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Renal function of MDR-TB patients treated with kanamycin regimens or concomitantly with antiretroviral agents

Author: Leufkens H. G.M.
Mantel-Teeuwisse A. K.
Mavhunga Farai
Mekonen T. T.
Mengistu A.
Rennie Timothy
Ruswa N.
Sagwa E. L.
Publication venue
Publication date: 01/12/2017
Field of study

SETTING: To compare renal insufficiency among mul-tidrug-resistant tuberculosis (MDR-TB) patients treated with kanamycin (KM) based regimens and those treated concomitantly with tenofovir disoproxil fumarate (TDF) or other antiretroviral therapy (ART) regimens in Namibia. DESIGN: Retrospective review of the treatment records and laboratory tests of patients initiated on MDR-TB treatment (January–December 2014). The glomerular filtration rates (eGFR) estimated pre- and post-treatment were compared using the analysis of variance test. Renal insufficiency was defined as an eGFR of,60 ml/ min/1.73 m2. Use of KM or TDF and association with renal insufficiency was assessed using Kaplan-Meier plots and Cox proportional hazards analysis. RESULTS: The baseline mean eGFR for the three groups was similar (P ¼ 0.24): 139.3 6 25.6 ml/min for the KM group (n ¼ 68), 131.1 6 25.7 ml/min for the KMþTDF group (n ¼ 44) and 134.2634.4 ml/min for the KMþOther group (n ¼ 23). After 8 months, the values had declined significantly to respectively 104.8 6 37.5 ml/min (P, 0.001), 101.5 6 38.3 ml/min (P, 0.001) and 111.5 6 41.7 ml/min (P ¼ 0.01). Co-treatment with KMþART was associated with an increased risk of renal insufficiency (hazard ratio [HR] 1.8, 95%CI 0.7–4.1, P ¼ 0.20 for KMþTDF, and HR 3.5, 95%CI 1.4–8.2, P ¼ 0.005 for KMþOther ART). CONCLUSION: Renal function declined at a similar rate in MDR-TB patients treated with KM-based regimens compared with patients treated concomitantly with TDF-based or other ART. The risk of renal insufficiency was greater for patients on ART

Utrecht University Repository

Track E Implementation Science, Health Systems and Economics

Author: Abolarin O.
Ackers M.
Ackers M.
Adouko S.
Adungosi J.
Afolayan F.
Aghokeng A.
Agot K.
Ahimbisibwe A.
Ahmed Y.
Akwei Addo N.
Alary M.
Alexander G.
Ali S.A.
Allman D.
Alumando E.S.
Alves J.
Amanyire G.
Amenyah R.
Angela A.
Anthony G.
Anthony J.
Ardura Garcia C.
Arrighi Y.
Asante F.
Asante K.
Ashigbie P.
Assouan I.
Atibu J.
Atuahene K.
Avafia T.
Avalos A.
Ayieko B.
Ayuaya T.
Babu R.
Barros H.
Barry M.
Behets F.
Bertrand J.
Bertrand J.
Bhardwaj K.
Bhende A.
Bilguissa D.
Birdthistle I.
Birger R.
Black D.
Bogart L.
Bogg L.
Bollinger T.
Bor J.
Bor J.
Boulet P.
Boyer S.
Brink B.
Brockington S.
Buhendwa L.
Burrone E.
Byonanebye D.
Bärnighausen T.
Bärnighausen T.
Bärnighausen T.
Carrieri M.P.
Castor D.
Castor D.
Chabikuli O.
Chadambuka A.
Chamie G.
Chamie G.
Chamie G.
Chandisarewa W.
Chandrashekar S.
Charlebois E.
Charlebois E.
Charlebois E.D.
Chasela C.S.
Chavez J.
Cheng X.
Chetty S.
Chidarikire T.
Chikwinya B.
Chileshe C.
Chimbindi N.Z.
Chipimo M.
Chisoko C.
Churchman E.
Churchyard G.
Ciccacci F.
Clark T.
Clark T.
Clark T.
Cockburn J.
Cohn J.
Coleman S.
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Dagunduro T.
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Publication venue: 'International AIDS Society'
Publication date: 01/10/2012
Field of study

Peer Reviewedhttps://deepblue.lib.umich.edu/bitstream/2027.42/138412/1/jia218443.pd

Deep Blue Documents at the University of Michigan

Enhanced infection prophylaxis reduces mortality in severely immunosuppressed HIV-infected adults and older children initiating antiretroviral therapy in Kenya, Malawi, Uganda and Zimbabwe: the REALITY trial

Author: Abach J
Abdallah J
Abdallah S
Abdallah S
Aberle-Grasse J
Abimiku A
Abishev A
Abongomera G
Aboud M
Aboud M
Abramovitz D
Abrams E
Abrams E
Abrams E
Abrams E
Abravaya K
Abreu L
Achra A
Adera F
Adetokunboh O
Adeyemi O
Adeyemi O
Adipo T
Affolabi D
Agegnehu D
Agius P
Agolory S
Agot K
Agot K
Agovi A-A
Aguiar P
Aguilar-Martinez J
Agutu C
Ahmed M
Ahmed R
Ahmed S
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Aizire J
Ajibola G
Ajok S
Albert-Hope C
Alejos B
Alexander G
Alicea C
Allen H
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Allen S
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Alloui C
Altice F
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Amara R
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Amin J
Amin T
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Amoros I
Anahtar M
Ananworanich J
Ananworanich J
Ancuta P
Andama A
Anderegg N
Anderson A
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Anderson J
Anderson S
Andersson M
Andrade A
Andrew E
Andrew P
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Angel J
Angelidou K
Anglaret X
Anoma C
Ansari A
Apetrei C
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Apondi E
Aptekar S
Ardiet D
Arellano G
Arenas-Pinto A
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Arunmanakul A
Asari V
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Asiimwe S
Asiimwe S
Asiimwe S
Asokan M
Aspin C
Athiambo M
Atuhumuza E
Atujuna M
Audet C
Auerbach J
Auld A
Aung P
Aurpibul L
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Avalos A
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Dias PG
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Dimba A
Dinanga JD
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Dirawo J
Diseko M
Dlamini D
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Doherty T
Dolezal C
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Dores CD
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Dronda F
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Finlayson T
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Galárraga O
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Ghebremichael
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Golub
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Granados CD
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Greene E
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Griffith S
Griffiths A
Griffiths A
Grimwood A
Grinsztejn B
Grinsztejn B
Grobler A
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Gross R
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Group AAVTA
Group AS
Group E-NS
Group FS
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Kapogiannis
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Karim QA
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Karim QA
Karim QA
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Lewin
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Lewinsohn D
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Publication venue: 'International AIDS Society'
Publication date: 01/01/2016
Field of study

Meeting abstract FRAB0101LB from 21st International AIDS Conference 18–22 July 2016, Durban, South Africa. Introduction: Mortality from infections is high in the first 6 months of antiretroviral therapy (ART) among HIV‐infected adults and children with advanced disease in sub‐Saharan Africa. Whether an enhanced package of infection prophylaxis at ART initiation would reduce mortality is unknown. Methods: The REALITY 2×2×2 factorial open‐label trial (ISRCTN43622374) randomized ART‐naïve HIV‐infected adults and children >5 years with CD4 <100 cells/mm3. This randomization compared initiating ART with enhanced prophylaxis (continuous cotrimoxazole plus 12 weeks isoniazid/pyridoxine (anti‐tuberculosis) and fluconazole (anti‐cryptococcal/candida), 5 days azithromycin (anti‐bacterial/protozoal) and single‐dose albendazole (anti‐helminth)), versus standard‐of‐care cotrimoxazole. Isoniazid/pyridoxine/cotrimoxazole was formulated as a scored fixed‐dose combination. Two other randomizations investigated 12‐week adjunctive raltegravir or supplementary food. The primary endpoint was 24‐week mortality. Results: 1805 eligible adults (n = 1733; 96.0%) and children/adolescents (n = 72; 4.0%) (median 36 years; 53.2% male) were randomized to enhanced (n = 906) or standard prophylaxis (n = 899) and followed for 48 weeks (3.8% loss‐to‐follow‐up). Median baseline CD4 was 36 cells/mm3 (IQR: 16–62) but 47.3% were WHO Stage 1/2. 80 (8.9%) enhanced versus 108(12.2%) standard prophylaxis died before 24 weeks (adjusted hazard ratio (aHR) = 0.73 (95% CI: 0.54–0.97) p = 0.03; Figure 1) and 98(11.0%) versus 127(14.4%) respectively died before 48 weeks (aHR = 0.75 (0.58–0.98) p = 0.04), with no evidence of interaction with the two other randomizations (p > 0.8). Enhanced prophylaxis significantly reduced incidence of tuberculosis (p = 0.02), cryptococcal disease (p = 0.01), oral/oesophageal candidiasis (p = 0.02), deaths of unknown cause (p = 0.02) and (marginally) hospitalisations (p = 0.06) but not presumed severe bacterial infections (p = 0.38). Serious and grade 4 adverse events were marginally less common with enhanced prophylaxis (p = 0.06). CD4 increases and VL suppression were similar between groups (p > 0.2). Conclusions: Enhanced infection prophylaxis at ART initiation reduces early mortality by 25% among HIV‐infected adults and children with advanced disease. The pill burden did not adversely affect VL suppression. Policy makers should consider adopting and implementing this low‐cost broad infection prevention package which could save 3.3 lives for every 100 individuals treated

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