Sensitivity of Leishmania spp. to Glibenclamide and 4-Aminopiridine: A Tool for the Study of Drug Resistance Development

We have demonstrated that Leishmania spp. grown as promastigotes, are sensitive to the K+ channel inhibitors 4-aminopyridine and glibenclamide. Their host cells, the macrophages, are not affected by similar concentrations of the drugs. We have also initiated the molecular characterization of the mechanisms involved in the development of drug resistance to glibenclamide by the parasite. Therefore, we have selected experimentally and begun to characterize the Venezuelan Leishmania (Leishmania) strain, NR resistant to glibenclamide [NR(Gr)]. The analysis of genomic DNA evidenced the existence of a fragment which apparently is amplified in NR(Gr). The fragment recognized by the pgpA probe, related to the Leishmania P-glycoprotein family and which was originally isolated from L. tarentolae, showed a size polymorfism between the sensitive and the resistant strain. These results suggest that the development of resistance to glibenclamide in the strain NR(Gr) might be associated with the amplification of the ltpgpA or related gene(s)

Leishmania; chemotherapy; glibenclamide; 4-aminopyridine; drug resistance; P-glycoprotein

Authorship

Alicia Ponte-Sucre

Yelitza Campos

Jorge Vázquez

Heidrun Moll

Alexis Mendoza-León

SCIMAGO INSTITUTIONS RANKINGS

Figures | Tables

Figures (5)
Tables (1)

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Fig. 1:
Leishmania identification. Genomic DNA from New World Leishmania was digested with the endonuclease Pst I, fractionated on 1% agarose gel, and transferred to a nylon membrane. The blot was hybridized at medium stringency conditions (2x SSC, 0.1% SDS 2X Denhardt solution, 100 µg/ml calf thymus DNA, 67°C) to the Leishmania ß-tubulin clone pLgß4. L. (L.) mexicana M379 (lane 1), L. (L.) amazonensis PH8C5 (lane 2) L. (V.) braziliensis M2903 (lane 4) and L. (V.) guyanensis M4147 (lane 5), were used to identify the Venezuelan L. (L.) NR strain (Lane 3). Molecular weight markers are from the Hind III digestions of l-DNA.

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Fig. 2: effect of the ion channel inhibitors 4-aminopyridine (u) and glibenclamide (l) on the viability of stationary phase of the
Leishmania (L.) NR strain. Data are presented as the mean ± standard error of the mean of 6 replicates. To estimate the fraction of free drug concentration of GLIB in the medium the following equation was used: a_pt = 1/[[alb_pt/alb_nl)][(1-a_nl )/(a_nl) +1], where alb_nland a_nl refer to values of concentration of albumin and the fraction of free drug in an standard condition and alb_ptand a_pt those present in the experimental medium respectively. Use of this equation assumes a molar concentration of drug far less than that of albumin, only one type of drug binding site on albumin and no cooperative binding interactions.

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Fig. 3: sensitivity of the Venezuelan strain
Leishmania (L.) NR strain (sensitive to glibenclamide) to glibenclamide 3 µM (u) and 16 µM (t) and development of resistance by NR to GLIB 3 µM at week 2 (l) and 3 (s) of subculture (a) and number of alive Leishmania (L.) NRcells per field in a sensitive strain NR(Gs) under control conditions and number of alive NR cells in a resistant strain NR(Gr) exposed to GLIB 16 µM (b). Magnification 400 x.

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Fig. 3: sensitivity of the Venezuelan strain
Leishmania (L.) NR strain (sensitive to glibenclamide) to glibenclamide 3 µM (u) and 16 µM (t) and development of resistance by NR to GLIB 3 µM at week 2 (l) and 3 (s) of subculture (a) and number of alive Leishmania (L.) NRcells per field in a sensitive strain NR(Gs) under control conditions and number of alive NR cells in a resistant strain NR(Gr) exposed to GLIB 16 µM (b). Magnification 400 x.

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Fig. 4: southern blot analysis of pgpA sequences in
Leishmania. Genomic DNA from the Venezuelan Leishmania (L.) NR strain (Gs) and (Gr) was digested independently with the enzymes Bam HI (1), Pst I (2) and Hind III (3), fractionated on a 1% agarose gel and transferred to a nitrocellulose blot. The blot was hybridized to the pgpA probe under low stringency conditions. The arrows show the size polymorphism of the fragment obtained by the restriction analysis with Pst I.

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Fig. 1: Leishmania identification. Genomic DNA from New World Leishmania was digested with the endonuclease Pst I, fractionated on 1% agarose gel, and transferred to a nylon membrane. The blot was hybridized at medium stringency conditions (2x SSC, 0.1% SDS 2X Denhardt solution, 100 µg/ml calf thymus DNA, 67°C) to the Leishmania ß-tubulin clone pLgß4. L. (L.) mexicana M379 (lane 1), L. (L.) amazonensis PH8C5 (lane 2) L. (V.) braziliensis M2903 (lane 4) and L. (V.) guyanensis M4147 (lane 5), were used to identify the Venezuelan L. (L.) NR strain (Lane 3). Molecular weight markers are from the Hind III digestions of l-DNA.

Fig. 2: effect of the ion channel inhibitors 4-aminopyridine (u) and glibenclamide (l) on the viability of stationary phase of the Leishmania (L.) NR strain. Data are presented as the mean ± standard error of the mean of 6 replicates. To estimate the fraction of free drug concentration of GLIB in the medium the following equation was used: a_pt = 1/[[alb_pt/alb_nl)][(1-a_nl )/(a_nl) +1], where alb_nland a_nl refer to values of concentration of albumin and the fraction of free drug in an standard condition and alb_ptand a_pt those present in the experimental medium respectively. Use of this equation assumes a molar concentration of drug far less than that of albumin, only one type of drug binding site on albumin and no cooperative binding interactions.

Fig. 3: sensitivity of the Venezuelan strain Leishmania (L.) NR strain (sensitive to glibenclamide) to glibenclamide 3 µM (u) and 16 µM (t) and development of resistance by NR to GLIB 3 µM at week 2 (l) and 3 (s) of subculture (a) and number of alive Leishmania (L.) NRcells per field in a sensitive strain NR(Gs) under control conditions and number of alive NR cells in a resistant strain NR(Gr) exposed to GLIB 16 µM (b). Magnification 400 x.

Fig. 4: southern blot analysis of pgpA sequences in Leishmania. Genomic DNA from the Venezuelan Leishmania (L.) NR strain (Gs) and (Gr) was digested independently with the enzymes Bam HI (1), Pst I (2) and Hind III (3), fractionated on a 1% agarose gel and transferred to a nitrocellulose blot. The blot was hybridized to the pgpA probe under low stringency conditions. The arrows show the size polymorphism of the fragment obtained by the restriction analysis with Pst I.

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Instituto Oswaldo Cruz, Ministério da Saúde Av. Brasil, 4365 - Pavilhão Mourisco, Manguinhos, 21040-900 Rio de Janeiro RJ Brazil, Tel.: (55 21) 2562-1222, Fax: (55 21) 2562 1220 - Rio de Janeiro - RJ - Brazil
E-mail: memorias@fiocruz.br

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Sensitivity of Leishmania spp. to Glibenclamide and 4-Aminopiridine: A Tool for the Study of Drug Resistance Development

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