Differential Effects of Paromomycin on Ribosomes of
            <i>Leishmania mexicana</i>
            and Mammalian Cells

Fernández, María Elena Márquez; Malchiodi, Emilio L.; Algranati, Israel D.

doi:10.1128/aac.00506-10

Cited by 50 publications

(40 citation statements)

References 38 publications

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“…The LC 50 values obtained for the 6′-OH AGs (Paromomycin and G418) were in the μM range, and showed good agreement with previous published values for these compounds (18,35,36). The obtained LC 50 values for the 6′-NH 2 derivatives (Neomycin and Gentamicin) were higher than those obtained for the 6′-OH derivatives, and are also in good agreement with previously reported work demonstrating the lower potency of Neomycin B, compared with Paromomycin, for treatment of leishmaniasis (18). These results are also correlated well with the fact that 6′-NH 2 derivatives are less effective against AG resistant bacterial strains containing an A1408G substitution (30).…”

Section: In Vitro Inhibition Of Leishmania Donovani and Leishmania Majorsupporting

confidence: 75%

“…Although no direct evidence is currently available showing that G418 induces miscoding by leishmanial ribosomes, G418 has long been marked as a potent miscoding agent in eukaryotes (38). In addition, a recent work has demonstrated the ability of a structurally related derivative, Paromomycin, to induce miscoding in Leishmania (18). Our modeling data with Paromomycin indeed indicate that the two compounds share a rather great similarity in their binding mechanisms and both might cause the induction of an ON-state conformation upon binding (Fig.…”

Section: Discussionmentioning

confidence: 99%

“…However, the rRNA A site is highly conserved among organisms belonging to all five kingdoms of life (Fig. 1), and together with recent evidence showing that AGs interfere with the leishmanial protein synthesis machinery (9,18,19), this implies that the putative binding site of AGs in Leishmania is similar to that present in bacteria; namely, the leishmanial A site. Recent works by Kondo and coworkers (10,20) described the binding pattern of several natural and semisynthetic AGs to an A1408G mutant Mycobacterium A-site construct.…”

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confidence: 97%

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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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Section: In Vitro Inhibition Of Leishmania Donovani and Leishmania Majorsupporting

confidence: 75%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 97%

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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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“…This antibiotic has shown strong anti-leishmania activity when used alone or in combination with other drugs [75]. In a recent work, advances on the molecular basis for the differential effect of paromomycin on Leishmania have been reported [4]. In this work it was demonstrated that paromomycin selectively inhibits the rate of in vitro protein synthesis by trypanosomatid ribosomes, comparing to mammalian extracts.…”

Section: Selective Inhibition Of Trypanosomatid Ribosomes By Paromomycinmentioning

confidence: 75%

“…Interestingly, this region forms the decoding center, and is also the action site of aminoglycoside antibiotics. Moreover, differences in this region have shown to be responsible for the higher susceptibility of trypanosomatid ribosomes to the aminoglycoside paromomycin [4], as will be discussed below.…”

Section: Introductionmentioning

confidence: 99%

Ribosomes from Trypanosomatids: Unique Structural and Functional Properties

Ayub¹,

Lapadula²,

Hoebeke³

et al. 2012

Cell-Free Protein Synthesis

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Additional information is available at the end of the chapter http://dx.doi.org/10.5772/48336 IntroductionTrypanosomatids are a monophyletic group of protozoa that diverged early from the eukaryotic lineage, constituting valuable model organisms for studying variability in different highly conserved processes including protein synthesis. Moreover, several species of trypanosomatids are causing agents of endemic diseases in the third world. There are many evidences suggesting that translation in these organisms shows important differences with that of model organisms such as yeast and mammals. These unique features, which have a great potential relevance for both basic and applied research, will be discussed in this chapter. Structural analysis Cryo-electron microscopy map of Trypanosoma cruzi ribosome: Unique features of the rRNAUsing the cryo-electron microscopy (cryo-EM) technique, a 12Å resolution density map of the T. cruzi 80S ribosome has been constructed [1]. The overall structure of the T. cruzi 80S ribosome exhibits well defined small (40S) and large (60S) subunits (Figure 1). Some of the landmark characteristics of the ribosome structure can be identified in the density map. Compared with the 80S ribosome from yeast, both the small and large ribosomal subunits from T. cruzi are larger, mainly due to the size of the ribosomal RNA molecules. T. cruzi rRNA (18S rRNA: 2,315 nt and 28S rRNA: 4,151 nt) is one-fifth larger than yeast rRNA (18S rRNA: 1,798 nt; 25S rRNA: 3,392 nt) in total number of nucleotides.Although the T. cruzi 80S ribosome possesses conserved ribosomal structures, it exhibits many distinctive structural features in both the small and large subunits. Compared with other eukaryotic ribosomes, the T. cruzi ribosomal 40S subunit appears expanded, due to the addition of a large piece of density adjacent to the platform region ( Figure 1). As can be seen in the secondary structure of the T. cruzi 18S rRNA (Figure 2), this extra density must be attributed to two large expansion segments (ES) in domain II of the 18S rRNA, ES6 and ES7, designated as insertions of helices 21 and 26. These are the two largest ES in the T. cruzi 18S rRNA, involving 504 and 147 nucleotides, respectively.

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