Self-administered Versus Directly Observed Once-Weekly Isoniazid and Rifapentine Treatment of Latent Tuberculosis Infection: A Randomized Trial

Robert Belknap, David Holland, Pei-Jean Feng, Joan-Pau Millet, Joan A Caylà, Neil A Martinson, Alicia Wright, Michael P Chen, Ruth N Moro, Nigel A Scott, Bert Arevalo, José M Miró, Margarita E Villarino, Marc Weiner, Andrey S Borisov, TB Trials Consortium iAdhere Study Team, Philip Slocum, John K Podgore, Sanda D Small, Mauricio Vecino, Edward M Gardner, Jacqueline D Moore, Randall Reves, Laurie Luna, Neil Schluger, Joseph Burzynski, Vilma Montero, Mascha Elskamp, Payam Nahid, Cindy Merrifield, Irina Rudoy, Julie Higashi, Phil Hopewell, Jose Antonio Martinez, M Carmen Ligero, Laura Garcia, Marta Sala, Emma Fernández, Anna Vilella, Amparo Tricas, Virginia Pomar, M Antonia Sambeat, Jéssica Muñoz, Angels Fontanet, Antonio Moreno, M Llanos Roldán, Arancha Romero, Lucia del Baño, Laia Fina, Pilar Gorrindo, Angels Orcau, Jesús Ospina, Adrià Curran, Israel Molina, Fernando Salvador, Adrian Sanchez-Montalva, Nuria Saborit, Jose Angel Rodrigo, Xavier Martinez, Sonia Uriona, Xavier Martinez-lacasa, Roser Font, Carles Fernández, Hernando Knobel, Neus Jové, Maria Jimenez, Maria Luiza da Souza, Adela Cantos, Richard Chaisson, Chi Chiu Leung, Kwok Chiu Chang, Kalin Fong, Lai Chu Kan, Diane D Wing, Narciso Lopez, Juan J Uribe, Fred M Gordin, S Sonia Qasba, Debra Ann Benator, Shirley Cummins, Carol D Hamilton, Jason E Stout, Elizabeth Ellen Tolley, Emily J Hecker, Melissa Engle, Polo Pavon, Rogelio Duque, Timothy R Sterling, Amy Kerrigan, Diedra Lynnette Freeman, Robert Belknap, David Holland, Pei-Jean Feng, Joan-Pau Millet, Joan A Caylà, Neil A Martinson, Alicia Wright, Michael P Chen, Ruth N Moro, Nigel A Scott, Bert Arevalo, José M Miró, Margarita E Villarino, Marc Weiner, Andrey S Borisov, TB Trials Consortium iAdhere Study Team, Philip Slocum, John K Podgore, Sanda D Small, Mauricio Vecino, Edward M Gardner, Jacqueline D Moore, Randall Reves, Laurie Luna, Neil Schluger, Joseph Burzynski, Vilma Montero, Mascha Elskamp, Payam Nahid, Cindy Merrifield, Irina Rudoy, Julie Higashi, Phil Hopewell, Jose Antonio Martinez, M Carmen Ligero, Laura Garcia, Marta Sala, Emma Fernández, Anna Vilella, Amparo Tricas, Virginia Pomar, M Antonia Sambeat, Jéssica Muñoz, Angels Fontanet, Antonio Moreno, M Llanos Roldán, Arancha Romero, Lucia del Baño, Laia Fina, Pilar Gorrindo, Angels Orcau, Jesús Ospina, Adrià Curran, Israel Molina, Fernando Salvador, Adrian Sanchez-Montalva, Nuria Saborit, Jose Angel Rodrigo, Xavier Martinez, Sonia Uriona, Xavier Martinez-lacasa, Roser Font, Carles Fernández, Hernando Knobel, Neus Jové, Maria Jimenez, Maria Luiza da Souza, Adela Cantos, Richard Chaisson, Chi Chiu Leung, Kwok Chiu Chang, Kalin Fong, Lai Chu Kan, Diane D Wing, Narciso Lopez, Juan J Uribe, Fred M Gordin, S Sonia Qasba, Debra Ann Benator, Shirley Cummins, Carol D Hamilton, Jason E Stout, Elizabeth Ellen Tolley, Emily J Hecker, Melissa Engle, Polo Pavon, Rogelio Duque, Timothy R Sterling, Amy Kerrigan, Diedra Lynnette Freeman

Abstract

Background: Expanding latent tuberculosis treatment is important to decrease active disease globally. Once-weekly isoniazid and rifapentine for 12 doses is effective but limited by requiring direct observation.

Objective: To compare treatment completion and safety of once-weekly isoniazid and rifapentine by self-administration versus direct observation.

Design: An open-label, phase 4 randomized clinical trial designed as a noninferiority study with a 15% margin. Seventy-five percent or more of study patients were enrolled from the United States for a prespecified subgroup analysis. (ClinicalTrials.gov: NCT01582711).

Setting: Outpatient tuberculosis clinics in the United States, Spain, Hong Kong, and South Africa.

Participants: 1002 adults (aged ≥18 years) recommended for treatment of latent tuberculosis infection.

Intervention: Participants received once-weekly isoniazid and rifapentine by direct observation, self-administration with monthly monitoring, or self-administration with weekly text message reminders and monthly monitoring.

Measurements: The primary outcome was treatment completion, defined as 11 or more doses within 16 weeks and measured using clinical documentation and pill counts for direct observation, and self-reports, pill counts, and medication event-monitoring devices for self-administration. The main secondary outcome was adverse events.

Results: Median age was 36 years, 48% of participants were women, and 77% were enrolled at the U.S. sites. Treatment completion was 87.2% (95% CI, 83.1% to 90.5%) in the direct-observation group, 74.0% (CI, 68.9% to 78.6%) in the self-administration group, and 76.4% (CI, 71.3% to 80.8%) in the self-administration-with-reminders group. In the United States, treatment completion was 85.4% (CI, 80.4% to 89.4%), 77.9% (CI, 72.7% to 82.6%), and 76.7% (CI, 70.9% to 81.7%), respectively. Self-administered therapy without reminders was noninferior to direct observation in the United States; no other comparisons met noninferiority criteria. A few drug-related adverse events occurred and were similar across groups.

Limitation: Persons with latent tuberculosis infection enrolled in South Africa would not routinely be treated programmatically.

Conclusion: These results support using self-administered, once-weekly isoniazid and rifapentine to treat latent tuberculosis infection in the United States, and such treatment could be considered in similar settings when direct observation is not feasible.

Primary funding source: Centers for Disease Control and Prevention.

Figures

Figure 1
Figure 1
Study flow diagram DOT = directly observed therapy; LTBI = latent tuberculosis infection; SAT = self-administered therapy; TB = tuberculosis. *Common reasons: did not understand a language available for translation, 41%; history of ≥1 wk of treatment of active TB or LTBI, 19%; HIV-positive with CD4 count 9 cells/L or antiretroviral medications contraindicated with rifapentine, 8%. †Common reasons: preferred regular treatment, 13%; considered DOT to be too inconvenient, 9%; not interested in study medications, 9%; worried about pill burden with once-weekly treatment, 7%. ‡ Common reasons: active, symptomatic comorbidities, 28%; concern for poor adherence, 20%; decision to treat with different regimen, 18%. § The first participant enrolled in each household was randomly assigned to a treatment group. Subsequent participants enrolled from the same household were automatically assigned to the same group as the first participant. || 4 participants (2 in each of the SAT groups) were enrolled as contacts of a person with active TB before susceptibility results had returned showing resistance to isoniazid or rifampin in the source patient. Treatment was stopped, and these participants were included in the safety analysis but excluded from treatment completion.
Figure 2
Figure 2
Weighted treatment completion for all participants, by study group. DOT = directly observed therapy; SAT = self-administered therapy.

Source: PubMed

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