Abstract

Recently, the prices of antiretroviral drugs have dropped dramatically, low cost generic drugs have become available, and further lowering of the price of patented drugs is anticipated thus paving the way for greater access to antiretroviral therapy for treatment of HIV disease in resource-constrained settings where the need is greatest. Hence there is a need to urgently develop innovative strategies to provide antiretroviral therapy safely, effectively and with high levels of adherence in the context of under- developed health care delivery systems. This CAPRISA project proposes the strategy of linking antiretroviral therapy to the widely available, affordable and sustainable tuberculosis directly observed therapy strategy. It proposes that such a strategy, by addressing issues of therapeutic potency and adherence, will enhance therapeutic outcome for both diseases. A once a day regimen of didanosine (ddl), lamivudine (3TC) and efavirenz will be used in combination with conventional anti-tuberculosis therapy. Since tuberculosis is the commonest presenting illness in AIDS patients in much of the developing world, the integration of HIV and tuberculosis care is an efficient method of identifying those in greatest need of antiretroviral therapy. Eligible patients, who are co-infected with HIV and tuberculosis, will be randomized to either the intervention arm, where both antituberculosis and antiretroviral drugs are provided through directly observed therapy with an enhanced adherence intervention, or the control arm where they receive anti-tuberculosis treatment through the existing directly observed therapy program. Upon completion of tuberculosis therapy at 6 months, the patients in both study arms are provided ongoing HIV care, which includes self-administered anti-retroviral therapy, at an AIDS clinic at a local hospital. The primary endpoint is the case fatality rate at 18 months after the diagnosis of the tuberculosis-HIV co-infection. The secondary outcomes include the impact of the intervention on the patient's clinical status, viral load, CD4 count, drug adherence, drug resistance, tuberculosis cure rates, tuberculosis relapse rates and drug adverse events. The findings of this study could have a major impact in resource-constrained settings with existing tuberculosis directly observed therapy programs, as it would provide an affordable and effective strategy for the successful implementation of antiretroviral therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program--Cooperative Agreements (U19)
Project #
1U19AI051794-01
Application #
6547956
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2002-01-01
Project End
2006-12-31
Budget Start
Budget End
Support Year
1
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of Kwazulu-Natal
Department
Type
DUNS #
637360244
City
Durban
State
Country
South Africa
Zip Code
3630

  Publications

Sheward, Daniel J; Marais, Jinny; Bekker, Valerie et al. (2018) HIV Superinfection Drives De Novo Antibody Responses and Not Neutralization Breadth. Cell Host Microbe 24:593-599.e3
Johnson, Erik L; Doria-Rose, Nicole A; Gorman, Jason et al. (2018) Sequencing HIV-neutralizing antibody exons and introns reveals detailed aspects of lineage maturation. Nat Commun 9:4136
Garrett, Nigel; Norman, Emily; Leask, Kerry et al. (2018) Acceptability of Early Antiretroviral Therapy Among South African Women. AIDS Behav 22:1018-1024
Setliff, Ian; McDonnell, Wyatt J; Raju, Nagarajan et al. (2018) Multi-Donor Longitudinal Antibody Repertoire Sequencing Reveals the Existence of Public Antibody Clonotypes in HIV-1 Infection. Cell Host Microbe 23:845-854.e6
Harichund, Charlene; Moshabela, M (2018) Acceptability of HIV Self-Testing in Sub-Saharan Africa: Scoping Study. AIDS Behav 22:560-568
Naidoo, Kogieleum; Yende-Zuma, Nonhlanhla; Augustine, Stanton (2018) A retrospective cohort study of body mass index and survival in HIV infected patients with and without TB co-infection. Infect Dis Poverty 7:35
Moosa, Yumna; Tanko, Ramla F; Ramsuran, Veron et al. (2018) Case report: mechanisms of HIV elite control in two African women. BMC Infect Dis 18:54
Selhorst, Philippe; Masson, Lindi; Ismail, Sherazaan D et al. (2017) Cervicovaginal Inflammation Facilitates Acquisition of Less Infectious HIV Variants. Clin Infect Dis 64:79-82
Scheepers, Cathrine; Chowdhury, Sudipa; Wright, W Shea et al. (2017) Serum glycan-binding IgG antibodies in HIV-1 infection and during the development of broadly neutralizing responses. AIDS 31:2199-2209
Ngandu, Nobubelo K; Carlson, Jonathan M; Chopera, Denis R et al. (2017) Brief Report: Selection of HIV-1 Variants With Higher Transmission Potential by 1% Tenofovir Gel Microbicide. J Acquir Immune Defic Syndr 76:43-47

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