Second-generation pterocarpanquinones: synthesis and antileishmanial activity

Faiões, Viviane dos Santos; Frota, Lívia C. R. M. da; Cunha-Júnior, Edézio Ferreira; Barcellos, Júlio C. F.; Silva, Thayssa Da; Netto, Chaquip D.; Da-Silva, Silvia A. G.; Silva, Alcides J. M. da; Costa, Paulo R. R.; Torres-Santos, Eduardo Caio

doi:10.1186/s40409-018-0174-7

Cited by 6 publications

(3 citation statements)

References 40 publications

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“…Considering Colombia as a country with a significant number of pathogenic Leishmania species in circulation, these facts are very critical, bearing in mind that parasite sensitivity to antileishmanial agents relies on Leishmania species [70,71]. For instance, a study evaluated dehydroabietylamine derivatives and found species-dependent susceptibility for several of them [72], being consistent with other reports [73,74]. Indeed, owing to the role of intraand inter-species Leishmania susceptibility [71,75,76], the incorporation of drug-resistant strains during antileishmanial research programs have been strongly recommended [77].…”

Section: General Findingssupporting

confidence: 76%

Colombian Contributions Fighting Leishmaniasis: A Systematic Review on Antileishmanials Combined with Chemoinformatics Analysis

2020

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Leishmaniasis is a parasitic morbid/fatal disease caused by Leishmania protozoa. Twelve million people worldwide are appraised to be currently infected, including ca. two million infections each year, and 350 million people in 88 countries are at risk of becoming infected. In Colombia, cutaneous leishmaniasis (CL) is a public health problem in some tropical areas. Therapeutics is based on traditional antileishmanial drugs, but this practice has several drawbacks for patients. Thus, the search for new antileishmanial agents is a serious need, but the lack of adequately funded research programs on drug discovery has hampered its progress. Some Colombian researchers have conducted different research projects focused on the assessment of the antileishmanial activity of naturally occurring and synthetic compounds against promastigotes and/or amastigotes. Results of such studies have separately demonstrated important hits and reasonable potential, but a holistic view of them is lacking. Hence, we present the outcome from a systematic review of the literature (under PRISMA guidelines) on those Colombian studies investigating antileishmanials during the last thirty-two years. In order to combine the general efforts aiming at finding a lead against Leishmania panamensis (one of the most studied and incident parasites in Colombia causing CL) and to recognize structural features of representative compounds, fingerprint-based analyses using conventional machine learning algorithms and clustering methods are shown. Abstraction from such a meta-description led to describe some function-determining molecular features and simplify the clustering of plausible isofunctional hits. This systematic review indicated that the Colombian efforts for the antileishmanials discovery are increasingly intensified, though improvements in the followed pathways must be definitively pursued. In this context, a brief discussion about scope, strengths and limitations of such advances and relationships is addressed.

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Section: General Findingssupporting

confidence: 76%

Colombian Contributions Fighting Leishmaniasis: A Systematic Review on Antileishmanials Combined with Chemoinformatics Analysis

2020

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“…High-throughput screening has been employed by several researchers either as phenotypic screens [32,102,121,122] or target-specific, such as Leishmania protein disulfide isomerase [40,123]. Several compound classes have been identified with potent antileishmanial activity, including substituted 1,2-dioxanes [124], mono-arylimidamides [125], pterocarpanquinones [126], C-10b-substituted dihydropyrrolo [1,2-b]isoquinolines [127], amino-substituted 1H-phenalen-1-ones [128], and chalcones [129]. For example, Ortalli et al (2018) synthesized 31 novel chalcone compounds, with 16 compounds showing activity against L. donovani promastigotes [129].…”

Section: Drug Discovery Targeting Multiple Species Of Leishmaniamentioning

confidence: 99%

Drug Discovery for Cutaneous Leishmaniasis: A Review of Developments in the Past 15 Years

Corman,

McNamara,

Bakowski

2023

Microorganisms

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Leishmaniasis is a group of vector-borne, parasitic diseases caused by over 20 species of the protozoan Leishmania spp. The three major disease classifications, cutaneous, visceral, and mucocutaneous, have a range of clinical manifestations from self-healing skin lesions to hepatosplenomegaly and mucosal membrane damage to fatality. As a neglected tropical disease, leishmaniasis represents a major international health challenge, with nearly 350 million people living at risk of infection a year. The current chemotherapeutics used to treat leishmaniasis have harsh side effects, prolonged and costly treatment regimens, as well as emerging drug resistance, and are predominantly used for the treatment of visceral leishmaniasis. There is an undeniable need for the identification and development of novel chemotherapeutics targeting cutaneous leishmaniasis (CL), largely ignored by concerted drug development efforts. CL is mostly non-lethal and the most common presentation of this disease, with nearly 1 million new cases reported annually. Recognizing this unaddressed need, substantial yet fragmented progress in early drug discovery efforts for CL has occurred in the past 15 years and was outlined in this review. However, further work needs to be carried out to advance early discovery candidates towards the clinic. Importantly, there is a paucity of investment in the translation and development of therapies for CL, limiting the emergence of viable solutions to deal with this serious and complex international health problem.

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“…The assays were performed in triplicate in 96-well plates (Costar, New York, United States). Inhibition parasite growth was assessed by a fluorescent assay, Resazurin (Sigma-Aldrich) (Faiões et al, 2018). Briefly, 50 µM of resazurin was added per well, and then the samples were incubated for an additional 2 h. The fluorescence was measured using a Spectra Max GEMINI XPS spectrofluorometer (Molecular Devices, Silicon Valley, United States) at excitation and emission wavelengths of 560 and 590 nm, respectively.…”

Section: Antipromastigote Activitymentioning

confidence: 99%

Efficacy of Spironolactone Treatment in Murine Models of Cutaneous and Visceral Leishmaniasis

et al. 2021

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Translational studies involving the reuse and association of drugs are approaches that can result in higher success rates in the discovery and development of drugs for serious public health problems, including leishmaniasis. If we consider the number of pathogenic species in relation to therapeutic options, this arsenal is still small, and each drug possesses a disadvantage in terms of toxicity, efficacy, price, or treatment regimen. In the search for new drugs, we performed a drug screening of L. amazonensis promastigotes and intracellular amastigotes of fifty available drugs belonging to several classes according to their pharmacophoric group. Spironolactone, a potassium-sparing diuretic, proved to be the most promising drug candidate. After demonstrating the in vitro antileishmanial activity, we evaluated the efficacy on a murine experimental model with L. amazonensis and L. infantum. The treatment controlled the cutaneous lesion and reduced the parasite burden of L. amazonensis significantly, as effectively as meglumine antimoniate. The treatment of experimental visceral leishmaniasis was effective in reducing the parasite load on the main affected organs (spleen and liver) via high doses of spironolactone. The association between spironolactone and meglumine antimoniate promoted better control of the parasite load in the spleen and liver compared to the group treated with meglumine antimoniate alone. These results reveal a possible benefit of the concomitant use of spironolactone and meglumine antimoniate that should be studied more in depth for the future possibility of repositioning for leishmaniasis co-therapy.

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Second-generation pterocarpanquinones: synthesis and antileishmanial activity

Cited by 6 publications

References 40 publications

Colombian Contributions Fighting Leishmaniasis: A Systematic Review on Antileishmanials Combined with Chemoinformatics Analysis

Colombian Contributions Fighting Leishmaniasis: A Systematic Review on Antileishmanials Combined with Chemoinformatics Analysis

Drug Discovery for Cutaneous Leishmaniasis: A Review of Developments in the Past 15 Years

Efficacy of Spironolactone Treatment in Murine Models of Cutaneous and Visceral Leishmaniasis

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