Impact of tuberculosis screening and isoniazid preventive therapy on incidence of TB and death in the TB/HIV in Rio de Janeiro (THRio) study B. Durovni1,2,

Slides:

Advertisements

Similar presentations

AIDS-Related Tuberculosis in Rio de Janeiro, Brazil Antonio G F Pacheco.

Advertisements

Sponsored by NIH/NIAID/DAIDS Completed Observation of the Randomized Placebo-Controlled Phase of iPrEx with co-funding by the Bill & Melinda Gates Foundation.

Tuberculosis incidence and risk factors among adult patients receiving HAART in Senegal: a 7-year cohort study Assane DIOUF et al. IRD/UMR 145 CRCF, CHNU.

Risk factors and true outcomes of children lost to follow-up from antiretroviral therapy in Lilongwe, Malawi C. Ardura Gracia, H. Tweya, C Feldacker, S.

High Rates of Tuberculosis in Patients Accessing HAART in Rural South Africa – Implications for HIV and TB Treatment Programs Kogieleum Naidoo on behalf.

Antiretroviral therapy eligibility at enrollment and time to treatment initiation in Ethiopia Chloe A. Teasdale 1, Chunhui Wang 1, Sileshi Lulseged 1,

Monica Gandhi MD, MPH Associate Professor and Women’s HIV Clinic provider, HIV/AIDS Division San Francisco General Hospital/ UCSF Safe Poz Love, U.S. Positive.

Mortality and causes of death among women living with HIV in the UK in the era of highly-active antiretroviral therapy Sara Croxford, A Kitching, M Kall,

The hidden HIV epidemic: what do mathematical models tell us? The case of France Virginie Supervie, Jacques Ndawinz & Dominique Costagliola U943 Inserm.

Most deaths among children enrolled in two program settings in Cambodia occur within the first 6 months after enrolment. Early mortality rates were more.

S AFETY OF I SONIAZID P REVENTIVE T HERAPY A MONG HIV- INFECTED P REGNANT W OMEN IN H IGH TB I NCIDENCE S ETTINGS : STUDY UPDATE OF IMPAACT P1078 (APPRISE)

The ninth Technical Advisory Group and National TB Managers meeting

HIV and STI Department - Centre for Infections Predictors of non-AIDS related death in a national cohort of HIV-diagnosed adults Meaghan Kall, Ruth Smith,

HIV Early Treatment Project Groups 1 and 2 n Among HIV-infected participants in sub-Saharan Africa, does initiation of antiretroviral treatment (ART) at.

Unit 5: IPT Isoniazid TB Preventive Therapy

Introduction DCDOH supports HIV test and treat activities - increased number of HIV tests performed, emphasis on earlier linkage to care. Limited data.

The Effect of Syphilis Co-infection on Clinical Outcomes in HIV-Infected Persons The Effect of Syphilis Co-infection on Clinical Outcomes in HIV-Infected.

Johns Hopkins Center for Tuberculosis Research

Isoniazid preventive therapy in a time of HIV, TB, and MDR.

Increased clinical events in HIV-infected patients who achieve full virologic suppression but fail to attain a CD4 count ≥ 200 cells/mm 3 after one year.

Max O’Donnell, Nesri Padayatchi, Iqubal Master, Garth Osburn, Robert Horsburgh Treatment of Extensively Drug Resistant Tuberculosis Among Patients with.

The Immunologic Efficacy of Antiretroviral Therapy among HIV-infected Patients in North America and Africa Elvin Geng* 1, Eric Vittinghoff 1, Jean Nachega.

Management and Development for Health (MDH)

HIV and STI Department, Health Protection Agency - Colindale HIV and AIDS Reporting System HIV in the United Kingdom: 2012 Overview.

6 th Biannual Joint HIV Sector Review Meeting Nov 11-13,2014 Ministry of Health and Social Welfare Mwanaisha Nyamkara, NTLP Werner Maokola, NACP Nov 11,

Laura Mucci, Pharm.D. Candidate Mercer University 2012 Preceptor: Dr. Rahimi February 2012.

Impact of Highly Active Antiretroviral Therapy on the Incidence of HIV- encephalopathy among perinatally- infected children and adolescents. Kunjal Patel,

Life expectancy of patients treated with ART in the UK: UK CHIC Study Margaret May University of Bristol, Department of Social Medicine, Bristol.

Neurocognitive Impairment in HIV-Infected Subjects on HAART: Prevalence and Associations Kevin Robertson *1, Kunling Wu 2, Thomas Parsons 1, Ron Ellis.

David Dowdy, Elvin Geng, Katerina Christopoulos, James Kahn, C. Bradley Hare, Daniel Wlodarczyk, Diane Havlir Internal Medicine Residency Program, UCSF.

TB-HIV INTEGRATION IN THE WORKPLACE 2 nd Private Sector Conference on HIV and AIDS Presenter: Dr S Charalambous.

TREATMENT OF SERO-DISCORDANT COUPLES: IMPLICATIONS FOR YOUNG PEOPLE JJ KUMWENDA (FRCP-UK)

CREATE Biostatistics Core THRio Statistical Considerations Analysis Plan.

The effect of tuberculosis treatment on virologic and immunologic response to combination antiretroviral therapy among South African children Heidi M.

THRio Antonio G F Pacheco. THRioOutline –Database setup Creating a master table with main outcomes –Mortality recovery with linkage Issues and differences.

Lecture 9: Analysis of intervention studies Randomized trial - categorical outcome Measures of risk: –incidence rate of an adverse event (death, etc) It.

Effect of community-wide isoniazid preventive therapy on tuberculosis among South African gold miners “Thibelo TB” Aurum Health Research LSHTM JHU Gold.

CREATE Biostatistics Core Functions Summary of activities Challenges / coming year’s activities.

Scale up TB/HIV activities in Asia Pacific 8-9Aug09 1 TB/HIV collaborative activities in Thailand Sriprapa Nateniyom, M.D. TB Bureau, Department of Disease.

AN INTERNATIONAL MULTI-CENTRE, RANDOMISED, DOUBLE- BLIND, PLACEBO-CONTROLLED TRIAL TO EVALUATE THE EFFICACY AND SAFETY OF 0.5% AND 2% PRO 2000 GELS FOR.

THE 6 TH NATIONAL SCIENTIFIC CONFERENCE ON HIV/AIDS Yield and impact of repeated screening for tuberculosis and isoniazid preventive therapy among patients.

CREATE Biostatistics Core THRio Statistical Considerations Analysis of baseline data—esp. truncation Analysis of main study data—esp. correlation.

Strategies for Management of Antiretroviral Therapy Study Wafaa El-Sadr and James Neaton for the SMART Study Team.

HIV Testing in Acute Care Settings Rich Rothman, MD, PhD, FACEP CDC, DHHS, OraSure Technologies, Abbott  Historical.

Long-Term Comparison of Nevirapine Versus Efavirenz When Combined with Other Antiretroviral Drugs in HIV-1 Positive Antiretroviral-Naïve Persons- The NNRTI.

Figure 2: Trends in currently prescribed antiretroviral therapy % prescribed HAART increased from 74% to 83% Trends in ART use, HIV viral load, and CD4.

Tuberculosis and HIV-AIDS: Achievements with ARV access Dr. Humberto Costa, MD Minister of Health, Brazil.

Estimating the population impact of homelessness on HIV viral suppression among people who use drugs Brandon DL Marshall, 1 Beth Elson, 1 Sabina Dobrer,

Paz Bailey G 1, Sternberg M 1, Puren AJ 2, Markowitz LE 1, Ballard R 1, Delany S 3, Hawkes S 4, Nwanyanwu O 1, Ryan C 1, and Lewis DA 5 1. NCHHSTP, CDC.

Effect of ART on malaria parasitaemia and clinical episodes in adults in rural Uganda: A population-based cohort study Billy N. Mayanja 1, Kathy Baisley.

Acute Renal Failure in HIV- Infected Individuals Greatly Increases Risk for In-Hospital Mortality Slideset on: Wyatt CM, Arons RR, Klotman PE, Klotman.

HAART Initiation Within 2 Weeks of Seroconversion Associated With Virologic and Immunologic Benefits Slideset on: Hecht FM, Wang L, Collier A, et al. A.

CD4 trajectory among HIV positive patients receiving HAART in a large East African HIV care centre Agnes N. Kiragga 1, Beverly Musick 2 Ronald Bosch, Ann.

Efavirenz Use Not Associated With Depressive Episodes, According to Analysis of Randomized Clinical Trial Outcomes Slideset on: Journot V, Chene G, De.

Successfully enrolled in HIV Care but not linked to timely Treatment: Poor retention and Monitoring of Pre-ART patients who are not yet eligible for ART.

Slideset on: Emery S, Neuhaus JA, Phillips AN, et al. Major clinical outcomes in antiretroviral therapy (ART)-naive participants and in those not receiving.

SAFETY AND EFFICACY OF MVA85A, A NEW TUBERCULOSIS VACCINE, IN INFANTS PREVIOUSLY VACCINATED WITH BCG: A RANDOMISED, PLACEBO-CONTROLLED PHASE 2B TRIAL Michele.

First-Line Treatment of HIV Infection With Either NNRTI- or PI-Based Regimens Effective for Long-term Disease Control Slideset on: MacArthur RD, Novak.

Randomized clinical trial to determine efficacy and safety of antiretroviral therapy one week after tuberculosis therapy in patients with CD4 counts

Incidence of tuberculosis in the first year of antiretroviral treatment in West-African HIV-infected adults B. Tchakounte Youngui1, P. Coffie2, E. Messou3,

Participants 18year old+

Dr. Velephi Okello, Principal Investigator, MaxART Trial

Dorina Onoya1, Tembeka Sineke1, Alana Brennan1,2, Matt Fox1,2

Tolerability of Isoniazid Preventive therapy Among HIV infected Cohort in Nigeria Folajinmi Oluwasina Strategic Information Unit AIDS Healthcare Foundation,

C R E A E Consortium to Respond Effectively to the AIDS-TB Epidemic

Management and Development for Health (MDH)

Kevin M De Cock MD CDC Kenya Nairobi, September 21, 2003

Surveillance for TB in HIV Care and Treatment Settings (CTS)

Melissa Herrin, Jan Tate ScD, MPH & Amy Justice, MD, PhD

Collaborative TB/HIV activities 2011 Tables, Graphs & Maps

Presentation transcript:

Impact of tuberculosis screening and isoniazid preventive therapy on incidence of TB and death in the TB/HIV in Rio de Janeiro (THRio) study B. Durovni1,2, V. Saraceni1, A. Pacheco3, S. Cavalcante1,3, S. Cohn4, B. King4, L. Moulton4, R. Chaisson4, J. Golub4, THRio study group 1Rio de Janeiro City Health Secretariat, Rio de Janeiro, Brazil, 2Federal University of Rio de Janeiro, Rio de Janeiro, Brazil, 3Fiocruz, Rio de Janeiro, Brazil, 4Johns Hopkins University, Baltimore, United States

THRio Objectives To determine if implementation of a policy of widespread use of isoniazid preventive therapy (IPT) in HIV-infected patients with access to ARV therapy reduces the incidence of active TB and death in the HIV clinic population Scale up of tuberculin skin testing (TST) and IPT among HIV-infected patients in public primary health units in Rio de Janeiro within the current HIV clinic infrastructure In an effort to reduce: TB Incidence Mortality

Setting 29 Public Health units managed by the Health Department of Rio de Janeiro City AP5.3 AP5.2 AP4 AP5.1 AP3.3 AP3.2 AP1 AP3.1 AP 2.1 AP2.2 3

THRio Study Design and Timeline Cluster-Randomized, Step-Wedge Trial Sep 05 Jan 08 48 60 Aug 09 Intervention and Follow-up Period (for all clinics) 4

Intervention Training clinics to properly implement TB screening and adhere to TST/IPT policy for all HIV-infected patients TST to be done for all eligible clinic patients No prior TB history No prior IPT No prior +TST IPT x 6 months for all TST+ without active TB and all contacts of active TB cases 5

TST and IPT 69% had at least one TST placed and read 83% started IPT 0.84% had an adverse event 84% completed IPT

Time to TST and Time to IPT Before and After THRio Intervention Time to TST and time to IPT are both markedly improved post-intervention Durovni et al., AIDS 2010, 24 (suppl 5):S49–S56

Methods for Current Analysis Primary endpoints: Incidence of TB and TB or death at the clinic level before and after the intervention Eligible patients who made > 1 visit after 1 Sept 2003 ‘Eligible’ = no prior TB or IPT ‘Prevalent’ TB and deaths (within 60 days of enrollment) excluded Patients remain in the denominator until TB or Death Intent-to-treat Analysis – includes all eligibles “Stayers” Analysis -- among those remaining in clinic contact, censoring those missing for >1 year (mITT) Statistical analysis: Crude hazard ratios (HR) obtained from frailty-adjusted Cox models are presented

CONSORT Diagram (modified for stepped wedge cluster-randomized trial) Clinics Eligible for Inclusion (n=29) Clinics Receiving Intervention (n=29) Patients in Clinics Eligible for Intervention (n=12,815) Eligible patients contributing to control phase (n=9,853 ) Eligible patients contributing to intervention phase (n= 10,840) Patients in Clinics Ineligible for Intervention (n=4,480)

THRio cohort characteristics (n=12,815) Median age: 37 years old Male: 61% Median years since HIV diagnosis: 2.4 years HAART at entry: 60% Median CD4 cell count at entry: 403 cells/mm3

Incidence of TB Over Time X: start of intervention | : control case | : intervention case

THRio Results TB cases, total contribution time, incidence per 100pyrs Control Phase Intervention Phase Cases 221 254 Person years 16,834 23,126 Rate/100pyrs 1.31 1.10 TB/Death cases, total contribution time, incidence per 100pyrs Control Phase Intervention Phase Cases 617 696 Person years 16,834 23,126 Rate/100pyrs 3.67 3.01

THRio Results: Unadjusted Cox Models Outcome Cases HR (95% CI) p-value Intent To Treat TB 475 0.87 (0.68-1.10) 0.233 TB or Death 1313 0.72 (0.62-0.82) <0.001 Intent-to-treat – Among all eligibles

THRio Results: Unadjusted Cox Models Outcome Cases HR (95% CI) p-value Intent To Treat TB 475 0.87 (0.68-1.10) 0.233 TB or Death 1313 0.72 (0.62-0.82) <0.001 Modified To Treat (Stayers) 403 0.57 (0.44-0.76) TB or Death 1073 0.56 (0.47-0.66) Intent-to-treat – Among all eligibles Stayers – mITT - Among those remaining in clinic contact (Patients censored at the moment they go one year without a clinic contact)

Conclusions Overall, the THRio intervention had a modest impact (13% reduction) on TB, but showed an important and statistically significant impact on TB and death (28% reduction) in the primary intent-to-treat analysis; The “Stayers” analysis, including those who were more likely to be exposed to the intervention (mITT), showed an even larger and highly significant impact on reduction of TB incidence (43%) and TB incidence and death (44%) TST screening and provision of IPT to HIV-infected patients with access to highly active antiretroviral therapy significantly reduces the risk of TB and death and should be widely implemented

THRio Study Team Rio de Janeiro Betina Durovni Solange Cavalcante Valeria Saraceni Antonio Pacheco Giselle Israel Vitoria Vellozo Rita Ferreira Lilian Lauria THRio Study Team JHU Richard Chaisson Jonathan Golub Larry Moulton Silvia Cohn Bonnie King Anne Efron Susan Dorman THRio Study Team Funding: Bill and Melinda Gates Foundation