2018
DOI: 10.7196/samj.2018.v108i2.12573
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Characteristics and early outcomes of children and adolescents treated with darunavir/ritonavir-, raltegravir- or etravirine-containing antiretroviral therapy in the Western Cape Province of South Africa

Abstract: RESEARCHBy 2012, the estimated number of children (0 -14 years of age) receiving antiretroviral therapy (ART) in South Africa (SA) was 140 541, representing an estimated 63% of those requiring treatment. [1,2] As increasing numbers of children are started on first-and second-line ART, the demand for third-line regimens in children and adolescents with treatment failure is likely to increase. It is estimated that currently <1% of people on ART globally are receiving third-line regimens, and it is unknown what p… Show more

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Cited by 3 publications
(2 citation statements)
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“…[17,22,23] With the SA national antiretroviral treatment guidelines in the past (2004 -2007) having advocated full-dose RTV in children aged <6 months and those on concomitant rifampicinbased antituberculosis therapy, [12] 6 (27.3%) of the children in our cohort with major PI mutations had been on full-dose RTV. Similar findings from a number of small studies of children on full-dose RTV support the development of major PI resistance mutations, with reported rates of 37.1%, [24] 50% [18] and 72%. [14] However, the high proportion of children with major PI-associated resistance mutations in our cohort (95.5%) cannot be explained by prior use of RTV alone.…”
Section: Discussionsupporting
confidence: 71%
See 1 more Smart Citation
“…[17,22,23] With the SA national antiretroviral treatment guidelines in the past (2004 -2007) having advocated full-dose RTV in children aged <6 months and those on concomitant rifampicinbased antituberculosis therapy, [12] 6 (27.3%) of the children in our cohort with major PI mutations had been on full-dose RTV. Similar findings from a number of small studies of children on full-dose RTV support the development of major PI resistance mutations, with reported rates of 37.1%, [24] 50% [18] and 72%. [14] However, the high proportion of children with major PI-associated resistance mutations in our cohort (95.5%) cannot be explained by prior use of RTV alone.…”
Section: Discussionsupporting
confidence: 71%
“…Baseline clinical information on the study participants reflects a pattern consistent with poor outcomes. [18] While the overall median age of initiation of cART was 3 years, 13.6% of the children were initiated at ages between 10 and 16 years and 91.0% were clinically staged as WHO III or IV. In addition, 40.9% of the children had a nadir CD4+ T-cell percentage between 0% and 10%.…”
Section: Discussionmentioning
confidence: 96%