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A Novel Sensitive Immunoassay Targeting the 5-Methylthio-d-Xylofuranose–Lipoarabinomannan Epitope Meets the WHO's Performance Target for Tuberculosis Diagnosis

The only currently commercialized point-of-care assay for tuberculosis (TB) that measures lipoarabinomannan (LAM) in urine (Alere LF-LAM) has insufficient sensitivity. We evaluated the potential of 100 novel monoclonal antibody pairs targeting a variety of LAM epitopes on a sensitive electrochemilum...

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Autores principales: Sigal, George B., Pinter, Abraham, Lowary, Todd L., Kawasaki, Masanori, Li, Andra, Mathew, Anu, Tsionsky, Michael, Zheng, Ruixiang Blake, Plisova, Tatiana, Shen, Ke, Katsuragi, Kiyonori, Choudhary, Alok, Honnen, William J., Nahid, Payam, Denkinger, Claudia M., Broger, Tobias
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6258851/
https://www.ncbi.nlm.nih.gov/pubmed/30257899
http://dx.doi.org/10.1128/JCM.01338-18
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author Sigal, George B.
Pinter, Abraham
Lowary, Todd L.
Kawasaki, Masanori
Li, Andra
Mathew, Anu
Tsionsky, Michael
Zheng, Ruixiang Blake
Plisova, Tatiana
Shen, Ke
Katsuragi, Kiyonori
Choudhary, Alok
Honnen, William J.
Nahid, Payam
Denkinger, Claudia M.
Broger, Tobias
author_facet Sigal, George B.
Pinter, Abraham
Lowary, Todd L.
Kawasaki, Masanori
Li, Andra
Mathew, Anu
Tsionsky, Michael
Zheng, Ruixiang Blake
Plisova, Tatiana
Shen, Ke
Katsuragi, Kiyonori
Choudhary, Alok
Honnen, William J.
Nahid, Payam
Denkinger, Claudia M.
Broger, Tobias
author_sort Sigal, George B.
collection PubMed
description The only currently commercialized point-of-care assay for tuberculosis (TB) that measures lipoarabinomannan (LAM) in urine (Alere LF-LAM) has insufficient sensitivity. We evaluated the potential of 100 novel monoclonal antibody pairs targeting a variety of LAM epitopes on a sensitive electrochemiluminescence platform to improve the diagnostic accuracy. In the screening, many antibody pairs showed high reactivity to purified LAM but performed poorly at detecting urinary LAM in clinical samples, suggesting differences in antigen structure and immunoreactivity of the different LAM sources. The 12 best antibody pairs from the screening were tested in a retrospective case-control study with urine samples from 75 adults with presumptive TB. The best antibody pair reached femtomolar analytical sensitivity for LAM detection and an overall clinical sensitivity of 93% (confidence interval [CI], 80% to 97%) and specificity of 97% (CI, 85% to 100%). Importantly, in HIV-negative subjects positive for TB by sputum smear microscopy, the test achieved a sensitivity of 80% (CI, 55% to 93%). This compares to an overall sensitivity of 33% (CI, 20% to 48%) of the Alere LF-LAM and a sensitivity of 13% (CI, 4% to 38%) in HIV-negative subjects in the same sample set. The capture antibody targets a unique 5-methylthio-d-xylofuranose (MTX)-dependent epitope in LAM that is specific to the Mycobacterium tuberculosis complex and shows no cross-reactivity with fast-growing mycobacteria or other bacteria. The present study provides evidence that improved assay methods and reagents lead to increased diagnostic accuracy. The results of this work have informed the development of a sensitive and specific novel LAM point-of-care assay with the aim to meet the WHO's performance target for TB diagnosis.
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spelling pubmed-62588512018-12-13 A Novel Sensitive Immunoassay Targeting the 5-Methylthio-d-Xylofuranose–Lipoarabinomannan Epitope Meets the WHO's Performance Target for Tuberculosis Diagnosis Sigal, George B. Pinter, Abraham Lowary, Todd L. Kawasaki, Masanori Li, Andra Mathew, Anu Tsionsky, Michael Zheng, Ruixiang Blake Plisova, Tatiana Shen, Ke Katsuragi, Kiyonori Choudhary, Alok Honnen, William J. Nahid, Payam Denkinger, Claudia M. Broger, Tobias J Clin Microbiol Immunoassays The only currently commercialized point-of-care assay for tuberculosis (TB) that measures lipoarabinomannan (LAM) in urine (Alere LF-LAM) has insufficient sensitivity. We evaluated the potential of 100 novel monoclonal antibody pairs targeting a variety of LAM epitopes on a sensitive electrochemiluminescence platform to improve the diagnostic accuracy. In the screening, many antibody pairs showed high reactivity to purified LAM but performed poorly at detecting urinary LAM in clinical samples, suggesting differences in antigen structure and immunoreactivity of the different LAM sources. The 12 best antibody pairs from the screening were tested in a retrospective case-control study with urine samples from 75 adults with presumptive TB. The best antibody pair reached femtomolar analytical sensitivity for LAM detection and an overall clinical sensitivity of 93% (confidence interval [CI], 80% to 97%) and specificity of 97% (CI, 85% to 100%). Importantly, in HIV-negative subjects positive for TB by sputum smear microscopy, the test achieved a sensitivity of 80% (CI, 55% to 93%). This compares to an overall sensitivity of 33% (CI, 20% to 48%) of the Alere LF-LAM and a sensitivity of 13% (CI, 4% to 38%) in HIV-negative subjects in the same sample set. The capture antibody targets a unique 5-methylthio-d-xylofuranose (MTX)-dependent epitope in LAM that is specific to the Mycobacterium tuberculosis complex and shows no cross-reactivity with fast-growing mycobacteria or other bacteria. The present study provides evidence that improved assay methods and reagents lead to increased diagnostic accuracy. The results of this work have informed the development of a sensitive and specific novel LAM point-of-care assay with the aim to meet the WHO's performance target for TB diagnosis. American Society for Microbiology 2018-11-27 /pmc/articles/PMC6258851/ /pubmed/30257899 http://dx.doi.org/10.1128/JCM.01338-18 Text en Copyright © 2018 Sigal et al. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Immunoassays
Sigal, George B.
Pinter, Abraham
Lowary, Todd L.
Kawasaki, Masanori
Li, Andra
Mathew, Anu
Tsionsky, Michael
Zheng, Ruixiang Blake
Plisova, Tatiana
Shen, Ke
Katsuragi, Kiyonori
Choudhary, Alok
Honnen, William J.
Nahid, Payam
Denkinger, Claudia M.
Broger, Tobias
A Novel Sensitive Immunoassay Targeting the 5-Methylthio-d-Xylofuranose–Lipoarabinomannan Epitope Meets the WHO's Performance Target for Tuberculosis Diagnosis
title A Novel Sensitive Immunoassay Targeting the 5-Methylthio-d-Xylofuranose–Lipoarabinomannan Epitope Meets the WHO's Performance Target for Tuberculosis Diagnosis
title_full A Novel Sensitive Immunoassay Targeting the 5-Methylthio-d-Xylofuranose–Lipoarabinomannan Epitope Meets the WHO's Performance Target for Tuberculosis Diagnosis
title_fullStr A Novel Sensitive Immunoassay Targeting the 5-Methylthio-d-Xylofuranose–Lipoarabinomannan Epitope Meets the WHO's Performance Target for Tuberculosis Diagnosis
title_full_unstemmed A Novel Sensitive Immunoassay Targeting the 5-Methylthio-d-Xylofuranose–Lipoarabinomannan Epitope Meets the WHO's Performance Target for Tuberculosis Diagnosis
title_short A Novel Sensitive Immunoassay Targeting the 5-Methylthio-d-Xylofuranose–Lipoarabinomannan Epitope Meets the WHO's Performance Target for Tuberculosis Diagnosis
title_sort novel sensitive immunoassay targeting the 5-methylthio-d-xylofuranose–lipoarabinomannan epitope meets the who's performance target for tuberculosis diagnosis
topic Immunoassays
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6258851/
https://www.ncbi.nlm.nih.gov/pubmed/30257899
http://dx.doi.org/10.1128/JCM.01338-18
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