Prolonged infectiousness of tuberculosis patients in a directly observed therapy short-course program with standardized therapy

Sean P. Fitzwater; Luz Caviedes; Robert H. Gilman; Jorge Coronel; Doris LaChira; Cayo Salazar; Juan Carlos Saravia; Krishna Reddy; Jon S. Friedland; David A.J. Moore

doi:10.1086/655127

Prolonged infectiousness of tuberculosis patients in a directly observed therapy short-course program with standardized therapy

Sean P. Fitzwater, Luz Caviedes, Robert H. Gilman, Jorge Coronel, Doris LaChira, Cayo Salazar, Juan Carlos Saravia, Krishna Reddy, Jon S. Friedland, David A.J. Moore

Bloomberg School of Public Health

Research output: Contribution to journal › Article › peer-review

45 Scopus citations

Abstract

Background. Effective tuberculosis control is compromised by a lack of clarity about the timeframe of viable Mycobacterium tuberculosis shedding after treatment initiation under programmatic conditions. This study quantifies time to conversion from smear and culture positivity to negativity in unselected tuberculosis patients receiving standardized therapy in a directly observed therapy short-course (DOTS) program. Methods. Longitudinal cohort study following up 93 adults initiating tuberculosis therapy in Lima, Peru. Baseline culture and drug susceptibility tests (DSTs) were performed using the MBBacT, proportion, and microscopic observation drug susceptibility (MODS) methods. Smear microscopy and MODS liquid culture were performed at baseline and weekly for 4 weeks then every other week for 26 weeks. Results. Median conversion time from culture positivity to culture negativity of 38.5 days was unaffected by baseline smear status. Patients with fully susceptible tuberculosis had a median time to culture conversion of 37 days; 10% remained culture positive at day 60. Delayed culture conversion was associated with multidrug resistance, regardless of DST method used; non-multidrug resistance as defined by the proportion method and MODS (but not MBBacT) was also associated with delay. Persistent day 60 smear positivity yielded positive and negative predictive values of 67% and 92%, respectively, for detecting multidrug resistance. Conclusions. Smear and culture conversion in treated tuberculosis patients takes longer than is conventionally believed, even with fully susceptible disease, and must be accounted for in tuberculosis treatment and prevention programs. Persistent day 60 smear positivity is a poor predictor of multidrug resistance. The industrialized-world convention of universal baseline DST for tuberculosis patients should become the standard of care in multidrug resistance-affected resource-limited settings.

Original language	English (US)
Pages (from-to)	371-378
Number of pages	8
Journal	Clinical Infectious Diseases
Volume	51
Issue number	4
DOIs	https://doi.org/10.1086/655127
State	Published - Aug 15 2010

ASJC Scopus subject areas

Microbiology (medical)
Infectious Diseases

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10.1086/655127

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@article{1a21198be770415095e4a384762b7327,

title = "Prolonged infectiousness of tuberculosis patients in a directly observed therapy short-course program with standardized therapy",

abstract = "Background. Effective tuberculosis control is compromised by a lack of clarity about the timeframe of viable Mycobacterium tuberculosis shedding after treatment initiation under programmatic conditions. This study quantifies time to conversion from smear and culture positivity to negativity in unselected tuberculosis patients receiving standardized therapy in a directly observed therapy short-course (DOTS) program. Methods. Longitudinal cohort study following up 93 adults initiating tuberculosis therapy in Lima, Peru. Baseline culture and drug susceptibility tests (DSTs) were performed using the MBBacT, proportion, and microscopic observation drug susceptibility (MODS) methods. Smear microscopy and MODS liquid culture were performed at baseline and weekly for 4 weeks then every other week for 26 weeks. Results. Median conversion time from culture positivity to culture negativity of 38.5 days was unaffected by baseline smear status. Patients with fully susceptible tuberculosis had a median time to culture conversion of 37 days; 10% remained culture positive at day 60. Delayed culture conversion was associated with multidrug resistance, regardless of DST method used; non-multidrug resistance as defined by the proportion method and MODS (but not MBBacT) was also associated with delay. Persistent day 60 smear positivity yielded positive and negative predictive values of 67% and 92%, respectively, for detecting multidrug resistance. Conclusions. Smear and culture conversion in treated tuberculosis patients takes longer than is conventionally believed, even with fully susceptible disease, and must be accounted for in tuberculosis treatment and prevention programs. Persistent day 60 smear positivity is a poor predictor of multidrug resistance. The industrialized-world convention of universal baseline DST for tuberculosis patients should become the standard of care in multidrug resistance-affected resource-limited settings.",

author = "Fitzwater, {Sean P.} and Luz Caviedes and Gilman, {Robert H.} and Jorge Coronel and Doris LaChira and Cayo Salazar and Saravia, {Juan Carlos} and Krishna Reddy and Friedland, {Jon S.} and Moore, {David A.J.}",

note = "Funding Information: Financial support. This study was supported by the Wellcome Trust (grant 064672/Z/01/Z, D.A.J.M.), the National Institute for Health Research Biomedical Research Centre funding scheme at Imperial College (J.S.F. and D.A.J.M.), the National Institute of Allergy and Infectious Diseases (grant T35AI065385, S.P.F.), the National Institutes of Health/Fogarty Global Research Training (grant 3D43 TW006581–04S1, R.H.G.), and the National Institutes of Health/Fogarty International Clinical Research Scholar Awards (K.P.R.). Funders took no part in the design or interpretation of the study. The content of this article is solely the responsibility of the authors and does not necessarily represent the views of the funding sources. Potential conflicts of interest. All authors: no conflicts.",

year = "2010",

month = aug,

day = "15",

doi = "10.1086/655127",

language = "English (US)",

volume = "51",

pages = "371--378",

journal = "Clinical Infectious Diseases",

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T1 - Prolonged infectiousness of tuberculosis patients in a directly observed therapy short-course program with standardized therapy

AU - Fitzwater, Sean P.

AU - Caviedes, Luz

AU - Gilman, Robert H.

AU - Coronel, Jorge

AU - LaChira, Doris

AU - Salazar, Cayo

AU - Saravia, Juan Carlos

AU - Reddy, Krishna

AU - Friedland, Jon S.

AU - Moore, David A.J.

N1 - Funding Information: Financial support. This study was supported by the Wellcome Trust (grant 064672/Z/01/Z, D.A.J.M.), the National Institute for Health Research Biomedical Research Centre funding scheme at Imperial College (J.S.F. and D.A.J.M.), the National Institute of Allergy and Infectious Diseases (grant T35AI065385, S.P.F.), the National Institutes of Health/Fogarty Global Research Training (grant 3D43 TW006581–04S1, R.H.G.), and the National Institutes of Health/Fogarty International Clinical Research Scholar Awards (K.P.R.). Funders took no part in the design or interpretation of the study. The content of this article is solely the responsibility of the authors and does not necessarily represent the views of the funding sources. Potential conflicts of interest. All authors: no conflicts.

PY - 2010/8/15

Y1 - 2010/8/15

N2 - Background. Effective tuberculosis control is compromised by a lack of clarity about the timeframe of viable Mycobacterium tuberculosis shedding after treatment initiation under programmatic conditions. This study quantifies time to conversion from smear and culture positivity to negativity in unselected tuberculosis patients receiving standardized therapy in a directly observed therapy short-course (DOTS) program. Methods. Longitudinal cohort study following up 93 adults initiating tuberculosis therapy in Lima, Peru. Baseline culture and drug susceptibility tests (DSTs) were performed using the MBBacT, proportion, and microscopic observation drug susceptibility (MODS) methods. Smear microscopy and MODS liquid culture were performed at baseline and weekly for 4 weeks then every other week for 26 weeks. Results. Median conversion time from culture positivity to culture negativity of 38.5 days was unaffected by baseline smear status. Patients with fully susceptible tuberculosis had a median time to culture conversion of 37 days; 10% remained culture positive at day 60. Delayed culture conversion was associated with multidrug resistance, regardless of DST method used; non-multidrug resistance as defined by the proportion method and MODS (but not MBBacT) was also associated with delay. Persistent day 60 smear positivity yielded positive and negative predictive values of 67% and 92%, respectively, for detecting multidrug resistance. Conclusions. Smear and culture conversion in treated tuberculosis patients takes longer than is conventionally believed, even with fully susceptible disease, and must be accounted for in tuberculosis treatment and prevention programs. Persistent day 60 smear positivity is a poor predictor of multidrug resistance. The industrialized-world convention of universal baseline DST for tuberculosis patients should become the standard of care in multidrug resistance-affected resource-limited settings.

AB - Background. Effective tuberculosis control is compromised by a lack of clarity about the timeframe of viable Mycobacterium tuberculosis shedding after treatment initiation under programmatic conditions. This study quantifies time to conversion from smear and culture positivity to negativity in unselected tuberculosis patients receiving standardized therapy in a directly observed therapy short-course (DOTS) program. Methods. Longitudinal cohort study following up 93 adults initiating tuberculosis therapy in Lima, Peru. Baseline culture and drug susceptibility tests (DSTs) were performed using the MBBacT, proportion, and microscopic observation drug susceptibility (MODS) methods. Smear microscopy and MODS liquid culture were performed at baseline and weekly for 4 weeks then every other week for 26 weeks. Results. Median conversion time from culture positivity to culture negativity of 38.5 days was unaffected by baseline smear status. Patients with fully susceptible tuberculosis had a median time to culture conversion of 37 days; 10% remained culture positive at day 60. Delayed culture conversion was associated with multidrug resistance, regardless of DST method used; non-multidrug resistance as defined by the proportion method and MODS (but not MBBacT) was also associated with delay. Persistent day 60 smear positivity yielded positive and negative predictive values of 67% and 92%, respectively, for detecting multidrug resistance. Conclusions. Smear and culture conversion in treated tuberculosis patients takes longer than is conventionally believed, even with fully susceptible disease, and must be accounted for in tuberculosis treatment and prevention programs. Persistent day 60 smear positivity is a poor predictor of multidrug resistance. The industrialized-world convention of universal baseline DST for tuberculosis patients should become the standard of care in multidrug resistance-affected resource-limited settings.

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Prolonged infectiousness of tuberculosis patients in a directly observed therapy short-course program with standardized therapy

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