Association of the endobiont double-stranded RNA virus LRV1 with treatment failure for human leishmaniasis caused by leishmania braziliensis in Peru and Bolivia

Vanessa Adaui; Lon Fye Lye; Natalia S. Akopyants; Mirko Zimic; Alejandro Llanos-Cuentas; Lineth Garcia; Ilse Maes; Simonne De Doncker; Deborah E. Dobson; Jorge Arevalo; Jean Claude Dujardin; Stephen M. Beverley

doi:10.1093/infdis/jiv354

Association of the endobiont double-stranded RNA virus LRV1 with treatment failure for human leishmaniasis caused by leishmania braziliensis in Peru and Bolivia

Vanessa Adaui, Lon Fye Lye, Natalia S. Akopyants, Mirko Zimic, Alejandro Llanos-Cuentas, Lineth Garcia, Ilse Maes, Simonne De Doncker, Deborah E. Dobson, Jorge Arevalo, Jean Claude Dujardin, Stephen M. Beverley

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Abstract

Cutaneous and mucosal leishmaniasis, caused in South America by Leishmania braziliensis, is difficult to cure by chemotherapy (primarily pentavalent antimonials [Sb^V]). Treatment failure does not correlate well with resistance in vitro, and the factors responsible for treatment failure in patients are not well understood. Many isolates of L. braziliensis (>25%) contain a double-stranded RNA virus named Leishmaniavirus 1 (LRV1), which has also been reported in Leishmania guyanensis, for which an association with increased pathology, metastasis, and parasite replication was found in murine models. Here we probed the relationship of LRV1 to drug treatment success and disease in 97 L. braziliensis-infected patients from Peru and Bolivia. In vitro cultures were established, parasites were typed as L. braziliensis, and the presence of LRV1 was determined by reverse transcription-polymerase chain reaction, followed by sequence analysis. LRV1 was associated significantly with an increased risk of treatment failure (odds ratio, 3.99; P =. 04). There was no significant association with intrinsic Sb^V resistance among parasites, suggesting that treatment failure arises from LRV1-mediated effects on host metabolism and/or parasite survival. The association of LRV1 with clinical drug treatment failure could serve to guide more-effective treatment of tegumentary disease caused by L. braziliensis.

Original language	English
Pages (from-to)	112-121
Number of pages	10
Journal	Journal of Infectious Diseases
Volume	213
Issue number	1
DOIs	https://doi.org/10.1093/infdis/jiv354
State	Published - Jan 1 2016

Keywords

leishmaniasis; L. braziliensis; antimony drug treatment; RNA viruses; Viannia; drug treatment failure; drug resistance; Totivirus

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10.1093/infdis/jiv354

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Adaui, V., Lye, L. F., Akopyants, N. S., Zimic, M., Llanos-Cuentas, A., Garcia, L., Maes, I., De Doncker, S., Dobson, D. E., Arevalo, J., Dujardin, J. C., & Beverley, S. M. (2016). Association of the endobiont double-stranded RNA virus LRV1 with treatment failure for human leishmaniasis caused by leishmania braziliensis in Peru and Bolivia. Journal of Infectious Diseases, 213(1), 112-121. https://doi.org/10.1093/infdis/jiv354

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title = "Association of the endobiont double-stranded RNA virus LRV1 with treatment failure for human leishmaniasis caused by leishmania braziliensis in Peru and Bolivia",

abstract = "Cutaneous and mucosal leishmaniasis, caused in South America by Leishmania braziliensis, is difficult to cure by chemotherapy (primarily pentavalent antimonials [SbV]). Treatment failure does not correlate well with resistance in vitro, and the factors responsible for treatment failure in patients are not well understood. Many isolates of L. braziliensis (>25%) contain a double-stranded RNA virus named Leishmaniavirus 1 (LRV1), which has also been reported in Leishmania guyanensis, for which an association with increased pathology, metastasis, and parasite replication was found in murine models. Here we probed the relationship of LRV1 to drug treatment success and disease in 97 L. braziliensis-infected patients from Peru and Bolivia. In vitro cultures were established, parasites were typed as L. braziliensis, and the presence of LRV1 was determined by reverse transcription-polymerase chain reaction, followed by sequence analysis. LRV1 was associated significantly with an increased risk of treatment failure (odds ratio, 3.99; P =. 04). There was no significant association with intrinsic SbV resistance among parasites, suggesting that treatment failure arises from LRV1-mediated effects on host metabolism and/or parasite survival. The association of LRV1 with clinical drug treatment failure could serve to guide more-effective treatment of tegumentary disease caused by L. braziliensis.",

keywords = "leishmaniasis; L. braziliensis; antimony drug treatment; RNA viruses; Viannia; drug treatment failure; drug resistance; Totivirus",

author = "Vanessa Adaui and Lye, {Lon Fye} and Akopyants, {Natalia S.} and Mirko Zimic and Alejandro Llanos-Cuentas and Lineth Garcia and Ilse Maes and {De Doncker}, Simonne and Dobson, {Deborah E.} and Jorge Arevalo and Dujardin, {Jean Claude} and Beverley, {Stephen M.}",

note = "Funding Information: We thank Catherine Ronet and Nicolas Fasel (University of Lausanne, Switzerland), for discussions and communicating unpublished results; F. Matthew Kuhlmann, for advice on the presentation of clinical data; and Jonathan Berman, for discussions concerning SbV treatment failures. This work was supported by the European Commission (to projects LeishBolPe [contract ERBIC18CT960123] and LeishNat-Drug-R [contract ICA4-CT-2001-10076], for parasite collection), the Directorate-General for Development Cooperation of the Belgian Government (framework agreement 03 [project 95502], for parasite characterization and data analysis), and the National Institutes of Health (grant AID R56 AI099364, for LRV1 analysis). Publisher Copyright: {\textcopyright} The Author 2015. Published by Oxford University Press for the Infectious Diseases Society of America.",

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doi = "10.1093/infdis/jiv354",

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Adaui, V, Lye, LF, Akopyants, NS, Zimic, M, Llanos-Cuentas, A, Garcia, L, Maes, I, De Doncker, S, Dobson, DE, Arevalo, J, Dujardin, JC & Beverley, SM 2016, 'Association of the endobiont double-stranded RNA virus LRV1 with treatment failure for human leishmaniasis caused by leishmania braziliensis in Peru and Bolivia', Journal of Infectious Diseases, vol. 213, no. 1, pp. 112-121. https://doi.org/10.1093/infdis/jiv354

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T1 - Association of the endobiont double-stranded RNA virus LRV1 with treatment failure for human leishmaniasis caused by leishmania braziliensis in Peru and Bolivia

AU - Adaui, Vanessa

AU - Lye, Lon Fye

AU - Akopyants, Natalia S.

AU - Zimic, Mirko

AU - Llanos-Cuentas, Alejandro

AU - Garcia, Lineth

AU - Maes, Ilse

AU - De Doncker, Simonne

AU - Dobson, Deborah E.

AU - Arevalo, Jorge

AU - Dujardin, Jean Claude

AU - Beverley, Stephen M.

N1 - Funding Information: We thank Catherine Ronet and Nicolas Fasel (University of Lausanne, Switzerland), for discussions and communicating unpublished results; F. Matthew Kuhlmann, for advice on the presentation of clinical data; and Jonathan Berman, for discussions concerning SbV treatment failures. This work was supported by the European Commission (to projects LeishBolPe [contract ERBIC18CT960123] and LeishNat-Drug-R [contract ICA4-CT-2001-10076], for parasite collection), the Directorate-General for Development Cooperation of the Belgian Government (framework agreement 03 [project 95502], for parasite characterization and data analysis), and the National Institutes of Health (grant AID R56 AI099364, for LRV1 analysis). Publisher Copyright: © The Author 2015. Published by Oxford University Press for the Infectious Diseases Society of America.

PY - 2016/1/1

Y1 - 2016/1/1

N2 - Cutaneous and mucosal leishmaniasis, caused in South America by Leishmania braziliensis, is difficult to cure by chemotherapy (primarily pentavalent antimonials [SbV]). Treatment failure does not correlate well with resistance in vitro, and the factors responsible for treatment failure in patients are not well understood. Many isolates of L. braziliensis (>25%) contain a double-stranded RNA virus named Leishmaniavirus 1 (LRV1), which has also been reported in Leishmania guyanensis, for which an association with increased pathology, metastasis, and parasite replication was found in murine models. Here we probed the relationship of LRV1 to drug treatment success and disease in 97 L. braziliensis-infected patients from Peru and Bolivia. In vitro cultures were established, parasites were typed as L. braziliensis, and the presence of LRV1 was determined by reverse transcription-polymerase chain reaction, followed by sequence analysis. LRV1 was associated significantly with an increased risk of treatment failure (odds ratio, 3.99; P =. 04). There was no significant association with intrinsic SbV resistance among parasites, suggesting that treatment failure arises from LRV1-mediated effects on host metabolism and/or parasite survival. The association of LRV1 with clinical drug treatment failure could serve to guide more-effective treatment of tegumentary disease caused by L. braziliensis.

AB - Cutaneous and mucosal leishmaniasis, caused in South America by Leishmania braziliensis, is difficult to cure by chemotherapy (primarily pentavalent antimonials [SbV]). Treatment failure does not correlate well with resistance in vitro, and the factors responsible for treatment failure in patients are not well understood. Many isolates of L. braziliensis (>25%) contain a double-stranded RNA virus named Leishmaniavirus 1 (LRV1), which has also been reported in Leishmania guyanensis, for which an association with increased pathology, metastasis, and parasite replication was found in murine models. Here we probed the relationship of LRV1 to drug treatment success and disease in 97 L. braziliensis-infected patients from Peru and Bolivia. In vitro cultures were established, parasites were typed as L. braziliensis, and the presence of LRV1 was determined by reverse transcription-polymerase chain reaction, followed by sequence analysis. LRV1 was associated significantly with an increased risk of treatment failure (odds ratio, 3.99; P =. 04). There was no significant association with intrinsic SbV resistance among parasites, suggesting that treatment failure arises from LRV1-mediated effects on host metabolism and/or parasite survival. The association of LRV1 with clinical drug treatment failure could serve to guide more-effective treatment of tegumentary disease caused by L. braziliensis.

KW - leishmaniasis; L. braziliensis; antimony drug treatment; RNA viruses; Viannia; drug treatment failure; drug resistance; Totivirus

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DO - 10.1093/infdis/jiv354

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SN - 0022-1899

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Association of the endobiont double-stranded RNA virus LRV1 with treatment failure for human leishmaniasis caused by leishmania braziliensis in Peru and Bolivia

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