Feasibility and impact of near-point-of-care integrated tuberculosis/HIV testing in Malawi and Zimbabwe

被引:6
作者
Wang, Melody [1 ]
Boeke, Caroline E. [1 ]
Rioja, Maria Rosezoil [1 ]
Maparo, Tatenda [2 ]
Banda, Clement [3 ]
Chavula, Chancy [3 ]
Gunda, Andrews [3 ]
Isaac, Jean [3 ]
Mangwiro, Alexio [2 ]
Mangwendeza, Phibeon Munyaradzi [2 ]
Mtaula, Jonathan [3 ]
Mwase, Christopher [3 ]
Doi, Naoko [1 ]
Peter, Trevor [1 ]
Kandulu, James [4 ]
Simbi, Raiva [5 ]
Khan, Shaukat [1 ]
Sacks, Jilian A. [1 ]
机构
[1] Clinton Hlth Access Initiat, Boston, MA USA
[2] Clinton Hlth Access Initiat, Harare, Zimbabwe
[3] Clinton Hlth Access Initiat, Lilongwe, Malawi
[4] Minist Hlth & Populat, Lilongwe, Malawi
[5] Minist Hlth & Child Care, Harare, Zimbabwe
关键词
GeneXpert; HIV care continuum; integrated testing; point of care; tuberculosis; testing; HIV VIRAL LOAD; SAHARAN AFRICAN COUNTRIES; SCALE-UP; DIAGNOSIS;
D O I
10.1097/QAD.0000000000003031
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Objectives: Near-point-of-care (POC) testing for early infant diagnosis (EID) and viral load expedites clinical action and improves outcomes but requires capital investment. We assessed whether excess capacity on existing near-POC devices used for TB diagnosis could be leveraged to increase near-POC HIV molecular testing, termed integrated testing, without compromising TB services. Design: Preimplementation/postimplementation studies in 10 health facilities in Malawi and 8 in Zimbabwe. Methods: Timeliness of EID and viral load test results and clinical action were compared between centralized and near-POC testing using Somers' D tests (continuous indicators) and risk ratios (RR, binary indicators); TB testing/treatment rates and timeliness were analyzed preintegration/postintegration. Results: With integration, average device utilization increased but did not exceed 55%. Despite the addition of HIV testing, TB test volumes, timeliness, and treatment initiations were maintained. Although few HIV-positive infants were identified, near-POC EID testing improved treatment initiation within 1 month by 57% compared with centralized EID [Malawi RR: 1.57, 95% confidence interval (CI) 0.98-2.52], and near-POC viral load testing significantly increased the proportion of patients with elevated viral load receiving clinical action within 1 month (Zimbabwe RR: 5.26, 95% CI 3.38-8.20; Malawi RR: 3.90, 95% CI 2.58-5.91). Conclusion: Integrating TB/HIV testing using existing multidisease platforms is feasible and enables increased access to rapid diagnostics without disrupting existing TB services. Our results serve as an example of a novel, efficient implementation model that can increase access to critical testing services across disease silos and should be considered for additional clinical applications.
引用
收藏
页码:2531 / 2537
页数:7
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