Leishmaniasis: Current status of available drugs and new potential drug targets

Singh, Nisha; Kumar, Manish; Singh, Rakesh Kumar

doi:10.1016/s1995-7645(12)60084-4

Cited by 336 publications

(289 citation statements)

References 127 publications

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“…Such works highlighted the potential of some AGs for treating nonsense mediated human genetic disorders by encoding near-cognate tRNA molecules at premature termination codon positions (5)(6)(7). Other studies have shown that specific AGs can be used as alternative treatments for infections caused by human parasitic protozoa such as trypanosomiasis, giardiasis, amoebiasis and leishmaniasis (8)(9)(10)(11)(12). Nevertheless, despite the great potential use of AGs for additional therapeutic purposes, very little information is available regarding their molecular mechanisms of action in eukaryotes.…”

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confidence: 99%

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Identification of the molecular attributes required for aminoglycoside activity against Leishmania

Shalev

Kondo

Kopelyanskiy³

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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Leishmaniasis, a parasitic disease caused by protozoa of the genus Leishmania , affects millions of people worldwide. Aminoglycosides are mostly known as highly potent, broad-spectrum antibiotics that exert their antibacterial activity by selectively targeting the decoding A site of the bacterial ribosome, leading to aberrant protein synthesis. Recently, some aminoglycosides have been clinically approved and are currently used worldwide for the treatment of leishmaniasis; however the molecular details by which aminoglycosides induce their deleterious effect on Leishmaina is still rather obscure. Based on high conservation of the decoding site among all kingdoms, it is assumed that the putative binding site of these agents in Leishmania is the ribosomal A site. However, although recent X-ray crystal structures of the bacterial ribosome in complex with aminoglycosides shed light on the mechanism of aminoglycosides action as antibiotics, no such data are presently available regarding their binding site in Leishmania . We present crystal structures of two different aminoglycoside molecules bound to a model of the Leishmania ribosomal A site: Geneticin (G418), a potent aminoglycoside for the treatment of leishmaniasis at a 2.65-Å resolution, and Apramycin, shown to be a strong binder to the leishmanial ribosome lacking an antileishmanial activity at 1.4-Å resolution. The structural data, coupled with in vitro inhibition measurements on two strains of Leishmania , provide insight as to the source of the difference in inhibitory activity of different Aminoglycosides. The combined structural and physiological data sets the ground for rational design of new, and more specific, aminoglycoside derivatives as potential therapeutic agents against leishmaniasis.

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confidence: 99%

“…It affects millions of people worldwide, appearing mainly in tropical and subtropical areas (12). The parasite is transmitted by sandflies and, depending on the type of disease, can be fatal if untreated.…”

mentioning

confidence: 99%

Identification of the molecular attributes required for aminoglycoside activity against Leishmania

Shalev

Kondo

Kopelyanskiy³

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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“…DHFR is a key enzyme in folate metabolism, linked to the production of thymidine (12). In several species of protozoa, the catalytic activities for the enzymes DHFR and TS reside on a single polypeptide chain, constituting a bifunctional DHFR-TS enzyme (14,15).…”

Section: Discussionmentioning

confidence: 99%

“…The ORF of the DHFR-TS has been amplified, cloned and sequenced; the sequences showed a high degree of conservation, both at nucleotide (96%) and protein (90%) level. The bifunctional enzyme has been thus considered as a potential drug target (12,15). Nevertheless, there are no reports on the bifunctional enzyme on Le.…”

Section: Discussionmentioning

confidence: 99%

“…A limited number of drugs is available and each has various shortcomings. Traditional antileishmanial systemic agents such as antimonials, pentamidine and amphotericin are limited by severe toxic side effects, emerging drug resistance and their requirement for parenteral administration (8)(9)(10)(11)(12). Newer agents such as oral miltefosine have shown efficacy and tolerability, although the efficacy of this compound has not been demonstrated for all Leishmania species.…”

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