside [64,65]. The antileishmanial activity of Sb(III) involves multiple pathways, such as: interaction with thiol metabolism of parasites resulting in deoxyribonucleic acid (DNA) fragmentation; inhibition of Leishmania type I DNA topoisomerase which promote adenosine triphosphate (ATP) and guanosine triphosphate (GTP) depletion resulting in the reduction or depletion of parasites energy; promotion the production of proinflammatory cytokines that can increase the release of reactive oxygen species [63].…”

“…Even though pentavalent antimonial drugs are still the first-line medication in several developing countries, they have several limitations due to the toxicity of Sb(III) [64]. These drugs require daily parenteral administration which causes local pain.…”

“…Systemic side effects such as hepatotoxicity, nephrotoxicity, pancreatitis, cardiac toxicity, myalgia, abdominal colic, nausea, vomiting, diarrhea are common during treatment [63,64]. In addition, the development of drug resistance decreases the effectiveness of these compounds [63,64,65]. The use of pentamidine is limited due to toxicity and drug resistance [47].…”

Future Prospects in the Treatment of Parasitic Diseases: 2-Amino-1,3,4-Thiadiazoles in Leishmaniasis

“…Accordingly, the World Health Organization has encouraged the development of new drugs to counter this disease. However, drug development is a time-consuming and expensive process 6 . Promising alternatives include the use of pharmaceutical technology in combination with different nanocarriers to minimize side effects and improve efficacy and bioavailability.…”

Use of pharmaceutical nanotechnology for the treatment of leishmaniasis

Chitosan-based particulate systems for drug and vaccine delivery in the treatment and prevention of neglected tropical diseases