A Dual Marker for Monitoring MDR-TB Treatment: Host-Derived miRNAs and M. tuberculosis-Derived RNA Sequences in Serum

BACKGROUND: In the absence of a late marker of treatment failure or relapse in MDR-TB patients, biomarkers based on host-miRNAs coupled with M. tuberculosis-RNAs evaluated in extracellular vesicles (EVs) are an alternative follow-up for MDR-TB disease. Characterization of EVs cargo to identify diffe...

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Autores principales: Carranza, Claudia, Herrera, María Teresa, Guzmán-Beltrán, Silvia, Salgado-Cantú, Manuel Guadalupe, Salido-Guadarrama, Ivan, Santiago, Elizabeth, Chávez-Galán, Leslie, Gutiérrez-González, Luis Horacio, González, Yolanda
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8600136/
https://www.ncbi.nlm.nih.gov/pubmed/34804048
http://dx.doi.org/10.3389/fimmu.2021.760468
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author Carranza, Claudia
Herrera, María Teresa
Guzmán-Beltrán, Silvia
Salgado-Cantú, Manuel Guadalupe
Salido-Guadarrama, Ivan
Santiago, Elizabeth
Chávez-Galán, Leslie
Gutiérrez-González, Luis Horacio
González, Yolanda
author_facet Carranza, Claudia
Herrera, María Teresa
Guzmán-Beltrán, Silvia
Salgado-Cantú, Manuel Guadalupe
Salido-Guadarrama, Ivan
Santiago, Elizabeth
Chávez-Galán, Leslie
Gutiérrez-González, Luis Horacio
González, Yolanda
author_sort Carranza, Claudia
collection PubMed
description BACKGROUND: In the absence of a late marker of treatment failure or relapse in MDR-TB patients, biomarkers based on host-miRNAs coupled with M. tuberculosis-RNAs evaluated in extracellular vesicles (EVs) are an alternative follow-up for MDR-TB disease. Characterization of EVs cargo to identify differentially expressed miRNAs before and after treatment, and to identify M. tuberculosis-derived RNA in serum EVs from resistant TB patients. METHODS: EVs were isolated from serum of 26 drug-resistant TB (DR-TB) patients and 16 healthy subjects. Differential expression of miRNAs in pooled exosomes from both untreated and treated patients was assessed and individually validated at different time points during treatment. In addition, M. tuberculosis RNA was amplified in the same samples by qPCR. RESULTS: A multivariate analysis using miR-let-7e-5p, -197-3p and -223-3p were found to be a more sensitive discriminator between healthy individuals and those with TB for both DR-TB (AUC= 0.96, 95%, CI=0.907-1) and MDR-TB groups (AUC= 0.95, 95%, CI= 0.89-1). Upregulation of miR-let-7e-5p were observed at the time of M. tuberculosis negative culture T(3-5) for MDR-TB group or for long-term T(9-15) for MDR-TB group without diabetes (T2DM). A second pathogen-based marker based on 30kDa and 5KST sequences was detected in 33% of the MDR-TB patients after the intensive phase of treatment. The miR-let7e-5p is a candidate biomarker for long-term monitoring of treatment for the group of MDR-TB without T2DM. A dual marker of host-derived miR-let7e-5p and M. tuberculosis-derived RNA for monitoring-TB treatment based in serum EVs. CONCLUSION: A dual marker consisting of host-derived miR-let7e-5p and M. tuberculosis-derived RNA, could be an indicator of treatment failure or relapse time after treatment was completed.
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spelling pubmed-86001362021-11-19 A Dual Marker for Monitoring MDR-TB Treatment: Host-Derived miRNAs and M. tuberculosis-Derived RNA Sequences in Serum Carranza, Claudia Herrera, María Teresa Guzmán-Beltrán, Silvia Salgado-Cantú, Manuel Guadalupe Salido-Guadarrama, Ivan Santiago, Elizabeth Chávez-Galán, Leslie Gutiérrez-González, Luis Horacio González, Yolanda Front Immunol Immunology BACKGROUND: In the absence of a late marker of treatment failure or relapse in MDR-TB patients, biomarkers based on host-miRNAs coupled with M. tuberculosis-RNAs evaluated in extracellular vesicles (EVs) are an alternative follow-up for MDR-TB disease. Characterization of EVs cargo to identify differentially expressed miRNAs before and after treatment, and to identify M. tuberculosis-derived RNA in serum EVs from resistant TB patients. METHODS: EVs were isolated from serum of 26 drug-resistant TB (DR-TB) patients and 16 healthy subjects. Differential expression of miRNAs in pooled exosomes from both untreated and treated patients was assessed and individually validated at different time points during treatment. In addition, M. tuberculosis RNA was amplified in the same samples by qPCR. RESULTS: A multivariate analysis using miR-let-7e-5p, -197-3p and -223-3p were found to be a more sensitive discriminator between healthy individuals and those with TB for both DR-TB (AUC= 0.96, 95%, CI=0.907-1) and MDR-TB groups (AUC= 0.95, 95%, CI= 0.89-1). Upregulation of miR-let-7e-5p were observed at the time of M. tuberculosis negative culture T(3-5) for MDR-TB group or for long-term T(9-15) for MDR-TB group without diabetes (T2DM). A second pathogen-based marker based on 30kDa and 5KST sequences was detected in 33% of the MDR-TB patients after the intensive phase of treatment. The miR-let7e-5p is a candidate biomarker for long-term monitoring of treatment for the group of MDR-TB without T2DM. A dual marker of host-derived miR-let7e-5p and M. tuberculosis-derived RNA for monitoring-TB treatment based in serum EVs. CONCLUSION: A dual marker consisting of host-derived miR-let7e-5p and M. tuberculosis-derived RNA, could be an indicator of treatment failure or relapse time after treatment was completed. Frontiers Media S.A. 2021-11-04 /pmc/articles/PMC8600136/ /pubmed/34804048 http://dx.doi.org/10.3389/fimmu.2021.760468 Text en Copyright © 2021 Carranza, Herrera, Guzmán-Beltrán, Salgado-Cantú, Salido-Guadarrama, Santiago, Chávez-Galán, Gutiérrez-González and González https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Carranza, Claudia
Herrera, María Teresa
Guzmán-Beltrán, Silvia
Salgado-Cantú, Manuel Guadalupe
Salido-Guadarrama, Ivan
Santiago, Elizabeth
Chávez-Galán, Leslie
Gutiérrez-González, Luis Horacio
González, Yolanda
A Dual Marker for Monitoring MDR-TB Treatment: Host-Derived miRNAs and M. tuberculosis-Derived RNA Sequences in Serum
title A Dual Marker for Monitoring MDR-TB Treatment: Host-Derived miRNAs and M. tuberculosis-Derived RNA Sequences in Serum
title_full A Dual Marker for Monitoring MDR-TB Treatment: Host-Derived miRNAs and M. tuberculosis-Derived RNA Sequences in Serum
title_fullStr A Dual Marker for Monitoring MDR-TB Treatment: Host-Derived miRNAs and M. tuberculosis-Derived RNA Sequences in Serum
title_full_unstemmed A Dual Marker for Monitoring MDR-TB Treatment: Host-Derived miRNAs and M. tuberculosis-Derived RNA Sequences in Serum
title_short A Dual Marker for Monitoring MDR-TB Treatment: Host-Derived miRNAs and M. tuberculosis-Derived RNA Sequences in Serum
title_sort dual marker for monitoring mdr-tb treatment: host-derived mirnas and m. tuberculosis-derived rna sequences in serum
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8600136/
https://www.ncbi.nlm.nih.gov/pubmed/34804048
http://dx.doi.org/10.3389/fimmu.2021.760468
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