Diagnostic biomarkers for active tuberculosis: progress and challenges
Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis ( Mtb ) transmissi...
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| Vydáno v: | EMBO molecular medicine Ročník 14; číslo 12; s. e14088 - n/a |
|---|---|
| Hlavní autoři: | , , , , , , , , , , |
| Médium: | Journal Article |
| Jazyk: | angličtina |
| Vydáno: |
London
Nature Publishing Group UK
07.12.2022
EMBO Press John Wiley and Sons Inc Springer Nature |
| Témata: | |
| ISSN: | 1757-4676, 1757-4684, 1757-4684 |
| On-line přístup: | Získat plný text |
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| Abstract | Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break
Mycobacterium tuberculosis
(
Mtb
) transmission cycles. In 2020 an estimated 9.9 million people fell ill from
Mtb
, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker‐ or biosignature‐based diagnostics using point‐of‐care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen‐ and host‐based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake.
Graphical Abstract
In this review, B. Andrade and colleagues discuss progress and challenges in the development of diagnostic biomarkers for active tuberculosis and propose potential solutions to improve tuberculosis biomarker validation and implementation. |
|---|---|
| AbstractList | Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break
Mycobacterium tuberculosis
(
Mtb
) transmission cycles. In 2020 an estimated 9.9 million people fell ill from
Mtb
, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker‐ or biosignature‐based diagnostics using point‐of‐care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen‐ and host‐based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake.
Graphical Abstract
In this review, B. Andrade and colleagues discuss progress and challenges in the development of diagnostic biomarkers for active tuberculosis and propose potential solutions to improve tuberculosis biomarker validation and implementation. Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis (Mtb) transmission cycles. In 2020 an estimated 9.9 million people fell ill from Mtb, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker- or biosignature-based diagnostics using point-of-care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen- and host-based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake. Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis ( Mtb ) transmission cycles. In 2020 an estimated 9.9 million people fell ill from Mtb , but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker‐ or biosignature‐based diagnostics using point‐of‐care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen‐ and host‐based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake. Abstract Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis (Mtb) transmission cycles. In 2020 an estimated 9.9 million people fell ill from Mtb, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker‐ or biosignature‐based diagnostics using point‐of‐care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen‐ and host‐based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake. Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis (Mtb) transmission cycles. In 2020 an estimated 9.9 million people fell ill from Mtb, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker‐ or biosignature‐based diagnostics using point‐of‐care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen‐ and host‐based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake. In this review, B. Andrade and colleagues discuss progress and challenges in the development of diagnostic biomarkers for active tuberculosis and propose potential solutions to improve tuberculosis biomarker validation and implementation. Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis (Mtb) transmission cycles. In 2020 an estimated 9.9 million people fell ill from Mtb, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker- or biosignature-based diagnostics using point-of-care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen- and host-based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake.Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis (Mtb) transmission cycles. In 2020 an estimated 9.9 million people fell ill from Mtb, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker- or biosignature-based diagnostics using point-of-care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen- and host-based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake. Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis (Mtb) transmission cycles. In 2020 an estimated 9.9 million people fell ill from Mtb, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker- or biosignature-based diagnostics using point-of-care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen- and host-based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake. Tuberculosis (TB) is a leading cause of morbidity and mortality from a single infectious agent, despite being preventable and curable. Early and accurate diagnosis of active TB is critical to both enhance patient care, improve patient outcomes, and break Mycobacterium tuberculosis (Mtb) transmission cycles. In 2020 an estimated 9.9 million people fell ill from Mtb, but only a little over half (5.8 million) received an active TB diagnosis and treatment. The World Health Organization has proposed target product profiles for biomarker‐ or biosignature‐based diagnostics using point‐of‐care tests from easily accessible specimens such as urine or blood. Here we review and summarize progress made in the development of pathogen‐ and host‐based biomarkers for active TB diagnosis. We describe several unique patient populations that have posed challenges to development of a universal diagnostic TB biomarker, such as people living with HIV, extrapulmonary TB, and children. We also review additional limitations to widespread validation and utilization of published biomarkers. We conclude with proposed solutions to enhance TB diagnostic biomarker validation and uptake. In this review, B. Andrade and colleagues discuss progress and challenges in the development of diagnostic biomarkers for active tuberculosis and propose potential solutions to improve tuberculosis biomarker validation and implementation. |
| Author | Andrade, Bruno B Krishnan, Sonya Queiroz, Artur T L Salgame, Padmini Gupta, Amita Barreto‐Duarte, Beatriz Scriba, Thomas J Sterling, Timothy R Ellner, Jerrold J Nogueira, Betânia M F Araújo‐Pereira, Mariana |
| AuthorAffiliation | 11 South African Tuberculosis Vaccine Initiative and Institute of Infectious Disease and Molecular Medicine, Division of Immunology, Department of Pathology University of Cape Town Cape Town South Africa 13 Curso de Medicina Faculdade de Tecnologia e Ciências (FTC) Salvador Brazil 9 Center of Data and Knowledge Integration for Health (CIDACS), Instituto Gonçalo Moniz Fundação Oswaldo Cruz Salvador Brazil 6 Programa de Pós‐Graduação em Clínica Médica Universidade Federal do Rio de Janeiro Rio de Janeiro Brazil 1 Programa de Pós‐graduação em Ciências da Saúde Universidade Federal da Bahia Salvador Brazil 7 Laboratório de Inflamação e Biomarcadores, Instituto Gonçalo Moniz Fundação Oswaldo Cruz Salvador Brazil 14 Curso de Medicina Escola Bahiana de Medicina e Saúde Pública (EBMSP) Salvador Brazil 5 Curso de Medicina Universidade Salvador (UNIFACS) Salvador Brazil 8 Faculdade de Medicina Universidade Federal da Bahia Salvador Brazil 4 Division of Infectious Diseases, Department of Medicine Johns Ho |
| AuthorAffiliation_xml | – name: 5 Curso de Medicina Universidade Salvador (UNIFACS) Salvador Brazil – name: 1 Programa de Pós‐graduação em Ciências da Saúde Universidade Federal da Bahia Salvador Brazil – name: 3 Multinational Organization Network Sponsoring Translational and Epidemiological Research (MONSTER) Initiative Salvador Brazil – name: 14 Curso de Medicina Escola Bahiana de Medicina e Saúde Pública (EBMSP) Salvador Brazil – name: 8 Faculdade de Medicina Universidade Federal da Bahia Salvador Brazil – name: 10 Department of Medicine, Centre for Emerging Pathogens Rutgers‐New Jersey Medical School Newark NJ USA – name: 2 Instituto Couto Maia Salvador Brazil – name: 6 Programa de Pós‐Graduação em Clínica Médica Universidade Federal do Rio de Janeiro Rio de Janeiro Brazil – name: 4 Division of Infectious Diseases, Department of Medicine Johns Hopkins University School of Medicine Baltimore MD USA – name: 11 South African Tuberculosis Vaccine Initiative and Institute of Infectious Disease and Molecular Medicine, Division of Immunology, Department of Pathology University of Cape Town Cape Town South Africa – name: 7 Laboratório de Inflamação e Biomarcadores, Instituto Gonçalo Moniz Fundação Oswaldo Cruz Salvador Brazil – name: 9 Center of Data and Knowledge Integration for Health (CIDACS), Instituto Gonçalo Moniz Fundação Oswaldo Cruz Salvador Brazil – name: 12 Division of Infectious Diseases, Department of Medicine Vanderbilt University Medical Center Nashville TN USA – name: 13 Curso de Medicina Faculdade de Tecnologia e Ciências (FTC) Salvador Brazil |
| Author_xml | – sequence: 1 givenname: Betânia M F surname: Nogueira fullname: Nogueira, Betânia M F organization: Programa de Pós‐graduação em Ciências da Saúde, Universidade Federal da Bahia, Instituto Couto Maia, Multinational Organization Network Sponsoring Translational and Epidemiological Research (MONSTER) Initiative – sequence: 2 givenname: Sonya surname: Krishnan fullname: Krishnan, Sonya organization: Division of Infectious Diseases, Department of Medicine, Johns Hopkins University School of Medicine – sequence: 3 givenname: Beatriz surname: Barreto‐Duarte fullname: Barreto‐Duarte, Beatriz organization: Multinational Organization Network Sponsoring Translational and Epidemiological Research (MONSTER) Initiative, Curso de Medicina, Universidade Salvador (UNIFACS), Programa de Pós‐Graduação em Clínica Médica, Universidade Federal do Rio de Janeiro, Laboratório de Inflamação e Biomarcadores, Instituto Gonçalo Moniz, Fundação Oswaldo Cruz – sequence: 4 givenname: Mariana surname: Araújo‐Pereira fullname: Araújo‐Pereira, Mariana organization: Multinational Organization Network Sponsoring Translational and Epidemiological Research (MONSTER) Initiative, Laboratório de Inflamação e Biomarcadores, Instituto Gonçalo Moniz, Fundação Oswaldo Cruz, Faculdade de Medicina, Universidade Federal da Bahia – sequence: 5 givenname: Artur T L surname: Queiroz fullname: Queiroz, Artur T L organization: Instituto Couto Maia, Center of Data and Knowledge Integration for Health (CIDACS), Instituto Gonçalo Moniz, Fundação Oswaldo Cruz – sequence: 6 givenname: Jerrold J surname: Ellner fullname: Ellner, Jerrold J organization: Department of Medicine, Centre for Emerging Pathogens, Rutgers‐New Jersey Medical School – sequence: 7 givenname: Padmini surname: Salgame fullname: Salgame, Padmini organization: Department of Medicine, Centre for Emerging Pathogens, Rutgers‐New Jersey Medical School – sequence: 8 givenname: Thomas J orcidid: 0000-0002-0641-1359 surname: Scriba fullname: Scriba, Thomas J organization: South African Tuberculosis Vaccine Initiative and Institute of Infectious Disease and Molecular Medicine, Division of Immunology, Department of Pathology, University of Cape Town – sequence: 9 givenname: Timothy R surname: Sterling fullname: Sterling, Timothy R organization: Division of Infectious Diseases, Department of Medicine, Vanderbilt University Medical Center – sequence: 10 givenname: Amita surname: Gupta fullname: Gupta, Amita organization: Division of Infectious Diseases, Department of Medicine, Johns Hopkins University School of Medicine – sequence: 11 givenname: Bruno B orcidid: 0000-0001-6833-3811 surname: Andrade fullname: Andrade, Bruno B email: bruno.andrade@fiocruz.br organization: Multinational Organization Network Sponsoring Translational and Epidemiological Research (MONSTER) Initiative, Curso de Medicina, Universidade Salvador (UNIFACS), Laboratório de Inflamação e Biomarcadores, Instituto Gonçalo Moniz, Fundação Oswaldo Cruz, Faculdade de Medicina, Universidade Federal da Bahia, Curso de Medicina, Faculdade de Tecnologia e Ciências (FTC), Curso de Medicina, Escola Bahiana de Medicina e Saúde Pública (EBMSP) |
| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/36314872$$D View this record in MEDLINE/PubMed |
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| Keywords | biomarkers diagnostic biomarkers active TB tuberculosis |
| Language | English |
| License | Attribution 2022 The Authors. Published under the terms of the CC BY 4.0 license. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited. |
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| SubjectTerms | active TB Biomarkers Child COVID-19 Diagnosis diagnostic biomarkers EMBO02 EMBO23 HIV Human immunodeficiency virus Humans Morbidity Patients Point of care testing Review Tuberculosis Tuberculosis - diagnosis |
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| Title | Diagnostic biomarkers for active tuberculosis: progress and challenges |
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