Your search keyword '"Cotton, Mark F."' showing total 38 results

1. Lung function tracking in children with perinatally acquired HIV following early antiretroviral therapy initiation.

Author

Gie, André, Davies, Claire, Vaida, Florin, Morrison, Julie, Maree, David, Otwombe, Kennedy, Browne, Sara H., van der Zalm, Marieke M., Cotton, Mark F., Innes, Steve, and Goussard, Pierre

Subjects

PRECOCIOUS puberty, IMMUNE reconstitution inflammatory syndrome, ANTIRETROVIRAL agents, BRONCHOPULMONARY dysplasia, HIV, LUNGS

Published

2023

2. Associations of HIV and iron status with gut microbiota composition, gut inflammation and gut integrity in South African school‐age children: a two‐way factorial case–control study.

Author

Goosen, Charlene, Proost, Sebastian, Baumgartner, Jeannine, Mallick, Kashish, Tito, Raul Y., Barnabas, Shaun L., Cotton, Mark F., Zimmermann, Michael B., Raes, Jeroen, and Blaauw, Renée

Subjects

FECAL analysis, HIV infections, BIOMARKERS, RELATIVE medical risk, IRON, GUT microbiome, INFLAMMATION, FATTY acid-binding proteins, IRON in the body, CASE-control method, ANTIRETROVIRAL agents, IRON deficiency, RESEARCH funding, ANEMIA

Abstract

Background: Human immunodeficiency virus (HIV) and iron deficiency (ID) affect many African children. Both HIV and iron status interact with gut microbiota composition and related biomarkers. The study's aim was to determine the associations of HIV and iron status with gut microbiota composition, gut inflammation and gut integrity in South African school‐age children. Methods: In this two‐way factorial case–control study, 8‐ to 13‐year‐old children were enrolled into four groups based on their HIV and iron status: (1) With HIV (HIV+) and ID (n = 43), (2) HIV+ and iron‐sufficient nonanaemic (n = 41), (3) without HIV (HIV−) and ID (n = 44) and (4) HIV− and iron‐sufficient nonanaemic (n = 38). HIV+ children were virally suppressed (<50 HIV RNA copies/ml) on antiretroviral therapy (ART). Microbial composition of faecal samples (16S rRNA sequencing) and markers of gut inflammation (faecal calprotectin) and gut integrity (plasma intestinal fatty acid–binding protein [I‐FABP]) were assessed. Results: Faecal calprotectin was higher in ID versus iron‐sufficient nonanaemic children (p = 0.007). I‐FABP did not significantly differ by HIV or iron status. ART‐treated HIV (redundancy analysis [RDA] R2 = 0.009, p = 0.029) and age (RDA R2 = 0.013 p = 0.004) explained the variance in the gut microbiota across the four groups. Probabilistic models showed that the relative abundance of the butyrate‐producing genera Anaerostipes and Anaerotruncus was lower in ID versus iron‐sufficient children. Fusicatenibacter was lower in HIV+ and in ID children versus their respective counterparts. The prevalence of the inflammation‐associated genus Megamonas was 42% higher in children with both HIV and ID versus HIV− and iron‐sufficient nonanaemic counterparts. Conclusions: In our sample of 8‐ to 13‐year‐old virally suppressed HIV+ and HIV− children with or without ID, ID was associated with increased gut inflammation and changes in the relative abundance of specific microbiota. Moreover, in HIV+ children, ID had a cumulative effect that further shifted the gut microbiota to an unfavourable composition. Key points: 1.Iron deficiency (ID) was associated with higher gut inflammation measured by faecal calprotectin.2.Gut mucosal integrity measured by intestinal fatty acid–binding protein did not differ by human immunodeficiency virus (HIV) or iron status.3.In HIV+ children, ID had a cumulative effect that promoted an unfavourable gut microbiota composition. [ABSTRACT FROM AUTHOR]

Published

2023

3. Optimizing the World Health Organization algorithm for HIV vertical transmission risk assessment by adding maternal self-reported antiretroviral therapy adherence.

Author

Fernández-Luis, Sheila, Lain, Maria Grazia, Serna-Pascual, Miquel, Domínguez-Rodríguez, Sara, Kuhn, Louise, Liberty, Afaaf, Barnabas, Shaun, Lopez-Varela, Elisa, Otwombe, Kennedy, Danaviah, Siva, Nastouli, Eleni, Palma, Paolo, Cotugno, Nicola, Spyer, Moira, Giannuzzi, Viviana, Giaquinto, Carlo, Violari, Avy, Cotton, Mark F., Nhampossa, Tacilta, and Klein, Nigel

Subjects

HIV prevention, ANTI-HIV agents, COMMUNICABLE diseases, SELF-evaluation, RETROSPECTIVE studies, ANTIRETROVIRAL agents, RISK assessment, PREGNANCY complications, VERTICAL transmission (Communicable diseases), ALGORITHMS

Abstract

Background: The World Health Organization (WHO) risk assessment algorithm for vertical transmission of HIV (VT) assumes the availability of maternal viral load (VL) result at delivery and early viral control 4 weeks after initiating antiretroviral treatment (ART). However, in many low-and-middle-income countries, VL is often unavailable and mothers' ART adherence may be suboptimal. We evaluate the inclusion of the mothers' self-reported adherence into the established WHO-algorithm to identify infants eligible for enhanced post-natal prophylaxis when mothers' VL result is not available at delivery.Methods: We used data from infants with perinatal HIV infection and their mothers enrolled from May-2018 to May-2020 in Mozambique, South Africa, and Mali. We retrospectively compared the performance of the WHO-algorithm with a modified algorithm which included mothers' adherence as an additional factor. Infants were considered at high risk if born from mothers without a VL result in the 4 weeks before delivery and with adherence <90%.Results: At delivery, 143/184(78%) women with HIV knew their status and were on ART. Only 17(12%) obtained a VL result within 4 weeks before delivery, and 13/17(76%) of them had VL ≥1000 copies/ml. From 126 women on ART without a recent VL result, 99(79%) had been on ART for over 4 weeks. 45/99(45%) women reported suboptimal (< 90%) adherence. A total of 81/184(44%) infants were classified as high risk of VT as per the WHO-algorithm. The modified algorithm including self-adherence disclosure identified 126/184(68%) high risk infants.Conclusions: In the absence of a VL result, mothers' self-reported adherence at delivery increases the number of identified infants eligible to receive enhanced post-natal prophylaxis. [ABSTRACT FROM AUTHOR]

Published

2022

4. Early ART-initiation and longer ART duration reduces HIV-1 proviral DNA levels in children from the CHER trial.

Author

Payne, Helen, Chan, Man K., Watters, Sarah A., Otwombe, Kennedy, Hsiao, Nei-Yuan, Babiker, Abdel, Violari, Avy, Cotton, Mark F., Gibb, Diana M., and Klein, Nigel J.

Subjects

HIV infections, DNA, MONONUCLEAR leukocytes, SERODIAGNOSIS, ANTIRETROVIRAL agents, TREATMENT duration, RNA, REGRESSION analysis, TREATMENT effectiveness, EARLY intervention (Education), DESCRIPTIVE statistics, CD4 lymphocyte count, POLYMERASE chain reaction, HIV, LONGITUDINAL method, ANTIGENS, EVALUATION, CHILDREN

Abstract

Background: Reduction of the reservoir of latent HIV-infected cells might increase the possibility of long-term remission in individuals living with HIV. We investigated factors associated with HIV-1 proviral DNA levels in children receiving different antiretroviral therapy (ART) strategies in the children with HIV early antiretroviral therapy (CHER) trial. Methods: Infants with HIV < 12 weeks old with CD4% ≥ 25% were randomized in the CHER trial to early limited ART for 40 or 96 weeks (ART-40 W, ART-96 W), or deferred ART (ART-Def). For ART-Def infants or following ART interruption in ART-40 W/ART-96 W, ART was started/re-started for clinical progression or CD4% < 25%. In 229 participants, HIV-1 proviral DNA was quantified by PCR from stored peripheral blood mononuclear cells from children who had received ≥ 24 weeks ART and two consecutive undetectable HIV-1 RNA 12–24 weeks apart. HIV-1 proviral DNA was compared between ART-Def and ART-96 W at week 96, and in all arms at week 248. Factors associated with HIV-1 proviral DNA levels were evaluated using linear regression. Findings: Longer duration of ART was significantly associated with lower HIV-1 proviral DNA at both 96 (p = 0.0003) and 248 weeks (p = 0.0011). Higher total CD8 count at ART initiation was associated with lower HIV-1 proviral DNA at both 96 (p = 0.0225) and 248 weeks (p = 0.0398). Week 248 HIV-1 proviral DNA was significantly higher in those with positive HIV-1 serology at week 84 than those with negative serology (p = 0.0042). Intepretation: Longer ART duration is key to HIV-1 proviral DNA reduction. Further understanding is needed of the effects of "immune-attenuation" through early HIV-1 exposure. Funding: Wellcome Trust, National Institutes of Health, Medical Research Council. [ABSTRACT FROM AUTHOR]

Published

2021

5. Tuberculosis infection and disease in South African adolescents with perinatally acquired HIV on antiretroviral therapy: a cohort study.

Author

Frigati, Lisa J, Wilkinson, Katalin A, Roux, Stanzi, Brown, Karryn, Ruzive, Sheena, Githinji, Leah, Petersen, Wonita, Belard, Sabine, Cotton, Mark F, Myer, Landon, and Zar, Heather J

Subjects

SOUTH Africans, ANTIRETROVIRAL agents, TUBERCULOSIS, COHORT analysis, HIV, IMMUNE reconstitution inflammatory syndrome, PLICA syndrome

Abstract

Introduction: There are limited data on Tuberculosis (TB) in adolescents with perinatally acquired HIV (APHIV). We examined the incidence and determinants of TB infection and disease in the Cape Town Adolescent Antiretroviral Cohort (CTAAC). Methods: Youth between nine and fourteen years on antiretroviral therapy (ART) for more than six months in public sector care, and age‐matched HIV‐negative adolescents, were enrolled between July 2013 through March 2015 and followed six‐monthly. Data were censored on 31 October 2018. Symptom screening, chest radiograph, viral load, CD4 count, QuantiFERON (QFT) and sputum for Xpert MTB/RIF, microscopy, culture and sensitivity were performed annually. TB infection was defined by a QFT of >0.35 IU/mL. TB diagnosis was defined as confirmed (culture or Xpert MTB/RIF positive) or unconfirmed (clinical diagnosis and started on TB treatment). Analyses examined the incidence and determinants of TB infection and disease. Results: Overall 496 HIV+ and 103 HIV‐negative participants (median age at enrolment 12 years (interquartile range, IQR 10.6 to 13.3) were followed for a median of 3.1 years (IQR 3.0 to 3.4); 50% (298/599) were male. APHIV initiated ART at median age 4.4 years (IQR 2.1 to 7.6). At enrolment, 376/496 (76%) had HIV viral load <40 copies/mL, median CD4 count was 713 cells/mm3 and 179/559 (32%) were QFT+, with no difference by HIV status (APHIV 154/468, 33%; HIV negative 25/91, 27%; p = 0.31). The cumulative QFT+ prevalence was similar (APHIV 225/492, 46%; 95%CI 41% to 50%; HIV negative 44/98, 45%; 95% CI 35% to 55%; p = 0.88). APHIV had a higher incidence of all TB disease than HIV‐negative adolescents (2.2/100PY, 95% CI 1.6 to 3.1 vs. 0.3/100PY, 95% CI 0.04 to 2.2; IRR 7.36, 95% CI 1.01 to 53.55). The rate of bacteriologically confirmed TB in APHIV was 1.3/100 PY compared to 0.3/100PY for HIV‐negative adolescents, suggesting a fourfold increased risk of developing TB disease in APHIV despite access to ART. In addition, a positive QFT at enrolment was not predictive of TB in this population. Conclusions: High incidence rates of TB disease occur in APHIV despite similar QFT conversion rates to HIV‐negative adolescents. Strategies to prevent TB in this vulnerable group must be strengthened. [ABSTRACT FROM AUTHOR]

Published

2021

6. ODYSSEY clinical trial design: a randomised global study to evaluate the efficacy and safety of dolutegravir-based antiretroviral therapy in HIV-positive children, with nested pharmacokinetic sub-studies to evaluate pragmatic WHO-weight-band based dolutegravir dosing

Author

Moore, Cecilia L., Turkova, Anna, Mujuru, Hilda, Kekitiinwa, Adeodata, Lugemwa, Abbas, Kityo, Cissy M., Barlow-Mosha, Linda N., Cressey, Tim R., Violari, Avy, Variava, Ebrahim, Cotton, Mark F., Archary, Moherndran, Compagnucci, Alexandra, Puthanakit, Thanyawee, Behuhuma, Osee, Saϊdi, Yacine, Hakim, James, Amuge, Pauline, Atwine, Lorna, and Musiime, Victor

Subjects

DOLUTEGRAVIR, HIV-positive children, EXPERIMENTAL design, ANTIRETROVIRAL agents, PHARMACOKINETICS, GLOBAL studies, TEENAGE girls

Abstract

Background: Dolutegravir (DTG)-based antiretroviral therapy (ART) is highly effective and well-tolerated in adults and is rapidly being adopted globally. We describe the design of the ODYSSEY trial which evaluates the efficacy and safety of DTG-based ART compared with standard-of-care in children and adolescents. The ODYSSEY trial includes nested pharmacokinetic (PK) sub-studies which evaluated pragmatic World Health Organization (WHO) weight-band-based DTG dosing and opened recruitment to children < 14 kg while dosing was in development. Methods: ODYSSEY (Once-daily DTG based ART in Young people vS. Standard thErapY) is an open-label, randomised, non-inferiority, basket trial comparing the efficacy and safety of DTG + 2 nucleos(t) ides (NRTIs) versus standard-of-care (SOC) in HIV-infected children < 18 years starting first-line ART (ODYSSEY A) or switching to second-line ART (ODYSSEY B). The primary endpoint is clinical or virological failure by 96 weeks. Results: Between September 2016 and June 2018, 707 children weighing ≥14 kg were enrolled; including 311 ART-naïve children and 396 children starting second-line. 47% of children were enrolled in Uganda, 21% Zimbabwe, 20% South Africa, 9% Thailand, 4% Europe. 362 (51%) participants were male; median age [range] at enrolment was 12.2 years [2.9–18.0]. 82 (12%) children weighed 14 to < 20 kg, 135 (19%) 20 to < 25 kg, 206 (29%) 25 to < 35 kg, 284 (40%) ≥35 kg. 128 (18%) had WHO stage 3 and 60 (8%) WHO stage 4 disease. Challenges encountered include: (i) running the trial across high- to low-income countries with differing frequencies of standard-of-care viral load monitoring; (ii) evaluating pragmatic DTG dosing in PK sub-studies alongside FDA- and EMA-approved dosing and subsequently transitioning participants to new recommended doses; (iii) delays in dosing information for children weighing 3 to < 14 kg and rapid recruitment of ART-naïve older/heavier children, which led to capping recruitment of participants weighing ≥35 kg in ODYSSEY A and extending recruitment (above 700) to allow for ≥60 additional children weighing between 3 to < 14 kg with associated PK; (iv) a safety alert associated with DTG use during pregnancy, which required a review of the safety plan for adolescent girls. Conclusions: By employing a basket design, to include ART-naïve and -experienced children, and nested PK sub-studies, the ODYSSEY trial efficiently evaluates multiple scientific questions regarding dosing and effectiveness of DTG-based ART in children. Trial registration: NCT, NCT02259127, registered 7th October 2014; EUDRACT, 2014–002632-14, registered 18th June 2014 (https://www.clinicaltrialsregister.eu/ctr-search/trial/2014-002632-14/ES); ISRCTN, ISRCTN91737921, registered 4th October 2014. [ABSTRACT FROM AUTHOR]

Published

2021

7. Recovery of HIV encephalopathy in perinatally infected children on antiretroviral therapy.

Author

Innes, Steve, Laughton, Barbara, Toorn, Ronald, Otwombe, Kennedy, Liberty, Afaaf, Dobbels, Els, Violari, Avy, Kruger, Mariana, Cotton, Mark F, and van Toorn, Ronald

Subjects

AIDS dementia complex, ANTIRETROVIRAL agents, CEREBRAL palsy, IMMUNE reconstitution inflammatory syndrome, VIRAL load, MOTOR neurons, BRAIN, RESEARCH, RESEARCH methodology, MOVEMENT disorders, DEVELOPMENTAL disabilities, CASE-control method, RETROSPECTIVE studies, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, RESEARCH funding, STATISTICAL sampling, GROWTH disorders, VERTICAL transmission (Communicable diseases), LONGITUDINAL method, DISEASE complications

Abstract

Aim: To describe the trajectory of clinical signs in children who developed human immunodeficiency virus encephalopathy (HIVE) after starting early antiretroviral therapy (ART).Method: This was a retrospective case-cohort description of HIVE among Cape Town participants from the Children with HIV Early AntiRetroviral treatment (CHER) trial. Criteria for HIVE diagnosis were at least two of: (1) acquired central motor deficit, (2) impaired brain growth, and (3) failure to attain or loss of developmental milestones in the absence of an alternative aetiology.Results: Of 133 surviving participants who initiated ART at a median age of 9 weeks and who were followed until a median age of 6 years, 20 (12%) developed HIVE at a median age 31 months (interquartile range 19-37). In these, the first neurological deterioration was noticed at a median age of 19 months, when 16 were on ART and nine had undetectable HIV viral load for a median of 12 months. Signs of upper motor neurons were present in 18, of whom 12 resolved and four had persistent spastic diplegia; 19 had motor delay, of whom 14 resolved; 12 had language delay, of whom 11 resolved; and 16 had impaired brain growth, of whom only five recovered. For the 16 participants already on ART at HIVE diagnosis, regimens were not altered in response to diagnosis.Interpretation: HIVE may occur despite early ART initiation and virological suppression and then resolve on unchanged ART, most likely as intrathecal inflammation subsides.What This Paper Adds: Despite suppressive antiretroviral therapy, children can develop human immunodeficiency virus encephalopathy, The most common manifestations are motor deficits and impaired brain growth. Most experience improvement, with many resolving without additional intervention. [ABSTRACT FROM AUTHOR]

Published

2020

8. Diffusion tensor imaging point to ongoing functional impairment in HIV-infected children at age 5, undetectable using standard neurodevelopmental assessments.

Author

Ackermann, Christelle, Andronikou, Savvas, Saleh, Muhammad G., Kidd, Martin, Cotton, Mark F., Meintjes, Ernesta M., and Laughton, Barbara

Subjects

HIV infection complications, COGNITION in children, HIV infections, HIV-positive persons, LONGITUDINAL method, MAGNETIC resonance imaging, NEUROPSYCHOLOGICAL tests, SOCIAL skills, VISUAL perception, ANTIRETROVIRAL agents, TREATMENT effectiveness, WHITE matter (Nerve tissue), CHILDREN

Abstract

Background: Perinatal HIV infection negatively impacts cognitive functioning of children, main domains affected are working memory, processing speed and executive function. Early ART, even when interrupted, improves neurodevelopmental outcomes. Diffusion tension imaging (DTI) is a sensitive tool assessing white matter damage. We hypothesised that white matter measures in regions showing HIV-related alterations will be associated with lower neurodevelopmental scores in specific domains related to the functionality of the affected tracts. Methods: DTI was performed on children in a neurodevelopmental sub study from the Children with HIV Early Antiretroviral (CHER) trial. Voxel-based group comparisons to determine regions where fractional anisotropy and mean diffusion differed between HIV+ and uninfected children were done. Locations of clusters showing group differences were identified using the Harvard–Oxford cortical and subcortical and John Hopkins University WM tractography atlases provided in FSL. This is a second review of DTI data in this cohort, which was reported in a previous study. Neurodevelopmental assessments including GMDS and Beery-Buktenica tests were performed and correlated with DTI parameters in abnormal white matter. Results: 38 HIV+ children (14 male, mean age 64.7 months) and 11 controls (4 male, mean age 67.7 months) were imaged. Two clusters with lower fractional anisotropy and 7 clusters with increased mean diffusion were identified in the HIV+ group. The only neurodevelopmental domain with a trend of difference between the HIV+ children and controls (p = 0.08), was Personal Social Quotient which correlated to improved myelination of the forceps minor in the control group. As a combined group there was a negative correlation between visual perception and radial diffusion in the right superior longitudinal fasciculus and left inferior longitudinal fasciculus, which may be related to the fact that these tracts, forming part of the visual perception pathway, are at a crucial state of development at age 5. Conclusion: Even directed neurodevelopmental tests will underestimate the degree of microstructural white matter damage detected by DTI. The visual perception deficit detected in the entire study population should be further examined in a larger study. [ABSTRACT FROM AUTHOR]

Published

2020

9. Measles Immunity at 4.5 Years of Age Following Vaccination at 9 and 15–18 Months of Age Among Human Immunodeficiency Virus (HIV)–infected, HIV-exposed–uninfected, and HIV-unexposed Children.

Author

Mutsaerts, Eleonora A M L, Nunes, Marta C, Rijswijk, Martijn N van, Klipstein-Grobusch, Kerstin, Otwombe, Kennedy, Cotton, Mark F, Violari, Avy, and Madhi, Shabir A

Subjects

DIAGNOSIS of HIV infections, MEASLES prevention, ANTIRETROVIRAL agents, ENZYME-linked immunosorbent assay, HIV infections, HIV-positive persons, IMMUNOGLOBULINS, MEASLES, MEASLES vaccines, VIRAL antibodies, TERMINATION of treatment, TREATMENT effectiveness, CHILDREN

Abstract

Background Human immunodeficiency virus (HIV)–infected and HIV-exposed–uninfected (HEU) children may be at increased risk of measles infection due to waning of immunity following vaccination. We evaluated persistence of antibodies to measles vaccination at 4.5 years of age in HIV-unexposed, HEU, and HIV-infected children with CD4+ ≥25% previously randomized to immediate antiretroviral therapy (ART) interrupted at 12 months (HIV/Immed-ART-12), 24 months (HIV/Immed-ART-24), or when clinically/immunologically indicated (HIV/Def-ART). The HIV/Def-ART group initiated ART by median 5.8 (interquartile range, 4.4–10.3) months of age. Methods In this study, HIV-unexposed (n = 95), HEU (n = 84), HIV/Immed-ART-12 (n = 70), HIV/Immed-ART-24 (n = 70), and HIV/Def-ART (n = 62) children were scheduled to receive measles vaccination at age 9 and 15–18 months. Antimeasles serum immunoglobulin G titers were quantified using enzyme-linked immunosorbent assay at 4.5 years. Results Compared with HIV-unexposed children (2860 mIU/mL), measles antibody geometric mean titers (GMTs) were significantly lower in both HIV/Immed-ART-12 (571; P <.001) and HIV/Immed-ART-24 (1136; P <.001) but similar in the HIV/Def-ART (2777) and HEU (3242) groups. Furthermore, compared with HIV-unexposed, antibody titers ≥330 mIU/mL (ie, presumed serocorrelate for protection; 99%) were also significantly lower in HIV/Immed-ART-12 (70%; P <.001) and HIV/Immed-ART-24 (83%; P <.001) but similar in the HIV/Def-ART (90%) and HEU (98%) groups. Conclusions HIV-infected children in whom ART was interrupted at either 12 or 24 months had lower GMTs and lower proportions with seroprotective titers than HIV-unexposed children, indicating a potential downside of ART treatment interruption. Clinical Trials Registration NCT00099658 and NCT00102960. [ABSTRACT FROM AUTHOR]

Published

2019

10. Paediatric ART Adherence in South Africa: A Comprehensive Analysis.

Author

van Elsland, Sabine L., Peters, Remco P. H., Grobbelaar, Nelis, Ketelo, Patiswa, Kok, Maarten O., Cotton, Mark F., and van Furth, A. Marceline

Subjects

CAREGIVERS, DRUGS, HIV infections, PSYCHOLOGY of HIV-positive persons, INTERVIEWING, RESEARCH methodology, PATIENT compliance, QUESTIONNAIRES, SELF-evaluation, SEX distribution, ANTIRETROVIRAL agents, FAMILY relations, SOCIOECONOMIC factors, CROSS-sectional method, DESCRIPTIVE statistics, CHILDREN

Abstract

Adherence to antiretroviral therapy (ART) remains a challenge for HIV-infected children. In this cross-sectional study, we used structured interview-administered questionnaires and medical records to measure adherence levels and factors associated with adherence and viral suppression. We included 195 South African children aged 2.1-12.9 on ART. Adherence levels ranged between 20.5% (pill count) and 89.1% (self-report). Boys were less adherent according to self-report, girls were less adherent according to pill count. Caregivers ensured medication was taken when the condition directly affected daily life. Well-functioning families and families with high SES provide a context supportive of adherence. Non-disclosure and difficulties administering medication negatively affected adherence and viral suppression. This study shows challenging levels of adherence impacting directly on viral suppression in a South African paediatric HIV program. Gender roles, non-disclosure and difficulty administering medication may undermine adherence and should be taken into account for clinical guidelines, policy design and inform strategies. [ABSTRACT FROM AUTHOR]

Published

2019

11. Perinatal HIV Infection or Exposure Is Associated With Low N-Acetylaspartate and Glutamate in Basal Ganglia at Age 9 but Not 7 Years.

Author

Robertson, Frances C., Holmes, Martha J., Cotton, Mark F., Dobbels, Els, Little, Francesca, Laughton, Barbara, van der Kouwe, André J. W., and Meintjes, Ernesta M.

Subjects

PERINATALLY-acquired HIV infections, BASAL ganglia, GLUTAMIC acid, ANTIRETROVIRAL agents, CREATINE, NUCLEAR magnetic resonance spectroscopy

Abstract

Abnormalities of the basal ganglia are frequently seen in HIV-infected (HIV+) children despite antiretroviral treatment (ART) initiation during childhood. Assessment of metabolites associated with neuronal integrity or with glial proliferation can present a sensitive description of metabolic events underlying basal ganglia structural changes. We used magnetic resonance spectroscopy to examine differences in creatine, choline, N-acetylaspartate (NAA), glutamate, and myo-inositol between HIV+ children and HIV-unexposed controls, as well as between HIV-exposed uninfected (HEU) children and HIV-unexposed controls at age 7 and at age 9. No differences in metabolites relative to the HIV-unexposed control group were found at age 7. However, at 9 years, both HIV+ and HEU had lower NAA and glutamate than unexposed control children. HEU children also had lower creatine and choline than control children. At age 7, lower CD4/CD8 ratio at enrollment was associated with lower choline levels. At age 9 lower CD4/CD8 at enrollment was associated with lower myo-inositol. Low NAA and glutamate at age 9, but not 7, suggest that basal ganglia neurons may be particularly affected by perinatal HIV/ART and that neuronal damage may be ongoing despite early ART and viral suppression. Reduced basal ganglia metabolite levels in HEU children suggest an effect of HIV exposure on childhood brain development that merits further investigation using neuroimaging and neurocognitive testing. [ABSTRACT FROM AUTHOR]

Published

2018

12. Favourable outcome in a child with symptomatic diagnosis of Glutaric aciduria type 1 despite vertical HIV infection and minor head trauma.

Author

Thomas, Angeline, Dobbels, Els F. M., Springer, Priscilla E., Ackermann, Christelle, Cotton, Mark F., and Laughton, Barbara

Subjects

GLUTARIC aciduria, GENETIC testing, ANTIRETROVIRAL agents, HIV infections, THERAPEUTICS, BRAIN imaging

Abstract

The first case of Glutaric aciduria Type 1(GA1) in an African child was reported in 2001. GA1 has a prevalence of 1:5000 in black South Africans. Although early diagnosis is essential for a favourable outcome, newborn screening is not routine in South Africa where an estimated 320,000 children have HIV infection. Neurodevelopmental delay and encephalopathy are complications of both HIV and GA1. In such a setting it is important to recognise that HIV and GA1 can occur simultaneously. We present an HIV-infected South African male child of Xhosa descent with macrocephaly who commenced combination antiretroviral therapy (ART) at 8 weeks of age in a clinical trial which included a neurodevelopmental sub-study. He developed short-lived focal seizures at 16 months after minor head trauma. Neurological examination was normal. Neuroimaging showed temporal lobe atrophy, subtle hyperintense signal change in the globus pallidus, and focal haemosiderosis in the right Sylvian fissure region. As findings were not in keeping with HIV encephalopathy, a urine metabolic screen was undertaken which suggested GA1. Genetic testing confirmed Arg293Trp mutation. He began L-carnitine and a low protein diet as a restricted diet was not practicable. At 21 months he developed pulmonary tuberculosis, requiring 6 months treatment. He did not develop any neurologic motor symptoms. Serial neurodevelopmental and neuropsychological test scores until 9 years were similar to healthy neighbourhood controls, except for mild language delay at 3½ years. Detection of GA1, probably facilitated through participation in a clinical trial, was pivotal for a favourable outcome. The concomitant use of ART and anti-tuberculous therapy in a child with GA1 appears safe. [ABSTRACT FROM AUTHOR]

Published

2018

13. Altered brain morphometry in 7-year old HIV-infected children on early ART.

Author

Nwosu, Emmanuel C., Robertson, Frances C., Holmes, Martha J., Cotton, Mark F., Dobbels, Els, Little, Francesca, Laughton, Barbara, van der Kouwe, Andre, and Meintjes, Ernesta M.

Subjects

ANTIRETROVIRAL agents, PEDIATRICS, MORPHOMETRICS, NEUROPSYCHOLOGICAL tests, MAGNETIC resonance imaging of the brain, THERAPEUTICS, HIV infections

Abstract

Even with the increased roll out of combination antiretroviral therapy (cART), paediatric HIV infection is associated with neurodevelopmental delays and neurocognitive deficits that may be accompanied by alterations in brain structure. Few neuroimaging studies have been done in children initiating ART before 2 years of age, and even fewer in children within the critical stage of brain development between 5 and 11 years. We hypothesized that early ART would limit HIV-related brain morphometric deficits at age 7. Study participants were 7-year old HIV-infected (HIV+) children from the Children with HIV Early Antiretroviral Therapy (CHER) trial whose viral loads were supressed at a young age, and age-matched uninfected controls. We used structural magnetic resonance imaging (MRI) and FreeSurfer (http://www.freesurfer.net/) software to investigate effects of HIV and age at ART initiation on cortical thickness, gyrification and regional brain volumes. HIV+ children showed reduced gyrification compared to controls in bilateral medial parietal regions, as well as reduced volumes of the right putamen, left hippocampus, and global white and gray matter and thicker cortex in small lateral occipital region. Earlier ART initiation was associated with lower gyrification and thicker cortex in medial frontal regions. Although early ART appears to preserve cortical thickness and volumes of certain brain structures, HIV infection is nevertheless associated with reduced gyrification in the parietal cortex, and lower putamen and hippocampus volumes. Our results indicate that in early childhood gyrification is more sensitive than cortical thickness to timing of ART initiation. Future work will clarify the implications of these morphometric effects for neuropsychological function. [ABSTRACT FROM AUTHOR]

Published

2018

14. Functional Connectivity Alterations between Networks and Associations with Infant Immune Health within Networks in HIV Infected Children on Early Treatment: A Study at 7 Years.

Author

Toich, Jadrana T. F., Taylor, Paul A., Holmes, Martha J., Gohel, Suril, Cotton, Mark F., Dobbels, Els, Laughton, Barbara, Little, Francesca, van der Kouwe, Andre J. W., Biswal, Bharat, and Meintjes, Ernesta M.

Subjects

HIV-positive children, THERAPEUTICS, HIV infections, IMMUNE system, NEURAL development, ANTIRETROVIRAL agents

Abstract

Although HIV has been shown to impact brain connectivity in adults and youth, it is not yet known to what extent long-term early antiretroviral therapy (ART) may alter these effects, especially during rapid brain development in early childhood. Using both independent component analysis (ICA) and seed-based correlation analysis (SCA), we examine the effects of HIV infection in conjunction with early ART on resting state functional connectivity (FC) in 7 year old children. HIV infected (HIV+) children were from the Children with HIV Early Antiretroviral Therapy (CHER) trial and all initiated ART before 18 months; uninfected children were recruited from an interlinking vaccine trial. To better understand the effects of current and early immune health on the developing brain, we also investigated among HIV+ children the association of FC at 7 years with CD4 count and CD4%, both in infancy (6-8 weeks) and at scan. Although we found no differences within any ICA-generated resting state networks (RSNs) between HIV+ and uninfected children (27 HIV+, 18 uninfected), whole brain connectivity to seeds located at RSN connectivity peaks revealed several loci of FC differences, predominantly from seeds in midline regions (posterior cingulate cortex, paracentral lobule, cuneus, and anterior cingulate). Reduced long-range connectivity and increased short-range connectivity suggest developmental delay. Within the HIV+ children, clinical measures at age 7 years were not associated with FC values in any of the RSNs; however, poor immune health during infancy was associated with localized FC increases in the somatosensory, salience and basal ganglia networks. Together these findings suggest that HIV may affect brain development from its earliest stages and persist into childhood, despite early ART. [ABSTRACT FROM AUTHOR]

Published

2018

15. Thymic Output and CD4 T-Cell Reconstitution in HIV-Infected Children on Early and Interrupted Antiretroviral Treatment: Evidence from the Children with HIV Early Antiretroviral Therapy Trial.

Author

Lewis, Joanna, Payne, Helen, Walker, A. Sarah, Otwombe, Kennedy, Gibb, Diana M., Babiker, Abdel G., Panchia, Ravindre, Cotton, Mark F., Violari, Avy, Klein, Nigel, and Callard, Robin E.

Subjects

HIGHLY active antiretroviral therapy, T cells, CHIMERIC antigen receptors, CELL-mediated cytotoxicity, ANTIRETROVIRAL agents

Abstract

Objectives: Early treatment of HIV-infected children and adults is important for optimal immune reconstitution. Infants' immune systems are more plastic and dynamic than older children's or adults', and deserve particular attention. This study aimed to understand the response of the HIV-infected infant immune system to early antiretroviral therapy (ART) and planned ART interruption and restart. Methods: Data from HIV-infected children enrolled the CHER trial, starting ART aged between 6 and 12 weeks, were used to explore the effect of ART on immune reconstitution. We used linear and non-linear regression and mixed-effects models to describe children's CD4 trajectories and to identify predictors of CD4 count during early and interrupted ART. Results: Early treatment arrested the decline in CD4 count but did not fully restore it to the levels observed in HIV-uninfected children. Treatment interruption at 40 or 96 weeks resulted in a rapid decline in CD4 T-cells, which on retreatment returned to levels observed before interruption. Naïve CD4 T-cell count was an important determinant of overall CD4 levels. A strong correlation was observed between thymic output and the stable CD4 count both before and after treatment interruption. Conclusion: Early identification and treatment of HIV-infected infants is important to stabilize CD4 counts at the highest levels possible. Once stabilized, children's CD4 counts appear resilient, with good potential for recovery following treatment interruption. The naïve T-cell pool and thymic production of naive cells are key determinants of children's CD4 levels. [ABSTRACT FROM AUTHOR]

Published

2017

16. Cross-cultural assessment of HIV-associated cognitive impairment using the Kaufman assessment battery for children: a systematic review.

Author

van Wyhe, Kaylee S., van de Water, Tanya, Boivin, Michael J., Cotton, Mark F., and Thomas, Kevin G. F.

Subjects

HIV infection complications, ANTIRETROVIRAL agents, COGNITIVE ability, NEUROPSYCHOLOGICAL tests, HIV infections, THERAPEUTICS

Abstract

Introduction: Despite improved efficacy of, and access to, combination antiretroviral therapy (cART), HIV-associated cognitive impairments remain prevalent in both children and adults. Neuropsychological tests that detect such impairment can help clinicians formulate effective treatment plans. The Kaufman Assessment Battery for Children (KABC), although developed and standardized in the United States, is used frequently in many different countries and cultural contexts to assess paediatric performance across various cognitive domains. This systematic review investigated the cross-cultural utility of the original KABC, and its 2nd edition (KABC-II), in detecting HIV-associated cognitive impairment in children and adolescents. Methods: We entered relevant keywords and MeSH terms into the PubMed, PsycInfo, EBSCOHost, ProQuest, and Scopus databases, with search limits set from 1983-2017. Two independent reviewers evaluated the retrieved abstracts and manuscripts. Studies eligible for inclusion in the review were those that (a) used the KABC/KABC-II to assess cognitive function in children/adolescents aged 2-18 years, (b) featured a definition of cognitive impairment (e.g. >2 SD below the mean) or compared the performance of HIV-infected and uninfected control groups, and (c) used a sample excluded from population on which the instruments were normed. Results and discussion: We identified nine studies (eight conducted in African countries, and one in the United Kingdom) to comprise the review's sample. All studies detected cognitive impairment in HIV-infected children, including those who were cART-naïve or who were cART treated and clinically stable. KABC/KABC-II subtests assessing simultaneous processing appeared most sensitive. Evaluation of the methodological quality of the selected studies by two independent reviews suggested that shortcomings included reporting and selection biases. Conclusions: This systematic review provides evidence for the cross-cultural utility of the KABC/KABC-II, particularly the simultaneous processing subtests, in detecting cognitive impairment in HIV-infected children (including those who are clinically stable). Although the current results suggest there is justification for using the KABC/KABC-II primarily in East Africa, further investigation is required to explore the instrument's utility in other HIV-prevalent regions of the globe. [ABSTRACT FROM AUTHOR]

Published

2017

17. Human Immunodeficiency Virus–exposed Uninfected Infants: Surviving and Thriving or Overlooked by Success?

Author

Slogrove, Amy L, Powis, Kathleen M, and Cotton, Mark F

Subjects

PREVENTION of communicable diseases, COMMUNICABLE diseases, DISEASE risk factors, HIV infection prognosis, HIV infection transmission, INFANT mortality, HIV infection complications, ANTIRETROVIRAL agents, BREASTFEEDING, HEALTH services accessibility, HIV infections, HOSPITAL care, INFANT health services, PREMATURE infants, PHENOTYPES, SEVERITY of illness index, VERTICAL transmission (Communicable diseases), MIDDLE-income countries, LOW-income countries, PRENATAL exposure delayed effects, CHILDREN, MORTALITY risk factors

Abstract

The author comments on the study by Goetghebuer et al that investigated risks of infant infection-related hospitalization in a human immunodeficiency virus (HIV)-exposed uninfected infants (HEU) cohort compared to HIV-unexposed (HU). The study established that initiation of maternal antiretroviral therapy before pregnancy reduced these risks. It notes that this study in high-income country with low HIV prevalence can not be generalized among poorer countries where most HEU children are born.

Published

2019

18. SPECIAL ISSUES AND MANAGEMENT OF HIV EXPOSED UNINFECTED INFANTS AND CHILDREN.

Author

Slogrove, Amy L. and Cotton, Mark F.

Subjects

*HIV prevention, *INFANTS, *HIV-positive persons, *CHILD health services, *ANTIRETROVIRAL agents

Abstract

New vertical HIV infections are declining and the numbers of HIV exposed but uninfected (HEU) infants and children are increasing. This positive trend is tempered by the realization that despite escaping HIV infection, the substantial population of HEU children bear consequences of being born to an HIV-infected mother. A structured approach to the care of these children may improve their long term health and well-being. We propose and discuss a 10-point care package for HEU infants centered on providing optimal basic child health management for all children both HIV-exposed and unexposed. Providing basic comprehensive child care interventions benefits all infants, both HIV-exposed and unexposed. For HEU infants, particular attention should be given to providing optimal vertical transmission prevention interventions and conducting appropriate HIV testing. Clinicians should be aware of the consequences of anti-retroviral (ARV) and HIV exposure on HEU infants. As vertical transmission prevention programs become more sophisticated there is a pressing need for the establishment of pharmacovigilance and long-term surveillance systems as well as affordable infant HIV diagnostic tests. [ABSTRACT FROM AUTHOR]

Published

2016

19. Acceptability and feasibility of mHealth and community-based directly observed antiretroviral therapy to prevent mother-to-child HIV transmission in South African pregnant women under Option B+: an exploratory study.

Author

Nachega, Jean B., Skinner, Donald, Jennings, Larissa, Magidson, Jessica F., Altice, Frederick L., Burke, Jessica G., Lester, Richard T., Uthman, Olalekan A., Knowlton, Amy R., Cotton, Mark F., Anderson, Jean R., and Theron, Gerhard B.

Subjects

ANTIRETROVIRAL agents, ANTI-HIV agents, MOBILE health, PREGNANCY complications, TEXT messages

Abstract

Objective: To examine the acceptability and feasibility of mobile health (mHealth)/short message service (SMS) and community-based directly observed antiretroviral therapy (cDOT) as interventions to improve antiretroviral therapy (ART) adherence for preventing mother-to-child human immunodeficiency virus (HIV) transmission (PMTCT). Design and methods: A mixed-method approach was used. Two qualitative focus group discussions with HIV-infected pregnant women (n=20) examined the acceptability and feasibility of two ART adherence interventions for PMTCT: 1) SMS text messaging and 2) patientnominated cDOT supporters. Additionally, 109 HIV-infected, pregnant South African women (18-30 years old) receiving PMTCT services under single-tablet antiretroviral therapy regimen during pregnancy and breastfeeding and continuing for life ("Option B+") were interviewed about mobile phone access, SMS use, and potential treatment supporters. Setting: A community primary care clinic in Cape Town, South Africa. Participants: HIV-infected pregnant women. Main outcomes: Acceptability and feasibility of mHealth and cDOT interventions. Results: Among the 109 women interviewed, individual mobile phone access and SMS use were high (>90%), and 88.1% of women were interested in receiving SMS ART adherence support messages such as reminders, motivation, and medication updates. Nearly all women (95%) identified at least one person close to them to whom they had disclosed their HIV status and would nominate as a cDOT supporter. Focus group discussions revealed that cDOT supporters and adherence text messages were valued, but some concerns regarding supporter time availability and risk of unintended HIV status disclosure were expressed. Conclusion: mHealth and/or cDOT supporter as interventions to improve ART adherence are feasible in this setting. However, safe HIV status disclosure to treatment supporters and confidentiality of text messaging content about HIV and ART were deemed crucial. [ABSTRACT FROM AUTHOR]

Published

2016

20. Early ART Results in Greater Immune Reconstitution Benefits in HIV-Infected Infants: Working with Data Missingness in a Longitudinal Dataset.

Author

Azzoni, Livio, Barbour, Russell, Papasavvas, Emmanouil, Glencross, Deborah K., Stevens, Wendy S., Cotton, Mark F., Violari, Avy, and Montaner, Luis J.

Subjects

HIV-positive infants, ANTIRETROVIRAL agents, HIV infections, THERAPEUTICS, HIV infections -- Immunological aspects, DISEASE progression, LONGITUDINAL method

Abstract

Background: Early initiation of anti-retroviral treatment (ART) decreases mortality as compared to deferred treatment, but whether it preserves immune cells from early loss or promotes their recovery remains undefined. Determination of complex immunological endpoints in infants is often marred by missing data due to missed visits and/or inadequate sampling. Specialized methods are required to address missingness and facilitate data analysis. Methods: We characterized the changes in cellular and humoral immune parameters over the first year of life in 66 HIV-infected infants (0–1 year of age) enrolled in the CHER study starting therapy within 12 weeks of birth (n = 42) or upon disease progression (n = 24). A convenience cohort of 23 uninfected infants aged 0–6 months born to mothers with HIV-1 infection was used as controls. Flow cytometry and ELISA were used to evaluate changes in natural killer (NK) cells, plasmacytoid dendritic cells (pDC), and CD4+ or CD8+ T-cell frequencies. Data missingness was assessed using Little's test. Complete datasets for analysis were created using Multiple Imputation (MI) or Bayesian modeling and multivariate analysis was conducted on the imputed datasets. Results: HIV-1-infected infants had greater frequency of CD4+ T cells with naïve phenotype, as well as higher serum IL-7 levels than HIV exposed/uninfected infants. The elevated data missingness was completely at random, allowing the use of both MI and Bayesian modeling. Both methods indicate that early ART initiation results in higher CD4+ T cell frequency, lower expression of CD95 in CD8+ T cell, and preservation of naïve T cell subsets. In contrast, innate immune effectors appeared to be similar independently of the timing of ART initiation. Conclusions: Early ART initiation in infants with perinatal HIV infection reduces immune activation and preserves an early expansion of naïve T-cells with undiminished innate cell numbers, giving greater immune reconstitution than achieved with deferred ART. Both statistical approaches concurred in this finding. [ABSTRACT FROM AUTHOR]

Published

2015

21. The last and first frontier - emerging challenges for HIV treatment and prevention in the first week of life with emphasis on premature and low birth weight infants.

Author

Cotton, Mark F, Holgate, Sandi, Nelson, Aurelie, Rabie, Helena, Wedderburn, Catherine, and Mirochnick, Mark

Subjects

*HIV infections, *THERAPEUTICS, *HIV prevention, *PERINATALLY-acquired HIV infections, *DIAGNOSIS of HIV infections, *LOW birth weight, *RISK factors in premature labor, *PREMATURE infants, *ANTIRETROVIRAL agents, *HEALTH, RISK factors

Abstract

Introduction There is new emphasis on identifying and treating HIV in the first days of life and also an appreciation that low birth weight (LBW) and preterm delivery (PTD) frequently accompany HIV-related pregnancy. Even in the absence of HIV, PTD and LBW contribute substantially to neonatal and infant mortality. HIV-exposed and -infected infants with these characteristics have received little attention thus far. As HIV programs expand to meet the 90-90-90 target for ending the HIV pandemic, attention should focus on newborn infants, including those delivered preterm or of LBW. Discussion In high prevalence settings, infant diagnosis of HIV is usually undertaken after the neonatal period. However, as in utero infection may be diagnosed at birth, earlier initiation of therapy may limit viral replication and prevent early damage. Globally, there is growing awareness that preterm and LBW infants constitute a substantial proportion of births each year. Preterm infants are at high risk for vertical transmission. Feeding difficulties, apnoea of prematurity and vulnerability to sepsis occur commonly. Feeding intolerance, a frequent occurrence, may compromise oral administration of medications. Although there is growing experience with post-exposure prophylaxis for HIV-exposed term newborn infants, there is less experience with preterm and LBW infants. For treatment, there are even fewer options for preterm infants. Only zidovudine has adequate dosing recommendations for treating term and preterm infants and has an intravenous formulation, essential if feeding intolerance occurs. Nevirapine dosing for prevention, but not treatment, is well established for both term and preterm infants. HIV diagnosis at birth is likely to be extremely stressful for new parents, more so if caring for preterm or LBW infants. Programs need to adapt to support the medical and emotional needs of young infants and their parents, where interventions may be lifesaving. Conclusions New focus is required for the newborn baby, including those born preterm, with LBW or small for gestational age to consolidate gains already made in early diagnosis and treatment of young children. [ABSTRACT FROM AUTHOR]

Published

2015

22. Early Antiretroviral Therapy in South African Children Reduces HIV-1-Infected Cells and Cell-Associated HIV-1 RNA in Blood Mononuclear Cells.

Author

van Zyl, Gert U, Bedison, Margaret A, van Rensburg, Anita Janse, Laughton, Barbara, Cotton, Mark F, and Mellors, John W

Subjects

DISEASE relapse prevention, ANTIRETROVIRAL agents, DNA analysis, RNA analysis, BLOOD, HIV, HIV infections, RESEARCH funding, VIRAL load, ANTI-HIV agents, MONONUCLEAR leukocytes

Abstract

We measured cell-associated human immunodeficiency virus (HIV)-1 DNA (CAD) and RNA (CAR) and plasma HIV-1 RNA in blood samples from 20 children in the Children with HIV Early Antiretroviral (CHER) cohort after 7-8 years of suppressive combination antiretroviral therapy (cART). Children who initiated cART early (<2 months; n = 12) had lower HIV-1 CAD (median, 48 vs 216; P < .01) and CAR (median, 5 vs 436; P < .01) per million peripheral blood mononuclear cells than children who started later (≥ 2 months; n = 8). Plasma HIV-1 RNA levels were not significantly lower in early-treated children (0.5 vs 1.2 copies/mL; P = .16). Early treatment at <2 months of age reduces the number of HIV-infected cells and HIV CAR. [ABSTRACT FROM AUTHOR]

Published

2015

23. Severe manifestations of extrapulmonary tuberculosis in HIV-infected children initiating antiretroviral therapy before 2 years of age.

Author

Walters, Elisabetta, Duvenhage, Joanie, Draper, Heather R., Hesseling, Anneke C., Van Wyk, Susan S., Cotton, Mark F., and Rabie, Helena

Subjects

TUBERCULOSIS research, ANTIRETROVIRAL agents, HIV-positive children, MYCOBACTERIAL diseases, MENINGITIS

Abstract

Background Early initiation of antiretroviral therapy (ART) in HIV-infected infants reduces mortality and opportunistic infections including tuberculosis (TB). However, young HIV-infected children remain at high risk of TB disease following mycobacterial infection. We document the spectrum of TB disease in HIV-infected children <2 years of age on ART. Methods Retrospective cohort study; records of children <2 years of age initiating routine ART at Tygerberg Children's Hospital, Cape Town, January 2003-December 2010 were reviewed. Clinical data at ART initiation (baseline) and TB episodes after ART initiation, to June 2012, were recorded. TB immune reconstitution syndrome (TB-IRIS) and incident TB were defined as TB diagnosed within 3 months, and >3 months after, ART initiation respectively. Baseline characteristics were compared in children with TB-IRIS and those with incident TB. Results In 494 children, median follow-up time on ART was 10.7 months. Fifty-five TB treatment episodes occurred after ART initiation: 23 (42%) TB-IRIS (incidence 21.9/100 person years ( py)) and 32 (58%) incident TB (incidence 3.9/100 py). Children with TB-IRIS and those with incident TB had similar baseline characteristics. Eight of 10 cases of extrapulmonary TB were severe: 4 IRIS (2 meningitis, 1 disseminated, 1 pericarditis) and 4 incident cases (1 each miliary, meningitis, pericarditis and spinal). Fifty-one children (10%) died (mortality rate 5.96/100 py). Starting ART at <1 year of age approached significance as a risk factor for TB-IRIS (adjusted OR (AOR) 8.64, p=0.06); weight-for-age Z score <-2 predicted death (AOR 6.37, p<0.001). Conclusions Severe TB manifestations were observed among young HIV-infected children on ART. [ABSTRACT FROM AUTHOR]

Published

2014

24. Early time-limited antiretroviral therapy versus deferred therapy in South African infants infected with HIV: results from the children with HIV early antiretroviral (CHER) randomised trial.

Author

Cotton, Mark F., Violari, Avy, Otwombe, Kennedy, Panchia, Ravindre, Dobbels, Els, Rabie, Helena, Josipovic, Deirdre, Liberty, Afaaf, Lazarus, Erica, Innes, Steve, van Rensburg, Anita Janse, Pelser, Wilma, Truter, Handre, Madhi, Shabir A., Handelsman, Edward, Jean-Philippe, Patrick, McIntyre, James A., Gibb, Diana M., and Babiker, Abdel G.

Subjects

*AIDS in children, *AIDS in infants, *COMBINATION drug therapy, *CLINICAL trials, *AIDS, *ANTIRETROVIRAL agents, *AIDS treatment

Abstract

Summary: Background Interim results from the children with HIV early antiretroviral (CHER) trial showed that early antiretroviral therapy (ART) was life-saving for infants infected with HIV. In view of the few treatment options and the potential toxicity associated with lifelong ART, in the CHER trial we compared early time-limited ART with deferred ART. Methods: CHER was an open-label randomised controlled trial of HIV-infected asymptomatic infants younger than 12 weeks in two South African trial sites with a percentage of CD4-positive T lymphocytes (CD4%) of 25% or higher. 377 infants were randomly allocated to one of three groups: deferred ART (ART-Def), immediate ART for 40 weeks (ART-40W), or immediate ART for 96 weeks (ART-96W), with subsequent treatment interruption. The randomisation schedule was stratified by clinical site with permuted blocks of random sizes to balance the numbers of infants allocated to each group. Criteria for ART initiation in the ART-Def group and re-initiation after interruption in the other groups were CD4% less than 25% in infancy; otherwise, the criteria were CD4% less than 20% or Centers for Disease Control and Prevention severe stage B or stage C disease. Combination therapy of lopinavir-ritonavir, zidovudine, and lamivudine was the first-line treatment regimen at ART initiation and re-initiation. The primary endpoint was time to failure of first-line ART (immunological, clinical, or virological) or death. Comparisons were done by intention-to-treat analysis, with use of time-to-event methods. This trial is registered with ClinicalTrials.gov, number NCT00102960. Findings: 377 infants were enrolled, with a median age of 7 • 4 weeks, CD4% of 35% and HIV RNA log 5 • 7 copies per mL. Median follow-up was 4 • 8 years, 34 infants (9%) were lost to follow-up. Median time to ART initiation in the ART-Def group was 20 weeks (IQR 16-25). Time to restarting of ART after interruption was 33 weeks (26-45) in ART-40W and 70 weeks (35-109) in ART-96W; at the end of the trial, 19% of patients in ART-40W and 32% of patients in ART-96W remained off ART. Proportions of follow-up time spent on ART were 81% in the ART-Def group, 70% in the ART-40W group, and 69% in the ART-96W group 48 (38%) of 125 children in the ART-Def group, 32 (25%) of 126 in the ART-40W group, and 26 (21%) of 126 in the ART-96W group reached in the primary endpoint. The hazard ratio, relative to ART-Def, was 0 • 59 (95% CI 0 • 38-0 • 93, p=0 • 02) for ART-40W and 0 • 47 (0 • 27-0 • 76, p=0 • 002) for ART-96W. Three children in ART-Def, three in ART-40W, and one in ART-96W switched to second-line ART. Interpretation: Early time-limited ART had better clinical and immunological outcomes than deferred ART, with no evidence of excess disease progression during subsequent treatment interruption and less overall ART exposure than deferred ART. Longer time on primary ART permits longer subsequent interruption, with marginally better outcomes. Funding US National Institutes of Health. INSET: Panel: Research in context. [ABSTRACT FROM AUTHOR]

Published

2013

25. High prevalence of lipoatrophy in pre-pubertal South African children on antiretroviral therapy: a cross-sectional study.

Author

Innes, Steve, Cotton, Mark F., Haubrich, Richard, Conradie, Maria M., van Niekerk, Margaret, Edson, Clair, Rabie, Helena, Jain, Sonia, Xiaoying Sun, Zöllner, Ekkehard W., Hough, Stephen, and Browne, Sara H.

Subjects

ANTIRETROVIRAL agents, ADIPOSE tissues, STAVUDINE, AIDS in children, CROSS-sectional method, AIDS treatment

Abstract

Background: Despite changes in WHO guidelines, stavudine is still used extensively for treatment of pediatric HIV in the developing world. Lipoatrophy in sub-Saharan African children can be stigmatizing and have far-reaching consequences. The severity and extent of lipoatrophy in pre-pubertal children living in sub-Saharan Africa is unknown. Methods: In this cross-sectional study, children who were 3-12 years old, on antiretroviral therapy and pre-pubertal were recruited from a Family HIV Clinic in South Africa. Lipoatrophy was identified and graded by consensus between two HIV pediatricians using a standardized grading scale. A professional dietician performed formal dietary assessment and anthropometric measurements of trunk and limb fat. Previous antiretroviral exposures were recorded. In a Dual-Energy X-ray Absorbtiometry (DXA) substudy body composition was determined in 42 participants. Results: Among 100 recruits, the prevalence of visually obvious lipoatrophy was 36% (95% CI: 27%-45%). Anthropometry and DXA measurements corroborated the clinical diagnosis of lipoatrophy: Both confirmed significant, substantial extremity fat loss in children with visually obvious lipoatrophy, when adjusted for age and sex. Adjusted odds ratio for developing lipoatrophy was 1.9 (95% CI: 1.3 - 2.9) for each additional year of accumulated exposure to standard dose stavudine. Cumulative time on standard dose stavudine was significantly associated with reductions in biceps and triceps skin-fold thickness (p=0.008). Conclusions: The prevalence of visually obvious lipoatrophy in pre-pubertal South African children on antiretroviral therapy is high. The amount of stavudine that children are exposed to needs review. Resources are needed to enable low-and-middle-income countries to provide suitable pediatric-formulated alternatives to stavudine-based pediatric regimens. The standard stavudine dose for children may need to be reduced. Diagnosis of lipoatrophy at an early stage is important to allow timeous antiretroviral switching to arrest progression and avoid stigmatization. Diagnosis using visual grading requires training and experience, and DXA and comprehensive anthropometry are not commonly available. A simple objective screening tool is needed to identify early lipoatrophy in resourcelimited settings where specialized skills and equipment are not available. [ABSTRACT FROM AUTHOR]

Published

2012

26. Early Antiretroviral Therapy and Mortality among HIV-Infected Infants.

Author

Violari, Avy, Cotton, Mark F., Gibb, Diana M., Babiker, Abdel G., Steyn, Jan, Madhi, Shabir A., Jean-Philippe, Patrick, and McIntyre, James A.

Subjects

*CLINICAL trials, *INFANT mortality, *HIV, *ANTIRETROVIRAL agents, *AZIDOTHYMIDINE, *INFANT health

Abstract

The article presents a clinical trial which investigated antiretroviral treatment strategies in the Children with HIV Early Antiretroviral Therapy trial. Infants with HIV from six to 12 weeks of age with a CD4 lymphocyte percentage of 25% or more were randomly assigned to receive lopinavir-ritonavir, zidovudine, and lamivudine when their CD4 percentage decreased to less than 20% or clinical criteria were met or limited antiretroviral therapy until 1 year of age or 2 years of age. Researchers found that early antiretroviral therapy and early HIV diagnosis reduced infant mortality by 76% and HIV progression by 75%.

Published

2008

27. Bacterial Disease and Antimicrobial Susceptibility Patterns in HIV-Infected, Hospitalized Children: A Retrospective Cohort Study.

Author

Jaspan, Heather B., Huang, Lyen C., Cotton, Mark F., Whitelaw, Andrew, and Myer, Landon

Subjects

BACTERIAL disease treatment, ANTI-infective agents, DRUG resistance in microorganisms, HIV prevention, ANTIRETROVIRAL agents, HOSPITAL care of children, METHICILLIN resistance

Abstract

Background: Serious bacterial infections are a major source of morbidity and mortality in HIV-infected children. The spectrum of disease is wide, and responsible organisms vary according to setting. The use of antibiotic prophylaxis and the emergence of multi-drug resistant bacteria necessitate examination of responsible organisms and their antibiotic susceptibility. Methodology/Principal Findings: A retrospective cohort study of all HIV-positive pediatric admissions at an urban public sector hospital in Cape Town between January 2002 and June 2006 was conducted. Children between the ages of one month and nine years with laboratory confirmed HIV status, serious bacterial infection, and a hospital length of stay of 5 days or more, were eligible for inclusion. Organisms isolated from blood, urine, and cerebral spinal fluid cultures and their antimicrobial susceptibility were examined, and compared according to timing of isolation to distinguish nosocomial versus community-acquired. One hundred and forty-one children were identified (median age 1.2 years), 39% of whom were on antiretrovirals started before or during this hospitalization. Bacterial infections involved all organ systems, however pneumonia was most common (67%). S. pneumoniae and S. aureus were the most common gram positive and K. pneumoniae was the most common gram negative organism. K pneumoniae isolates were resistant to many first and second line antibiotics, and were all considered nosocomial. All S. aureus isolates were methicillin resistant, some of which were community-acquired. Conclusions/Significance: Bacterial infections are an important source of co-morbidity in HIV-infected children in resourcelimited settings. Clinicians should have a low threshold to initiate antibiotics in children requiring hospitalization. Broad-spectrum antibiotics should be used judiciously. Clinicians caring for HIV-infected children should be cognizant of the most common organisms affecting such children, and of their local antimicrobial susceptibilities, when treating empirically for serious bacterial infections. [ABSTRACT FROM AUTHOR]

Published

2008

28. Ensuring the Involvement of Children in the Evaluation of New Tuberculosis Treatment Regimens.

Author

Burman, William J., Cotton, Mark F., Gibb, Diana M., Walker, A. Sarah, Vernon, Andrew A., and Donald, Peter R.

Subjects

*TUBERCULOSIS, *PEDIATRIC therapy, *CHILDREN'S health, *ANTIRETROVIRAL agents, *MEDICINE, *PEDIATRICS

Abstract

William Burman and colleagues review the barriers to involving children in studies of new tuberculosis treatments and recommend strategies for overcoming these barriers. [ABSTRACT FROM AUTHOR]

Published

2008

29. Clinical presentation and outcome of Tuberculosis in Human Immunodeficiency Virus infected children on anti-retroviral therapy.

Author

Walters, Elisabetta, Cotton, Mark F., Rabie, Helena, Schaaf, H. Simon, Walters, Lourens O., and Marais, Ben J.

Subjects

TUBERCULOSIS, HIV, EPIDEMICS, ANTIRETROVIRAL agents, JUVENILE diseases, CHILDREN'S health

Abstract

Background: The tuberculosis (TB) and human immunodeficiency virus (HIV) epidemics are poorly controlled in sub-Saharan Africa, where highly active antiretroviral treatment (HAART) has become more freely available. Little is known about the clinical presentation and outcome of TB in HIV-infected children on HAART. Methods: We performed a comprehensive file review of all children who commenced HAART at Tygerberg Children's Hospital from January 2003 through December 2005. Results: Data from 290 children were analyzed; 137 TB episodes were recorded in 136 children; 116 episodes occurred before and 21 after HAART initiation; 10 episodes were probably related to immune reconstitution inflammatory syndrome (IRIS). The number of TB cases per 100 patient years were 53.3 during the 9 months prior to HAART initiation, and 6.4 during post HAART follow-up [odds ratio (OR) 16.6; 95% confidence interval (CI) 12.5-22.4]. A positive outcome was achieved in 97/137 (71%) episodes, 6 (4%) cases experienced no improvement, 16 (12%) died and the outcome could not be established in 18 (13%). Mortality was less in children on HAART (1/21; 4.8%) compared to those not on HAART (15/116; 12.9%). Conclusion: We recorded an extremely high incidence of TB among HIV-infected children, especially prior to HAART initiation. Starting HAART at an earlier stage is likely to reduce morbidity and mortality related to TB, particularly in TB-endemic areas. Management frequently deviated from standard guidelines, but outcomes in general were good. [ABSTRACT FROM AUTHOR]

Published

2008

30. HIV-1 Persistence in Children during Suppressive ART.

Author

Katusiime, Mary Grace, Van Zyl, Gert U., Cotton, Mark F., and Kearney, Mary F.

Subjects

HIV, LANDSCAPES in art, ADULTS, ANTIRETROVIRAL agents, COMORBIDITY

Abstract

There is a growing number of perinatally HIV-1-infected children worldwide who must maintain life-long ART. In early life, HIV-1 infection is established in an immunologically inexperienced environment in which maternal ART and immune dynamics during pregnancy play a role in reservoir establishment. Children that initiated early antiretroviral therapy (ART) and maintained long-term suppression of viremia have smaller and less diverse HIV reservoirs than adults, although their proviral landscape during ART is reported to be similar to that of adults. The ability of these early infected cells to persist long-term through clonal expansion poses a major barrier to finding a cure. Furthermore, the effects of life-long HIV persistence and ART are yet to be understood, but growing evidence suggests that these individuals are at an increased risk for developing non-AIDS-related comorbidities, which underscores the need for an HIV cure. [ABSTRACT FROM AUTHOR]

Published

2021

31. The challenges of success: adolescents with perinatal HIV infection.

Author

Mofenson, Lynne M and Cotton, Mark F

Subjects

*HIV infections, *THERAPEUTICS, *HIV-positive youth, *HIV-positive children, *EPIDEMICS, *PREVENTION of communicable diseases in children, *ANTIRETROVIRAL agents, *ADULTS

Abstract

The great success in the prevention and treatment of pediatric HIV in high resource countries, and now in low resource countries, has changed the face of the HIV epidemic in children from one of near certain mortality to that of a chronic disease. However, these successes pose new challenges as perinatally HIV-infected youth survive into adulthood. Increased survival of HIV-infected children is associated with challenges in maintaining adherence to what is likely life-long therapy, and in selecting successive antiretroviral drug regimens, given the limited availability of pediatric formulations, limitations in pharmacokinetic and safety data of drugs in children, and the development of extensive drug resistance in multi-drug-experienced children. Pediatric HIV care must now focus on morbidity related to long-term HIV infection and its treatment. Survival into adulthood of perinatally HIV-infected youth in high resource countries provides important lessons about how the epidemic will change with increasing access to antiretroviral therapy for children in low resource countries. This series of papers will focus on issues related to management of perinatally infected youth and young adults [ABSTRACT FROM AUTHOR]

Published

2013

32. Childhood pneumonia: the role of viruses.

Author

Pitcher, Richard D., Lombard, Carl J., Cotton, Mark F., Beningfield, Stephen J., Workman, Lesley, and Zar, Heather J.

Subjects

CHEST X rays, HIV-positive children, AFRICANS, ANTIRETROVIRAL agents, RESPIRATORY infections in children, HEALTH

Abstract

Background There is limited knowledge of chest radiographic abnormalities over time in HIV-infected children in resource-limited settings. Objective To investigate the natural history of chest radiographic abnormalities in HIV-infected African children, and the impact of antiretroviral therapy (ART). Methods Prospective longitudinal study of the association of chest radiographic findings with clinical and immunological parameters. Chest radiographs were performed at enrolment, 6-monthly, when initiating ART and if indicated clinically. Radiographic abnormalities were classified as normal, mild or moderate severity and considered persistent if present for 6 consecutive months or longer. An ordinal multiple logistic regression model assessed the association of enrolment and timedependent variables with temporal radiographic findings. Results 258 children (median (IQR) age: 28 (13-51) months; median CD4+%: 21 (15-24)) were followed for a median of 24 (18-42) months. 70 (27%) were on ART at enrolment; 130 (50%) (median age: 33 (18-56) months) commenced ART during the study. 154 (60%) had persistent severe radiographic abnormalities, with median duration 18 (6-24) months. Among children on ART, 69% of radiographic changes across all 6-month transition periods were improvements, compared with 45% in those not on ART. Radiographic severity was associated with previous radiographic severity (OR=120.80; 95% CI 68.71 to 212.38), lack of ART (OR=1.72; 95% CI 1.29 to 2.27), enrolment age <18 months (OR=1.39; 95% CI 1.06 to 1.83), diffuse, severe radiographic abnormality at enrolment (OR=2.18; 95% CI 1.33 to 3.56), hospitalisation for lower respiratory tract infection during the previous 6 months (OR=1.88; 95% CI 1.06 to 3.30) and length of followup: at 18-24 months (OR=0.66; 95% CI 0.49 to 0.90), and at 30-54 months (OR=0.42; 95% CI 0.32 to 0.56). Conclusions Most children had severe radiographic abnormalities persisting for at least 18 months. ART was beneficial, reducing the risk of radiographic deterioration or increasing the likelihood of radiological improvement. [ABSTRACT FROM AUTHOR]

Published

2015

33. Antiretroviral Therapy in Children with Tuberculosis: Progress toward Defining the Issues.

Author

Cotton, Mark F., Rabie, Helena, and van Zyl, Gert U.

Subjects

*MEDICAL research, *ANTIRETROVIRAL agents, *TUBERCULOSIS treatment, *RIFAMPIN, *FAILURE to thrive syndrome, *THERAPEUTICS

Abstract

The authors reflect on the study that evaluates the effectiveness of antiretroviral therapy in children with tuberculosis. They contend that children cotreated for tuberculosis had significantly poorer virological outcomes due to factors such as failure to thrive and respiratory symptoms. The authors cite the lack of antiretroviral options and the lack of adequate data on children who require cotreatment with rifampicin and antiretroviral therapy.

Published

2010

34. Intact HIV Proviruses Persist in Children Seven to Nine Years after Initiation of Antiretroviral Therapy in the First Year of Life.

Author

Katusiime, Mary Grace, Halvas, Elias K., Wright, Imogen, Joseph, Kevin, Bale, Michael J., Kirby-McCullough, Bronwyn, Engelbrecht, Susan, Wei Shao, Wei-Shau Hu, Cotton, Mark F., Mellors, John W., Kearney, Mary F., and van Zyl, Gert U.

Subjects

*ANTIRETROVIRAL agents, *CLONE cells

Abstract

In adults starting antiretroviral therapy (ART) during acute infection, 2% of proviruses that persist on ART are genetically intact by sequence analysis. In contrast, a recent report in children treated early failed to detect sequence-intact proviruses. In another cohort of children treated early, we sought to detect and characterize proviral sequences after 6 to 9 years on suppressive ART. Peripheral blood mononuclear cells (PBMC) from perinatally infected children from the Children with HIV Early antiRetroviral (CHER) study were analyzed. Nearly full-length proviral amplification and sequencing (NFL-PAS) were performed at one time point after 6 to 9 years on ART. Amplicons with large internal deletions were excluded (<9 kb). All amplicons of ≥9 kb were sequenced and analyzed through a bioinformatic pipeline to detect indels, frameshifts, or hypermutations that would render them defective. In eight children who started ART at a median age of 5.4 months (range, 2.0 to 11.1 months), 733 single NFL-PAS amplicons were generated. Of these, 534 (72.9%) had large internal deletions, 174 (23.7%) had hypermutations, 15 (1.4%) had small internal deletions, 3 (1.0%) had deletions in the packaging signal/major splice donor site, and 7 (1.0%) were sequence intact. These 7 intact sequences were from three children who initiated ART after 2.3 months of age, one of whom had two identical intact sequences, suggestive of a cell clone harboring a replication-competent provirus. No intact proviruses were detected in four children who initiated ART before 2.3 months of age. Rare, intact proviruses can be detected in children who initiate ART after 2.3 months of age and are probably, as in adults, maintained by clonal expansion of cells infected before ART initiation. [ABSTRACT FROM AUTHOR]

Published

2020

35. Neurodevelopment at 11 months after starting antiretroviral therapy within 3 weeks of life.

Author

Laughton, Barbara, Naidoo, Shalena, Dobbels, Els F.M.T., Boivin, Michael J., van Rensburg, Anita Janse, Glashoff, Richard H., van Zyl, Gert U., Kruger, Mariana, and Cotton, Mark F.

Subjects

*ANTIRETROVIRAL agents, *NEURAL development, *CYTOMEGALOVIRUS diseases, *BIRTH weight, *VERTICAL transmission (Communicable diseases)

Abstract

Background: Antiretroviral therapy (ART) started between 7 and 12 weeks of age improves neurodevelopmental outcomes in HIV-infected (HIV+) infants, but the impact of even earlier initiation is not yet described. Objectives: We assessed the early neurodevelopment of HIV+ infants who started ART within 21 days of life. Method: Participants were enrolled from the public sector birth HIV-diagnosis programme. Inclusion criteria included the following: birth weight > 2000 g, infant commencing ART < 6 weeks and no infant cytomegalovirus disease. Antiretroviral therapy included Zidovudine/Lamivudine/Nevirapine for the first 2 weeks, the latter then replaced by Lopinavir/Ritonavir. Once body weight > 3 kg and gestational age > 44 weeks, Abacavir replaced Zidovudine. The Griffiths mental development scales (GMDS) were administered at 10–12 months. Results: Of 29 infants assessed, 23 (79%) were girls. Mean birth weight was 3002 ± 501 g. Twenty-four mothers (83%) received ART during pregnancy. Seven (24%) infants were diagnosed HIV+ within 48 h of birth. Median [interquartile range] viral load (VL) at diagnosis was 3904 [259–16 922] copies/mL, age starting ART was 6.0 [3–10] days and age at VL suppression was 19.1 [15–36] weeks. At the GMDS assessment, nine (31%) participants had detectable VL and 26 (90%) had World Health Organization (WHO) clinical stage I disease. The GMDS was performed at a mean age of 11.5 ± 0.8 months. Mean quotients were within the average range: Global Griffiths score was 103.6 ± 10.9 and mean quotients on the subscales ranged from lowest 95.9 ± 13.4 for locomotor to highest 112.8 ± 11.3 for hearing-and-language. Conclusion: Preliminary findings in this small group suggest that early neurodevelopmental scores are within the normal range in infants with perinatal HIV infection who started ART at a median of 6 days. [ABSTRACT FROM AUTHOR]

Published

2019

36. No evidence of HIV replication in children on antiretroviral therapy.

Author

Van Zyl, Gert U., Katusiime, Mary Grace, Wiegand, Ann, McManus, William R., Bale, Michael J., Halvas, Elias K., Luke, Brian, Boltz, Valerie F., Spindler, Jonathan, Laughton, Barbara, Engelbrecht, Susan, Coffin, John M., Cotton, Mark F., Wei Shao, Mellors, John W., Kearney, Mary F., and Shao, Wei

Subjects

*VIRAL replication, *ANTIRETROVIRAL agents, *HIV, *HIV-positive children, *VIREMIA, *CLINICAL trials, *COMPARATIVE studies, *HIV infections, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *EVALUATION research, *PHYSIOLOGY

Abstract

It remains controversial whether current antiretroviral therapy (ART) fully suppresses the cycles of HIV replication and viral evolution in vivo. If replication persists in sanctuary sites such as the lymph nodes, a high priority should be placed on improving ART regimes to target these sites. To investigate the question of ongoing viral replication on current ART regimens, we analyzed HIV populations in longitudinal samples from 10 HIV-1-infected children who initiated ART when viral diversity was low. Eight children started ART at less than ten months of age and showed suppression of plasma viremia for seven to nine years. Two children had uncontrolled viremia for fifteen and thirty months, respectively, before viremia suppression, and served as positive controls for HIV replication and evolution. These latter 2 children showed clear evidence of virus evolution, whereas multiple methods of analysis bore no evidence of virus evolution in any of the 8 children with viremia suppression on ART. Phylogenetic trees simulated with the recently reported evolutionary rate of HIV-1 on ART of 6 × 10-4 substitutions/site/month bore no resemblance to the observed data. Taken together, these data refute the concept that ongoing HIV replication is common with ART and is the major barrier to curing HIV-1 infection. [ABSTRACT FROM AUTHOR]

Published

2017

37. Nevirapine versus Ritonavir-Boosted Lopinavir for HIV-Infected Children.

Author

Violari, Avy, Lindsey, Jane C., Hughes, Michael D., Mujuru, Hilda A., Barlow-Mosha, Linda, Kamthunzi, Portia, Chi, Benjamin H., Cotton, Mark F., Moultrie, Harry, Khadse, Sandhya, Schimana, Werner, Bobat, Raziya, Purdue, Lynette, Eshleman, Susan H., Abrams, Elaine J., Millar, Linda, Petzold, Elizabeth, Mofenson, Lynne M., Jean-Philippe, Patrick, and Palumbo, Paul

Subjects

*NEVIRAPINE, *ANTIRETROVIRAL agents, *HIV infection transmission, *LOPINAVIR-ritonavir, *AZIDOTHYMIDINE, *HIV-positive children

Abstract

Background: Nevirapine-based antiretroviral therapy is the predominant (and often the only) regimen available for children in resource-limited settings. Nevirapine resistance after exposure to the drug for prevention of maternal-to-child human immunodeficiency virus (HIV) transmission is common, a problem that has led to the recommendation of ritonavir-boosted lopinavir in such settings. Regardless of whether there has been prior exposure to nevirapine, the performance of nevirapine versus ritonavir-boosted lopinavir in young children has not been rigorously established. Methods: In a randomized trial conducted in six African countries and India, we compared the initiation of HIV treatment with zidovudine, lamivudine, and either nevirapine or ritonavir-boosted lopinavir in HIV-infected children 2 to 36 months of age who had no prior exposure to nevirapine. The primary end point was virologic failure or discontinuation of treatment by study week 24. Results: A total of 288 children were enrolled; the median percentage of CD4+ T cells was 15%, and the median plasma HIV type 1 (HIV-1) RNA level was 5.7 log10 copies per milliliter. The percentage of children who reached the primary end point was significantly higher in the nevirapine group than in the ritonavir-boosted lopinavir group (40.8% vs. 19.3%; P<0.001). Among the nevirapine-treated children with virologic failure for whom data on resistance were available, more than half (19 of 32) had resistance at the time of virologic failure. In addition, the time to a protocol-defined toxicity end point was shorter in the nevirapine group (P=0.04), as was the time to death (P=0.06). Conclusions: Outcomes were superior with ritonavir-boosted lopinavir among young children with no prior exposure to nevirapine. Factors that may have contributed to the suboptimal results with nevirapine include elevated viral load at baseline, selection for nevirapine resistance, background regimen of nucleoside reverse-transcriptase inhibitors, and the standard ramp-up dosing strategy. The results of this trial present policymakers with difficult choices. (Funded by the National Institute of Allergy and Infectious Diseases and others; P1060 ClinicalTrials.gov number, NCT00307151.) [ABSTRACT FROM PUBLISHER]

Published

2012

38. Antiretroviral Treatment for Children with Peripartum Nevirapine Exposure.

Author

Palumbo, Paul, Lindsey, Jane C., Hughes, Michael D., Cotton, Mark F., Bobat, Raziya, Meyers, Tammy, Bwakura-Dangarembizi, Mutsawashe, Chi, Benjamin H., Musoke, Philippa, Kamthunzi, Portia, Schimana, Werner, Purdue, Lynette, Eshleman, Susan H., Abrams, Elaine J., Millar, Linda, Petzold, Elizabeth, Mofenson, Lynne M., Jean-Philippe, Patrick, and Violari, Avy

Subjects

*NEVIRAPINE, *HIV infection transmission, *ANTIRETROVIRAL agents, *VIROLOGY

Abstract

Background: Single-dose nevirapine is the cornerstone of the regimen for prevention of mother-to-child transmission of human immunodeficiency virus (HIV) in resource-limited settings, but nevirapine frequently selects for resistant virus in mothers and children who become infected despite prophylaxis. The optimal antiretroviral treatment strategy for children who have had prior exposure to single-dose nevirapine is unknown. Methods: We conducted a randomized trial of initial therapy with zidovudine and lamivudine plus either nevirapine or ritonavir-boosted lopinavir in HIV-infected children 6 to 36 months of age, in six African countries, who qualified for treatment according to World Health Organization (WHO) criteria. Results are reported for the cohort that included children exposed to single-dose nevirapine prophylaxis. The primary end point was virologic failure or discontinuation of treatment by study week 24. Enrollment in this cohort was terminated early on the recommendation of the data and safety monitoring board. Results: A total of 164 children were enrolled. The median percentage of CD4+ lymphocytes was 19%; a total of 56% of the children had WHO stage 3 or 4 disease. More children in the nevirapine group than in the ritonavir-boosted lopinavir group reached a primary end point (39.6% vs. 21.7%; weighted difference, 18.6 percentage-points; 95% confidence interval, 3.7 to 33.6; nominal P=0.02). Baseline resistance to nevirapine was detected in 18 of 148 children (12%) and was predictive of treatment failure. No significant between-group differences were seen in the rate of adverse events. Conclusions: Among children with prior exposure to single-dose nevirapine for perinatal prevention of HIV transmission, antiretroviral treatment consisting of zidovudine and lamivudine plus ritonavir-boosted lopinavir resulted in better outcomes than did treatment with zidovudine and lamivudine plus nevirapine. Since nevirapine is used for both treatment and perinatal prevention of HIV infection in resource-limited settings, alternative strategies for the prevention of HIV transmission from mother to child, as well as for the treatment of HIV infection, are urgently required. (Funded by the National Institutes of Health; ClinicalTrials.gov number, NCT00307151.) N Engl J Med 2010;363:1510-20. [ABSTRACT FROM AUTHOR]

Published

2010