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The Killing of African Trypanosomes by Ethidium Bromide

Introduced in the 1950s, ethidium bromide (EB) is still used as an anti-trypanosomal drug for African cattle although its mechanism of killing has been unclear and controversial. EB has long been known to cause loss of the mitochondrial genome, named kinetoplast DNA (kDNA), a giant network of interl...

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Autores principales: Roy Chowdhury, Arnab, Bakshi, Rahul, Wang, Jianyang, Yildirir, Gokben, Liu, Beiyu, Pappas-Brown, Valeria, Tolun, Gökhan, Griffith, Jack D., Shapiro, Theresa A., Jensen, Robert E., Englund, Paul T.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3002999/
https://www.ncbi.nlm.nih.gov/pubmed/21187912
http://dx.doi.org/10.1371/journal.ppat.1001226
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author Roy Chowdhury, Arnab
Bakshi, Rahul
Wang, Jianyang
Yildirir, Gokben
Liu, Beiyu
Pappas-Brown, Valeria
Tolun, Gökhan
Griffith, Jack D.
Shapiro, Theresa A.
Jensen, Robert E.
Englund, Paul T.
author_facet Roy Chowdhury, Arnab
Bakshi, Rahul
Wang, Jianyang
Yildirir, Gokben
Liu, Beiyu
Pappas-Brown, Valeria
Tolun, Gökhan
Griffith, Jack D.
Shapiro, Theresa A.
Jensen, Robert E.
Englund, Paul T.
author_sort Roy Chowdhury, Arnab
collection PubMed
description Introduced in the 1950s, ethidium bromide (EB) is still used as an anti-trypanosomal drug for African cattle although its mechanism of killing has been unclear and controversial. EB has long been known to cause loss of the mitochondrial genome, named kinetoplast DNA (kDNA), a giant network of interlocked minicircles and maxicircles. However, the existence of viable parasites lacking kDNA (dyskinetoplastic) led many to think that kDNA loss could not be the mechanism of killing. When recent studies indicated that kDNA is indeed essential in bloodstream trypanosomes and that dyskinetoplastic cells survive only if they have a compensating mutation in the nuclear genome, we investigated the effect of EB on kDNA and its replication. We here report some remarkable effects of EB. Using EM and other techniques, we found that binding of EB to network minicircles is low, probably because of their association with proteins that prevent helix unwinding. In contrast, covalently-closed minicircles that had been released from the network for replication bind EB extensively, causing them, after isolation, to become highly supertwisted and to develop regions of left-handed Z-DNA (without EB, these circles are fully relaxed). In vivo, EB causes helix distortion of free minicircles, preventing replication initiation and resulting in kDNA loss and cell death. Unexpectedly, EB also kills dyskinetoplastic trypanosomes, lacking kDNA, by inhibiting nuclear replication. Since the effect on kDNA occurs at a >10-fold lower EB concentration than that on nuclear DNA, we conclude that minicircle replication initiation is likely EB's most vulnerable target, but the effect on nuclear replication may also contribute to cell killing.
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spelling pubmed-30029992010-12-27 The Killing of African Trypanosomes by Ethidium Bromide Roy Chowdhury, Arnab Bakshi, Rahul Wang, Jianyang Yildirir, Gokben Liu, Beiyu Pappas-Brown, Valeria Tolun, Gökhan Griffith, Jack D. Shapiro, Theresa A. Jensen, Robert E. Englund, Paul T. PLoS Pathog Research Article Introduced in the 1950s, ethidium bromide (EB) is still used as an anti-trypanosomal drug for African cattle although its mechanism of killing has been unclear and controversial. EB has long been known to cause loss of the mitochondrial genome, named kinetoplast DNA (kDNA), a giant network of interlocked minicircles and maxicircles. However, the existence of viable parasites lacking kDNA (dyskinetoplastic) led many to think that kDNA loss could not be the mechanism of killing. When recent studies indicated that kDNA is indeed essential in bloodstream trypanosomes and that dyskinetoplastic cells survive only if they have a compensating mutation in the nuclear genome, we investigated the effect of EB on kDNA and its replication. We here report some remarkable effects of EB. Using EM and other techniques, we found that binding of EB to network minicircles is low, probably because of their association with proteins that prevent helix unwinding. In contrast, covalently-closed minicircles that had been released from the network for replication bind EB extensively, causing them, after isolation, to become highly supertwisted and to develop regions of left-handed Z-DNA (without EB, these circles are fully relaxed). In vivo, EB causes helix distortion of free minicircles, preventing replication initiation and resulting in kDNA loss and cell death. Unexpectedly, EB also kills dyskinetoplastic trypanosomes, lacking kDNA, by inhibiting nuclear replication. Since the effect on kDNA occurs at a >10-fold lower EB concentration than that on nuclear DNA, we conclude that minicircle replication initiation is likely EB's most vulnerable target, but the effect on nuclear replication may also contribute to cell killing. Public Library of Science 2010-12-16 /pmc/articles/PMC3002999/ /pubmed/21187912 http://dx.doi.org/10.1371/journal.ppat.1001226 Text en Roy Chowdhury et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Roy Chowdhury, Arnab
Bakshi, Rahul
Wang, Jianyang
Yildirir, Gokben
Liu, Beiyu
Pappas-Brown, Valeria
Tolun, Gökhan
Griffith, Jack D.
Shapiro, Theresa A.
Jensen, Robert E.
Englund, Paul T.
The Killing of African Trypanosomes by Ethidium Bromide
title The Killing of African Trypanosomes by Ethidium Bromide
title_full The Killing of African Trypanosomes by Ethidium Bromide
title_fullStr The Killing of African Trypanosomes by Ethidium Bromide
title_full_unstemmed The Killing of African Trypanosomes by Ethidium Bromide
title_short The Killing of African Trypanosomes by Ethidium Bromide
title_sort killing of african trypanosomes by ethidium bromide
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3002999/
https://www.ncbi.nlm.nih.gov/pubmed/21187912
http://dx.doi.org/10.1371/journal.ppat.1001226
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