Search

Your search keyword '"Ruton, Hinda"' showing total 32 results
Start Over Author "Ruton, Hinda"
32 results on '"Ruton, Hinda"'

1. Effect of early treatment with metformin on risk of emergency care and hospitalization among patients with COVID-19: The TOGETHER randomized platform clinical trial

Author

Reis, Gilmar, dos Santos Moreira Silva, Eduardo Augusto, Medeiros Silva, Daniela Carla, Thabane, Lehana, Cruz Milagres, Aline, Ferreira, Thiago Santiago, Quirino dos Santos, Castilho Vitor, de Figueiredo Neto, Adhemar Dias, Diniz Callegari, Eduardo, Monteiro Savassi, Leonardo Cançado, Campos Simplicio, Maria Izabel, Barra Ribeiro, Luciene, Oliveira, Rosemary, Harari, Ofir, Bailey, Holly, Forrest, Jamie I, Glushchenko, Alla, Sprague, Sheila, McKay, Paula, Rayner, Craig R., Ruton, Hinda, Guyatt, Gordon H., and Mills, Edward J.

Published
2022
Full Text
View/download PDF

2. Rwanda 20 years on: investing in life

Author

Binagwaho, Agnes, Farmer, Paul E, Nsanzimana, Sabin, Karema, Corine, Gasana, Michel, de Dieu Ngirabega, Jean, Ngabo, Fidele, Wagner, Claire M, Nutt, Cameron T, Nyatanyi, Thierry, Gatera, Maurice, Kayiteshonga, Yvonne, Mugeni, Cathy, Mugwaneza, Placidie, Shema, Joseph, Uwaliraye, Parfait, Gaju, Erick, Muhimpundu, Marie Aimee, Dushime, Theophile, Senyana, Florent, Mazarati, Jean Baptiste, Gaju, Celsa Muzayire, Tuyisenge, Lisine, Mutabazi, Vincent, Kyamanywa, Patrick, Rusanganwa, Vincent, Nyemazi, Jean Pierre, Umutoni, Agathe, Kankindi, Ida, Ntizimira, Christian, Ruton, Hinda, Mugume, Nathan, Nkunda, Denis, Ndenga, Espérance, Mubiligi, Joel M, Kakoma, Jean Baptiste, Karita, Etienne, Sekabaraga, Claude, Rusingiza, Emmanuel, Rich, Michael L, Mukherjee, Joia S, Rhatigan, Joseph, Cancedda, Corrado, Bertrand-Farmer, Didi, Bukhman, Gene, Stulac, Sara N, Tapela, Neo M, van der Hoof Holstein, Cassia, Shulman, Lawrence N, Habinshuti, Antoinette, Bonds, Matthew H, Wilkes, Michael S, Lu, Chunling, Smith-Fawzi, Mary C, Swain, JaBaris D, Murphy, Michael P, Ricks, Alan, Kerry, Vanessa B, Bush, Barbara P, Siegler, Richard W, Stern, Cori S, Sliney, Anne, Nuthulaganti, Tej, Karangwa, Injonge, Pegurri, Elisabetta, Dahl, Ophelia, and Drobac, Peter C

Subjects
Generic health relevance, Good Health and Well Being, Child, Child Mortality, Delivery of Health Care, Genocide, HIV Infections, Health Policy, Humans, Rwanda, Tuberculosis, Pulmonary, Warfare, Medical and Health Sciences, General & Internal Medicine
Abstract

Two decades ago, the genocide against the Tutsis in Rwanda led to the deaths of 1 million people, and the displacement of millions more. Injury and trauma were followed by the effects of a devastated health system and economy. In the years that followed, a new course set by a new government set into motion equity-oriented national policies focusing on social cohesion and people-centred development. Premature mortality rates have fallen precipitously in recent years, and life expectancy has doubled since the mid-1990s. Here we reflect on the lessons learned in rebuilding Rwanda's health sector during the past two decades, as the country now prepares itself to take on new challenges in health-care delivery.

Published
2014

3. An Assessment of the Knowledge and Perceptions of Precision Medicine (PM) in the Rwandan Healthcare Setting

Author

Musanabaganwa, Clarisse, primary, Ruton, Hinda, additional, Ruhangaza, Deogratias, additional, Nsabimana, Nicaise, additional, Kayitare, Emmanuel, additional, Muvunyi, Thierry Zawadi, additional, Semakula, Muhammed, additional, Ntirenganya, Faustin, additional, Musoni, Emile, additional, Ndoli, Jules, additional, Hategekimana, Elisee, additional, Nassir, Angus, additional, Makokha, Francis, additional, Uwimana, Aline, additional, Gasana, Joel, additional, Munezero, Pierre Celestin, additional, Uwinkindi, Francois, additional, Muvunyi, Claude Mambo, additional, Nyirazinyoye, Laetitia, additional, Mazarati, Jean Baptiste, additional, and Mutesa, Leon, additional

Published
2023
Full Text
View/download PDF

6. Early Treatment with Pegylated Interferon Lambda for Covid-19

Author

Reis, Gilmar, primary, Moreira Silva, Eduardo A.S., additional, Medeiros Silva, Daniela C., additional, Thabane, Lehana, additional, Campos, Vitoria H.S., additional, Ferreira, Thiago S., additional, Santos, Castilho V.Q., additional, Nogueira, Ana M.R., additional, Almeida, Ana P.F.G., additional, Savassi, Leonardo C.M., additional, Figueiredo-Neto, Adhemar D., additional, Dias, Ana C.F., additional, Freire Júnior, Adelino M., additional, Bitarães, Carina, additional, Milagres, Aline C., additional, Callegari, Eduardo D., additional, Simplicio, Maria I.C., additional, Ribeiro, Luciene B., additional, Oliveira, Rosemary, additional, Harari, Ofir, additional, Wilson, Lindsay A., additional, Forrest, Jamie I., additional, Ruton, Hinda, additional, Sprague, Sheila, additional, McKay, Paula, additional, Guo, Christina M., additional, Limbrick-Oldfield, Eve H., additional, Kanters, Steve, additional, Guyatt, Gordon H., additional, Rayner, Craig R., additional, Kandel, Christopher, additional, Biondi, Mia J., additional, Kozak, Robert, additional, Hansen, Bettina, additional, Zahoor, M. Atif, additional, Arora, Paul, additional, Hislop, Colin, additional, Choong, Ingrid, additional, Feld, Jordan J., additional, Mills, Edward J., additional, and Glenn, Jeffrey S., additional

Published
2023
Full Text
View/download PDF

7. Effectiveness of early-treatment interventions on self-reported long COVID: A multi-arm, multi-stage adaptive platform control trial

Author

Reis, Gilmar, primary, Wilson, Lindsay, additional, Ayers, Dieter, additional, Silva, Eduardo, additional, Medeiros, Daniela, additional, Thabane, Lehana, additional, Campos, Vitoria, additional, Ferreira, Thiago, additional, Santos, Castilho dos, additional, Nogueira, Ana Maria, additional, Almeida, Ana Paula, additional, Savassi, Leonardo, additional, Neto, Adhemar, additional, Rocha, Ana Carolina, additional, Bitarães, Carina, additional, Milagres, Aline, additional, Callegari, Eduardo, additional, Simplicio, Maria, additional, Ribeiro, Luciene, additional, França, Carla, additional, Oliveira, Rosemary, additional, Forrest, Jamie, additional, Harari, Ofir, additional, Ruton, Hinda, additional, Sprague, Sheila, additional, McKay, Paula, additional, Guo, Christina, additional, Silva, Josue, additional, Guyatt, Gordon, additional, Rayner, Craig, additional, Dybul, Mark, additional, Glenn, Jeffrey S, additional, and Mills, Edward, additional

Published
2023
Full Text
View/download PDF

8. A multi-center, adaptive, randomized, platform trial to evaluate the effect of repurposed medicines in outpatients with early coronavirus disease 2019 (COVID-19) and high-risk for complications: the TOGETHER master trial

Author

Zannat, Noor-E, Reis, Gilmar, Silva, Eduardo, Silva, Daniela, Thorlund, Kristian, Thabane, Lehana, Guyatt, Gordon, Forrest, Jamie, Glushchenko, Alla, Chernecki, Cameron, McKay, Paula, Sprague, Sheila, Harari, Ofir, Ruton, Hinda, Rayner, Craig, and Mills, Edward

Subjects
Life Sciences
Abstract

Background Although vaccines are currently available for coronavirus disease 2019 (COVID-19), there remains a need for an effective and affordable outpatient treatment for early COVID-19. Multiple repurposed drugs have shown promise in treating COVID-19. We describe a master protocol that will assess the efficacy of different repurposed drugs as treatments for early COVID-19 among outpatients at a high risk for severe complications. Methods The TOGETHER Trial is an international (currently in Brazil), multi-center platform adaptive randomized, placebo-controlled, clinical trial. Patients are included if they are at least 18 years of age, have a positive antigen test for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), and have an indication for high risk of disease severity, including co-morbidities, older age, or high body mass index. Eligible patients are randomized with equal chance to an investigational product (IP) or to placebo. The primary endpoint is emergency room required observation for more than 6 hours or hospitalization due to clinical worsening of COVID-19; up to 28 days after randomization. Key secondary endpoints include viral clearance, clinical improvement, hospitalization for any cause, mortality for any cause, and safety and tolerability of each IP. Scheduled interim analyses are conducted and reviewed by the Data and Safety Monitoring Committee (DSMC), who make recommendations on continuing or stopping each IP. The platform adaptive design go-no go decision rules are extended to dynamically incorporate external evidence on COVID-19 interventions from ongoing independent randomized clinical trials. Discussion Results from this trial will assist in the identification of therapeutics for COVID-19 that can easily be scaled in low- and middle-income settings. The novel methodological extension of the platform adaptive design to dynamically incorporate external evidence is one of the first of its kind and may provide highly valuable information for all COVID-19 trials going forward.

Published
2022
Full Text
View/download PDF

9. Assessing routine health information system performance during the tenth outbreak of Ebola virus disease (2018–2020) in the Democratic Republic of the Congo: A qualitative study in North Kivu

Author

Kyomba, Gabriel Kalombe, primary, Kiyombo, Guillaume Mbela, additional, Grépin, Karen A., additional, Mayaka, Serge Manitu, additional, Mambu, Thérèse Nyangi-Mondo, additional, Hategeka, Celestin, additional, Mapatano, Mala Ali, additional, Alcayna-Stevens, Lys, additional, Kapanga, Serge Kule, additional, Konde, Joël Nkima-Numbi, additional, Ngo, Dosithée Bebe, additional, Babakazo, Pélagie Diambalula, additional, Mafuta, Eric Musalu, additional, Lulebo, Aimée Mampasi, additional, Ruton, Hinda, additional, and Law, Michael R., additional

Published
2022
Full Text
View/download PDF

10. Towards Improving Data Quality in Electronic Medical Records: An Investigation of Data Completeness in a Tertiary Hospital in Rwanda.

Author

UWASE, Melissa, de Dieu IRADUKUNDA, Jean, RUSA, Divine Umutesi, NDAHIMANA, Raphael, MVUYEKURE, Briand, BIRINDABAGABO, Pascal, RUTON, Hinda, MPUNGA, Tharcisse, MUGISHA, Michael, TWIZERE, Celestin, and TUMUSIIME, David

Abstract

Data quality is a primary barrier to using electronic medical records (EMR) data for clinical and research purposes. Although EMR has been in use for a long time in LMICs, its data has been seldomly used. This study aimed to assess the completeness of demographic and clinical data in a tertiary hospital in Rwanda. We conducted a cross-sectional study and assessed 92,153 patient data recorded in EMR from October 1st to December 31st, 2022. The findings indicated that over 92% of social demographic data elements were complete, and the completeness of clinical data elements ranged from 27% to 89%. The completeness of data varied markedly by departments. We recommend an exploratory study to understand further reasons associated with the completeness of data in clinical departments. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

11. Effect of Early Treatment with Ivermectin among Patients with Covid-19

Author

Reis, Gilmar, primary, Silva, Eduardo A.S.M., additional, Silva, Daniela C.M., additional, Thabane, Lehana, additional, Milagres, Aline C., additional, Ferreira, Thiago S., additional, dos Santos, Castilho V.Q., additional, Campos, Vitoria H.S., additional, Nogueira, Ana M.R., additional, de Almeida, Ana P.F.G., additional, Callegari, Eduardo D., additional, Neto, Adhemar D.F., additional, Savassi, Leonardo C.M., additional, Simplicio, Maria I.C., additional, Ribeiro, Luciene B., additional, Oliveira, Rosemary, additional, Harari, Ofir, additional, Forrest, Jamie I., additional, Ruton, Hinda, additional, Sprague, Sheila, additional, McKay, Paula, additional, Guo, Christina M., additional, Rowland-Yeo, Karen, additional, Guyatt, Gordon H., additional, Boulware, David R., additional, Rayner, Craig R., additional, and Mills, Edward J., additional

Published
2022
Full Text
View/download PDF

12. Effect of early treatment with fluvoxamine on risk of emergency care and hospitalisation among patients with COVID-19: the TOGETHER randomised, platform clinical trial

Author

Reis, Gilmar, primary, dos Santos Moreira-Silva, Eduardo Augusto, additional, Silva, Daniela Carla Medeiros, additional, Thabane, Lehana, additional, Milagres, Aline Cruz, additional, Ferreira, Thiago Santiago, additional, dos Santos, Castilho Vitor Quirino, additional, de Souza Campos, Vitoria Helena, additional, Nogueira, Ana Maria Ribeiro, additional, de Almeida, Ana Paula Figueiredo Guimaraes, additional, Callegari, Eduardo Diniz, additional, de Figueiredo Neto, Adhemar Dias, additional, Savassi, Leonardo Cançado Monteiro, additional, Simplicio, Maria Izabel Campos, additional, Ribeiro, Luciene Barra, additional, Oliveira, Rosemary, additional, Harari, Ofir, additional, Forrest, Jamie I, additional, Ruton, Hinda, additional, Sprague, Sheila, additional, McKay, Paula, additional, Glushchenko, Alla V, additional, Rayner, Craig R, additional, Lenze, Eric J, additional, Reiersen, Angela M, additional, Guyatt, Gordon H, additional, and Mills, Edward J, additional

Published
2022
Full Text
View/download PDF

13. Latent Tuberculosis Infection and Associated Factors among Health Care Workers in Kigali, Rwanda.

Author

Claude Rutanga, David W Lowrance, John E Oeltmann, Grace Mutembayire, Matt Willis, Claude Bernard Uwizeye, Ruton Hinda, Chitou Bassirou, Steve Gutreuter, and Michel Gasana

Subjects
Medicine, Science
Abstract

Data are limited regarding tuberculosis (TB) and latent TB infection prevalence in Rwandan health facilities.We conducted a cross-sectional survey among healthcare workers (HCWs) in Kigali during 2010. We purposively selected the public referral hospital, both district hospitals, and randomly selected 7 of 17 health centers. School workers (SWs) from the nearest willing public schools served as a local reference group. We tested for latent TB infection (LTBI) using tuberculin skin testing (TST) and asked about past TB disease. We assessed risk of LTBI and past history of TB disease associated with hospital employment. Among HCWs, we assessed risk associated with facility type (district hospital, referral hospital, health center), work setting (inpatient, outpatient), and occupation.Age, gender, and HIV status was similar between the enrolled 1,131 HCWs and 381 SWs. LTBI was more prevalent among HCWs (62%) than SWs (39%). Adjusted odds of a positive TST result were 2.71 (95% CI 2.01-3.67) times greater among HCWs than SWs. Among HCWs, there was no detectable difference between prevalence of LTBI according to facility type, work setting, or occupation.HCWs are at greater risk of LTBI, regardless of facility type, work setting, or occupation. The current status of TB infection control practices should be evaluated in the entire workforce in all Rwandan healthcare facilities.

Published
2015
Full Text
View/download PDF

14. A multi-center, adaptive, randomized, platform trial to evaluate the effect of repurposed medicines in outpatients with early coronavirus disease 2019 (COVID-19) and high-risk for complications: the TOGETHER master trial protocol

Author

Reis, Gilmar, primary, Silva, Eduardo Augusto dos Santos Moreira, additional, Silva, Daniela Carla Medeiros, additional, Thorlund, Kristian, additional, Thabane, Lehana, additional, Guyatt, Gordon H., additional, Forrest, Jamie I., additional, Glushchenko, Alla V., additional, Chernecki, Cameron, additional, McKay, Paula, additional, Sprague, Sheila, additional, Harari, Ofir, additional, Ruton, Hinda, additional, Rayner, Craig R., additional, and Mills, Edward J., additional

Published
2021
Full Text
View/download PDF

15. HIV-free survival among nine- to 24-month-old children born to HIV-positive mothers in the Rwandan national PMTCT programme: a community-based household survey

Author

Ruton, Hinda, Mugwaneza, Placidie, Shema, Nadine, Lyambabaje, Alexandre, Bizimana, Jean De Dieu, Tsague, Landry, Nyankesha, Elevanie, Wagner, Claire M., Mutabazi, Vincent, Nyemazi, Jean Pierre, Nsanzimana, Sabin, Karema, Corine, and Binagwaho, Agnes

Subjects
HIV infection in children -- Prevention -- Patient outcomes -- Distribution, Community health services -- Evaluation -- Management, Disease transmission -- Prevention -- Demographic aspects, Mothers -- Health aspects, Company business management, Company distribution practices, Health
Abstract

Background: Operational effectiveness of large‐scale national programmes for the prevention of mother to child transmission (PMTCT) of HIV in sub‐Saharan Africa remains limited. We report on HIV‐free survival among nine‐ to 24‐month‐old children born to HIV‐positive mothers in the national PMTCT programme in Rwanda. Methods: We conducted a national representative household survey between February and May 2009. Participants were mothers who had attended antenatal care at least once during their most recent pregnancy, and whose children were aged nine to 24 months. A two‐stage stratified (geographic location of PMTCT site, maternal HIV status during pregnancy) cluster sampling was used to select mother‐infant pairs to be interviewed during household visits. Alive children born from HIV‐positive mothers (HIV‐exposed children) were tested for HIV according to routine HIV testing protocol. We calculated HIV‐free survival at nine to 24 months. We subsequently determined factors associated with mother to child transmission of HIV, child death and HIV‐free survival using logistic regression. Results: Out of 1448 HIV‐exposed children surveyed, 44 (3.0%) were reported dead by nine months of age. Of the 1340 children alive, 53 (4.0%) tested HIV positive. HIV‐free survival was estimated at 91.9% (95% confidence interval: 90.4‐93.3%) at nine to 24 months. Adjusting for maternal, child and health system factors, being a member of an association of people living with HIV (adjusted odds ratio: 0.7, 95% CI: 0.1‐0.995) improved by 30% HIV‐free survival among children, whereas the maternal use of a highly active antiretroviral therapy (HAART) regimen for PMTCT (aOR: 0.6, 95% CI: 0.3‐1.07) had a borderline effect. Conclusions: HIV‐free survival among HIV‐exposed children aged nine to 24 months is estimated at 91.9% in Rwanda. The national PMTCT programme could achieve greater impact on child survival by ensuring access to HAART for all HIV‐positive pregnant women in need, improving the quality of the programme in rural areas, and strengthening linkages with community‐based support systems, including associations of people living with HIV., Background Worldwide, 2.5 million children younger than 15 years were living with HIV in 2009, and more than 90% had been infected via mother to child transmission (MTCT) of HIV [...]

Published
2012
Full Text
View/download PDF

17. Impact of a free care policy on the utilisation of health services during an Ebola outbreak in the Democratic Republic of Congo: an interrupted time-series analysis

Author

Hung, Yuen W, primary, Law, Michael R, additional, Cheng, Lucy, additional, Abramowitz, Sharon, additional, Alcayna-Stevens, Lys, additional, Lurton, Grégoire, additional, Mayaka, Serge Manitu, additional, Olekhnovitch, Romain, additional, Kyomba, Gabriel, additional, Ruton, Hinda, additional, Ramazani, Sylvain Yuma, additional, and Grépin, Karen A, additional

Published
2020
Full Text
View/download PDF

19. Impact of a Free Health Care Policy in the Democratic Republic of the Congo During an Ebola Outbreak: An Interrupted Time-Series Analysis

Author

Hung, Yuen W., primary, Law, Michael R., additional, Cheng, Lucy, additional, Abramowitz, Sharon, additional, Alcayna-Stevens, Lys, additional, Lurton, Grégoire, additional, Mayaka, Serge M., additional, Olekhnovitch, Romain, additional, Kyomba, Gabriel, additional, Ruton, Hinda, additional, Ramazani, Sylvain Yuma, additional, and Grepin, Karen, additional

Published
2019
Full Text
View/download PDF

21. Scaling up early infant diagnosis of HIV in Rwanda, 2008–2010

Author

Cameron T Nutt, Placidie Mugwaneza, Ange Anitha Irakoze, Elena Chopyak, Peter Drobac, Corine Karema, Agnes Binagwaho, Lucinda B. Leung, Mawuena Agbonyitor, Anita Ahayo, Sachini Bandara, Sabin Nsanzimana, Alphonse Rukundo, Mary C. Smith Fawzi, Claire M. Wagner, and Ruton Hinda

Subjects
education.field_of_study, medicine.medical_specialty, Capacity Building, Public health law, business.industry, Health Policy, Public health, Population, Infant, Newborn, Rwanda, Public Health, Environmental and Occupational Health, AIDS Serodiagnosis, International health, HIV Infections, Infant, Newborn, Diseases, Infectious Disease Transmission, Vertical, Health facility, Environmental health, Humans, Medicine, Sample collection, Health care reform, education, business, Health policy
Abstract

More than 390,000 children are newly infected with HIV each year, only 28 per cent of whom benefit from early infant diagnosis (EID). Rwanda's Ministry of Health identified several major challenges hindering EID scale-up in care of HIV-positive infants. It found poor counseling and follow-up by caregivers of HIV-exposed infants, lack of coordination with maternal and child health-care programs, and long delays between the collection of samples and return of results to the health facility and caregiver. By increasing geographic access, integrating EID with vaccination programs, and investing in a robust mobile phone reporting system, Rwanda increased population coverage of EID from approximately 28 to 72.4 per cent (and to 90.3 per cent within the prevention of mother to child transmission program) between 2008 and 2011. Turnaround time from sample collection to receipt of results at the originating health facility was reduced from 144 to 20 days. Rwanda rapidly scaled up and improved its EID program, but challenges persist for linking infected infants to care.

Published
2012
Full Text
View/download PDF

22. HIV Prevalence Comparison Between Antenatal Sentinel Surveillance and Demographic and Health Survey in Rwanda

Author

Raphael Bitera, Jean Philippe Gatarayiha, Ruton Hinda, Jeanne Françoise Kayibanda, Bassirou Chitou, Adeline Kabeja, Michel Alary, and Louis Munyakazi

Subjects
Pediatrics, medicine.medical_specialty, education.field_of_study, demographic and health survey, business.industry, Population, Rwanda, Public Health, Environmental and Occupational Health, sentinel surveillance, Hiv prevalence, Article, HIV prevalence, Infectious Diseases, Virology, Medicine, Health survey, Marital status, Rural area, business, education, Demography
Abstract

Objective: To compare HIV prevalence from antenatal surveillance to that of the demographic and health survey (DHS), and to identify factors determining the difference of HIV prevalence between women recruited in these two surveys in Rwanda in 2005. Methods: Comparative cross-sectional study of HIV prevalence and socio-demographic factors collected by the antenatal survey in 13,745 pregnant women, seen in 30 health centres located throughout the country and those collected by the DHS among 5641 women, aged 15-49 years living in households located throughout the country. Log-binomial regression and direct standardization were used to estimate and compare HIV prevalence between the two surveys. Results: HIV prevalence in the antenatal survey was slightly higher than that in DHS women (4.1% versus 3.6% p=0.103). Socio-demographic characteristics were differently distributed between the two populations. Whereas, 59%, 93%, 53% of pregnant women were aged 20-29 years, married or cohabiting and living in rural areas respectively, the corresponding proportions among DHS women were 35%, 48% and 83% (p

Published
2011
Full Text
View/download PDF

23. Latent Tuberculosis Infection and Associated Factors among Health Care Workers in Kigali, Rwanda

Author

Michel Gasana, Chitou Bassirou, Grace Mutembayire, David W. Lowrance, John E. Oeltmann, Claude Bernard Uwizeye, Steve Gutreuter, Matthew Willis, Ruton Hinda, and Claude Rutanga

Subjects
Adult, Male, medicine.medical_specialty, Pediatrics, Tuberculosis, Referral, Health Personnel, education, Tuberculin, lcsh:Medicine, Natural history of disease, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Catchment Area, Health, Latent Tuberculosis, Risk Factors, Health care, Odds Ratio, medicine, Humans, Infection control, 030212 general & internal medicine, lcsh:Science, Aged, History of tuberculosis, 0303 health sciences, Schools, Multidisciplinary, Latent tuberculosis, Tuberculin Test, 030306 microbiology, business.industry, lcsh:R, Rwanda, 1. No poverty, Middle Aged, medicine.disease, bacterial infections and mycoses, 3. Good health, Family medicine, Female, lcsh:Q, Health Facilities, business, Research Article
Abstract

Introduction Data are limited regarding tuberculosis (TB) and latent TB infection prevalence in Rwandan health facilities. Methods We conducted a cross-sectional survey among healthcare workers (HCWs) in Kigali during 2010. We purposively selected the public referral hospital, both district hospitals, and randomly selected 7 of 17 health centers. School workers (SWs) from the nearest willing public schools served as a local reference group. We tested for latent TB infection (LTBI) using tuberculin skin testing (TST) and asked about past TB disease. We assessed risk of LTBI and past history of TB disease associated with hospital employment. Among HCWs, we assessed risk associated with facility type (district hospital, referral hospital, health center), work setting (inpatient, outpatient), and occupation. Results Age, gender, and HIV status was similar between the enrolled 1,131 HCWs and 381 SWs. LTBI was more prevalent among HCWs (62%) than SWs (39%). Adjusted odds of a positive TST result were 2.71 (95% CI 2.01–3.67) times greater among HCWs than SWs. Among HCWs, there was no detectable difference between prevalence of LTBI according to facility type, work setting, or occupation. Conclusion HCWs are at greater risk of LTBI, regardless of facility type, work setting, or occupation. The current status of TB infection control practices should be evaluated in the entire workforce in all Rwandan healthcare facilities.

Published
2015

25. Shared learning in an interconnected world: innovations to advance global health equity

Author

Massachusetts Institute of Technology. Department of Mechanical Engineering, Zurovcik, Danielle R., Binagwaho, Agnes, Nutt, Cameron T., Mutabazi, Vincent, Karema, Corine, Nsanzimana, Sabin, Gasana, Michel, Drobac, Peter C., Rich, Michael L., Uwaliraye, Parfait, Nyemazi, Jean Pierre, Murphy, Michael R., Wagner, Claire M., Makaka, Andrew, Ruton, Hinda, Mody, Gita N., Niconchuk, Jonathan A., Mugeni, Cathy, Ngabo, Fidele, Ngirabega, Jean de Dieu, Asiimwe, Anita, Farmer, Paul E., Massachusetts Institute of Technology. Department of Mechanical Engineering, Zurovcik, Danielle R., Binagwaho, Agnes, Nutt, Cameron T., Mutabazi, Vincent, Karema, Corine, Nsanzimana, Sabin, Gasana, Michel, Drobac, Peter C., Rich, Michael L., Uwaliraye, Parfait, Nyemazi, Jean Pierre, Murphy, Michael R., Wagner, Claire M., Makaka, Andrew, Ruton, Hinda, Mody, Gita N., Niconchuk, Jonathan A., Mugeni, Cathy, Ngabo, Fidele, Ngirabega, Jean de Dieu, Asiimwe, Anita, and Farmer, Paul E.

Abstract

The notion of "reverse innovation";--that some insights from low-income countries might offer transferable lessons for wealthier contexts--is increasingly common in the global health and business strategy literature. Yet the perspectives of researchers and policymakers in settings where these innovations are developed have been largely absent from the discussion to date. In this Commentary, we present examples of programmatic, technological, and research-based innovations from Rwanda, and offer reflections on how the global health community might leverage innovative partnerships for shared learning and improved health outcomes in all countries.

Published
2013

26. Shared learning in an interconnected world: innovations to advance global health equity

Author

Binagwaho, Agnes, primary, Nutt, Cameron T, additional, Mutabazi, Vincent, additional, Karema, Corine, additional, Nsanzimana, Sabin, additional, Gasana, Michel, additional, Drobac, Peter C, additional, Rich, Michael L, additional, Uwaliraye, Parfait, additional, Nyemazi, Jean, additional, Murphy, Michael R, additional, Wagner, Claire M, additional, Makaka, Andrew, additional, Ruton, Hinda, additional, Mody, Gita N, additional, Zurovcik, Danielle R, additional, Niconchuk, Jonathan A, additional, Mugeni, Cathy, additional, Ngabo, Fidele, additional, Ngirabega, Jean de Dieu, additional, Asiimwe, Anita, additional, and Farmer, Paul E, additional

Published
2013
Full Text
View/download PDF

27. Cell Phone-Based and Internet-Based Monitoring and Evaluation of the National Antiretroviral Treatment Program During Rapid Scale-Up in Rwanda

Author

Nsanzimana, Sabin, primary, Ruton, Hinda, additional, Lowrance, David W., additional, Cishahayo, Shabani, additional, Nyemazi, Jean Pierre, additional, Muhayimpundu, Ribakare, additional, Karema, Corine, additional, Raghunathan, Pratima L., additional, Binagwaho, Agnes, additional, and Riedel, David J., additional

Published
2012
Full Text
View/download PDF

28. Estimation of the size of the female sex worker population in Rwanda using three different methods.

Author

Mutagoma, Mwumvaneza, Kayitesi, Catherine, Gwiza, Aimé, Ruton, Hinda, Koleros, Andrew, Gupta, Neil, Balisanga, Helene, Riedel, David J, and Nsanzimana, Sabin

Subjects
HIV prevention, POPULATION density, SEX work
Abstract

HIV prevalence is disproportionately high among female sex workers compared to the general population. Many African countries lack useful data on the size of female sex worker populations to inform national HIV programmes. A female sex worker size estimation exercise using three different venue-based methodologies was conducted among female sex workers in all provinces of Rwanda in August 2010. The female sex worker national population size was estimated using capture-recapture and enumeration methods, and the multiplier method was used to estimate the size of the female sex worker population in Kigali. A structured questionnaire was also used to supplement the data. The estimated number of female sex workers by the capture-recapture method was 3205 (95% confidence interval: 2998-3412). The female sex worker size was estimated at 3348 using the enumeration method. In Kigali, the female sex worker size was estimated at 2253 (95% confidence interval: 1916-2524) using the multiplier method. Nearly 80% of all female sex workers in Rwanda were found to be based in the capital, Kigali. This study provided a first-time estimate of the female sex worker population size in Rwanda using capture-recapture, enumeration, and multiplier methods. The capture-recapture and enumeration methods provided similar estimates of female sex worker in Rwanda. Combination of such size estimation methods is feasible and productive in low-resource settings and should be considered vital to inform national HIV programmes. [ABSTRACT FROM AUTHOR]

Published
2015
Full Text
View/download PDF

29. Under-two child mortality according to maternal HIV status in Rwanda: assessing outcomes within the National PMTCT Program.

Author

Mugwaneza, Placidie, Shema, Nadine Umutoni Wa, Ruton, Hinda, Rukundo, Alphonse, Lyambabaje, Alexandre, de Dieu Bizimana, Jean, Tsague, Landry, Wagner, Claire M., Nyankesha, Elévanie, Muita, Jane, Mutabazi, Vincent, Nyemazi, Jean Pierre, Nsanzimana, Sabin, Karema, Corine, and Binagwaho, Agnes

Abstract

Introduction: We sought to compare risk of death among children aged under-2 years born to HIV positive mother (HIV-exposed) and to HIV negative mother (HIV non-exposed), and identify determinants of under-2 mortality among the two groups in Rwanda. Methods: In a stratified, two-stage cluster sampling design, we selected mother-child pairs using national Antenatal Care (ANC) registers. Household interview with each mother was conducted to capture socio-demographic data and information related to pregnancy, delivery and post-partum. Data were censored at the date of child death. Using Cox proportional hazard model, we compared the hazard of death among HIV-exposed children and HIV nonexposed children. Results: Of 1,455 HIV-exposed children, 29 (2.0%; 95% CI: 1.3%-2.7%) died by 6 months compared to 18 children of the 1,565 HIV non-exposed children (1.2%; 95% CI: 0.6%-1.7%). By 9 months, cumulative risks of death were 3.0% (95%; CI: 2.2%-3.9%) and 1.3% (96%; CI: 0.7%-1.8%) among HIV-exposed and HIV non-exposed children, respectively. By 2 years, the hazard of death among HIVexposed children was more than 3 times higher (aHR:3.5; 95% CI: 1.8-6.9) among HIV-exposed versus non-exposed children. Risk of death by 9- 24 months of age was 50% lower among mothers who attended 4 or more antenatal care (ANC) visits (aHR: 0.5, 95% CI: 0.3-0.9), and 26% lower among families who had more assets (aHR: 0.7, 95% CI: 0.5-1.0). Conclusion: Infant mortality was independent of perinatal HIV exposure among children by 6 months of age. However, HIV-exposed children were 3.5 times more likely to die by 2 years. Fewer antenatal visits, lower household assets and maternal HIV seropositive status were associated with increased mortality by 9-24 months. [ABSTRACT FROM AUTHOR]

Published
2011

30. A consensus statement on dual purpose pathogen surveillance systems: The always on approach.

Author

van der Westhuizen HM, Soundararajan S, Berry T, Agus D, Carmona S, Ma P, Davis J, Walker S, Mokaya J, Bentley SD, Thomson NR, Silitoe J, Singer A, Hassan I, Mariano R, Akodu M, Seidman G, Sachedina N, Edgeworth J, Naidoo R, Makadzange T, Choi V, Gadde R, Scarpino SV, Bull C, Govender K, Ngongo B, Ruton H, Pronyk P, Smolina K, Li H, Barry D, Schaffer S, Moeder V, Gao G, Crook D, and Bell J

Abstract

Competing Interests: TB, JB, DC are current board members of the Global Pathogen Analysis Service Limited. DA and TM are previous board members of the Global Pathogen Analysis Service Limited. NS and JE are employed by Oxford Nanopore Technologies, where they also receive stock options. S Scarpino has options in Iliad biotechnologies. CB and KG were previously employed by the Global Pathogen Analysis Service Limited. BN is employed by Illumina Inc. where she also receives stock options. VM holds Illumina Inc stocks as a former employee. S Schaffer holds stock and stock options in Ilumina Inc and stock options in Hologic Inc. This does not alter our adherence to PLOS Global Public Health policies on sharing data and materials. HvdW, S Soundararajan, SC, PM, JD, DB, SW, JM, SB, NRT, JS, AS, IH, RM, MA, GS, RN, VC, RG, HR, PP, KS, HL and GG have no competing interests to declare. There are no patents products in development or marketed products associated with this research to declare.

Published
2024
Full Text
View/download PDF

31. Oral Fluvoxamine With Inhaled Budesonide for Treatment of Early-Onset COVID-19 : A Randomized Platform Trial.

Author

Reis G, Dos Santos Moreira Silva EA, Medeiros Silva DC, Thabane L, de Souza Campos VH, Ferreira TS, Quirino Dos Santos CV, Ribeiro Nogueira AM, Figueiredo Guimaraes Almeida AP, Cançado Monteiro Savassi L, de Figueiredo Neto AD, Bitarães C, Cruz Milagres A, Diniz Callegari E, Campos Simplicio MI, Barra Ribeiro L, Oliveira R, Harari O, Wilson LA, Forrest JI, Ruton H, Sprague S, McKay P, Guo CM, Guyatt GH, Rayner CR, Boulware DR, Ezer N, Lee TC, McDonald EG, Bafadhel M, Butler C, Rodrigues Silva J, Dybul M, and Mills EJ

Subjects
Adult, Humans, Budesonide adverse effects, Fluvoxamine, SARS-CoV-2, COVID-19 Drug Treatment, Treatment Outcome, COVID-19
Abstract

Background: Previous trials have demonstrated the effects of fluvoxamine alone and inhaled budesonide alone for prevention of disease progression among outpatients with COVID-19., Objective: To determine whether the combination of fluvoxamine and inhaled budesonide would increase treatment effects in a highly vaccinated population., Design: Randomized, placebo-controlled, adaptive platform trial. (ClinicalTrials.gov: NCT04727424)., Setting: 12 clinical sites in Brazil., Participants: Symptomatic adults with confirmed SARS-CoV-2 infection and a known risk factor for progression to severe disease., Intervention: Patients were randomly assigned to either fluvoxamine (100 mg twice daily for 10 days) plus inhaled budesonide (800 mcg twice daily for 10 days) or matching placebos., Measurements: The primary outcome was a composite of emergency setting retention for COVID-19 for more than 6 hours, hospitalization, and/or suspected complications due to clinical progression of COVID-19 within 28 days of randomization. Secondary outcomes included health care attendance (defined as hospitalization for any cause or emergency department visit lasting >6 hours), time to hospitalization, mortality, patient-reported outcomes, and adverse drug reactions., Results: Randomization occurred from 15 January to 6 July 2022. A total of 738 participants were allocated to oral fluvoxamine plus inhaled budesonide, and 738 received placebo. The proportion of patients observed in an emergency setting for COVID-19 for more than 6 hours or hospitalized due to COVID-19 was lower in the treatment group than the placebo group (1.8% [95% credible interval {CrI}, 1.1% to 3.0%] vs. 3.7% [95% CrI, 2.5% to 5.3%]; relative risk, 0.50 [95% CrI, 0.25 to 0.92]), with a probability of superiority of 98.7%. No relative effects were found between groups for any of the secondary outcomes. More adverse events occurred in the intervention group than the placebo group, but no important differences between the groups were detected., Limitation: Low event rate overall, consistent with contemporary trials in vaccinated populations., Conclusion: Treatment with oral fluvoxamine plus inhaled budesonide among high-risk outpatients with early COVID-19 reduced the incidence of severe disease requiring advanced care., Primary Funding Source: Latona Foundation, FastGrants, and Rainwater Charitable Foundation., Competing Interests: Disclosures: Disclosures can be viewed at www.acponline.org/authors/icmje/ConflictOfInterestForms.do?msNum=M22-3305.

Published
2023
Full Text
View/download PDF

32. Cell phone-based and internet-based monitoring and evaluation of the National Antiretroviral Treatment Program during rapid scale-up in Rwanda: TRACnet, 2004-2010.

Author

Nsanzimana S, Ruton H, Lowrance DW, Cishahayo S, Nyemazi JP, Muhayimpundu R, Karema C, Raghunathan PL, Binagwaho A, and Riedel DJ

Subjects
Adolescent, Adult, Child, Child, Preschool, Data Collection methods, Female, Humans, Male, Middle Aged, Population Surveillance methods, Rwanda, Young Adult, Anti-Retroviral Agents therapeutic use, Cell Phone, HIV Infections drug therapy, Internet, Program Evaluation methods
Abstract

Background: Monitoring and evaluation of antiretroviral treatment (ART) scale-up has been challenging in resource-limited settings. We describe an innovative cell-phone-based and internet-based reporting system (TRACnet) utilized in Rwanda., Methods: From January 2004 to June 30, 2010, all health facilities with ART services submitted standardized monthly aggregate reports of key indicators. National cohort data were analyzed to examine trends in characteristics of patients initiating ART and cumulative cohort outcomes. Estimates of HIV-infected patients eligible for ART were obtained from Joint United Nations Program on HIV/AIDS (Estimation and Projection Package-Spectrum, 2010)., Results: By June 30, 2010, 295 (65%) of 451 health centers, District and referral hospitals provided ART services; of these, 255 (86%) were located outside Kigali, the capital. Cell phone-based and internet-based reporting was used by 253 (86%) and 42 (14%), respectively. As of June 30, 2010, 83,041 patients were alive on ART, 6171 (6%) had died, and 9621 (10%) were lost-to-follow-up. Of those alive on ART, 7111 (8.6%) were children, 50,971 (61.4%) were female, and 1823 (2.2%) were on a second-line regimen. The proportion of all patients initiating ART at World Health Organization clinical stages 3 and 4 declined from 65% in 2005 to 27% in 2010. National ART coverage of eligible patients increased from 13% in 2005 to 79% in 2010., Conclusions: Rwanda has successfully expanded ART access and achieved high national ART coverage among eligible patients. TRACnet captured essential data about the ART program during rapid scale-up. Cell phone-based and internet-based reporting may be useful for monitoring and evaluation of similar public health initiatives in other resource-limited settings.

Published
2012
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results