The impact of HIV infection on skeletal maturity in peripubertal children in Zimbabwe: a cross-sectional study
The impact of HIV infection on skeletal maturity in peripubertal children in Zimbabwe: a cross-sectional study
Introduction: HIV infection and its treatment compromises skeletal development (growth and maturation). Skeletal maturity is assessed as bone age (BA) on hand and wrist radiographs. BA younger than chronological age (CA) indicates delayed development. We conducted a cross-sectional study to determine differences between BA and CA (i.e., skeletal maturity deviation [SMD]), and risk factors associated with SMD in peripubertal children with and without HIV established on antiretroviral therapy (ART) including use of tenofovir disoproxil fumarate (TDF).
Methods: children with HIV taking ART for at least two years and a comparison group of HIV-negative children, aged 8–16 years and frequency-matched by age and sex, were recruited from HIV clinics and local schools in the same catchment area, in Harare, Zimbabwe. BA was assessed from non-dominant hand-wrist radiographs using the Tanner Whitehouse 3 method. Negative SMD values correspond to delayed development, i.e., BA younger than CA. Multivariable linear regression models determined factors associated with SMD overall, and in children with HIV.
Results: in total, 534 participants (54% males) were included; by design CA was similar in males and females, whether living with or without HIV. Mean (SD) SMD was more negative in CWH than in HIV-negative children in both males [-1.4(1.4) vs. -0.4(1.1) years] and females [-1.1(1.3) vs. -0.0(1.2) years]. HIV infection and weight-for-age Z-score<-2 were associated with more negative SMD in both males and females after adjusting for socio-economic status, orphanhood, pubertal stage, and calcium intake. Age at ART initiation was associated with SMD in both males and females with those starting ART later more delayed: starting ART aged 4–8 years 1.14 (-1.84, -0.43), or over 8 years 1.47 (-2.30, -0.65) (p-value for trend < 0.001). Similar non-significant trends were seen in males. TDF exposure TDF exposure whether < 4years or ≥ 4 years was not associated with delayed development.
Conclusion: perinatally-acquired HIV infection and being underweight were independently associated with delayed skeletal maturation in both males and females. Starting ART later was independently associated with skeletal maturation delay in CWH. Given the known effects of delayed development on later health, it is important to find interventions to ensure healthy weight gain through early years and in CWH to initiate ART as early as possible.
Adolescent, Age Determination by Skeleton, Anti-HIV Agents/therapeutic use, Bone Development/drug effects, Case-Control Studies, Child, Cross-Sectional Studies, Female, HIV Infections/drug therapy, Humans, Male, Risk Factors, Tenofovir/therapeutic use, Zimbabwe/epidemiology, Adolescence, Puberty, Africa, HIV, Bone age, Children
Kowo-Nyakoko, Farirayi
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Gregson, Celia L.
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Westbury, Leo D.
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Madanhire, Tafadzwa
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Offiah, Amaka C.
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Micklesfield, Lisa K.
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Ferrand, Rashida Abbas
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Rehman, Andrea M.
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Ward, Kate A.
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Kowo-Nyakoko, Farirayi
51536d0c-2313-404d-bd3b-881b741d540f
Gregson, Celia L.
1df38b9c-c5c0-4444-8cee-dad379f2ab8d
Westbury, Leo D.
08fbb4e9-305c-4724-bd0c-b963a5054229
Madanhire, Tafadzwa
24f2c09f-1ee3-4674-9bf6-e201e1d17f6d
Offiah, Amaka C.
ef1703e9-d951-4499-adb7-292bbd031bbd
Micklesfield, Lisa K.
e73dd95b-ce79-4dc4-b0be-a8935eb069c8
Ferrand, Rashida Abbas
321e8fc2-c095-4c0f-9fec-9840e8feeddd
Rehman, Andrea M.
70df2a8e-aa95-4942-ad10-4644280f13bf
Ward, Kate A.
39bd4db1-c948-4e32-930e-7bec8deb54c7
Kowo-Nyakoko, Farirayi, Gregson, Celia L., Westbury, Leo D., Madanhire, Tafadzwa, Offiah, Amaka C., Micklesfield, Lisa K., Ferrand, Rashida Abbas, Rehman, Andrea M. and Ward, Kate A.
(2024)
The impact of HIV infection on skeletal maturity in peripubertal children in Zimbabwe: a cross-sectional study.
BMC Pediatrics, 24 (1), [480].
(doi:10.1186/s12887-024-04965-y).
Abstract
Introduction: HIV infection and its treatment compromises skeletal development (growth and maturation). Skeletal maturity is assessed as bone age (BA) on hand and wrist radiographs. BA younger than chronological age (CA) indicates delayed development. We conducted a cross-sectional study to determine differences between BA and CA (i.e., skeletal maturity deviation [SMD]), and risk factors associated with SMD in peripubertal children with and without HIV established on antiretroviral therapy (ART) including use of tenofovir disoproxil fumarate (TDF).
Methods: children with HIV taking ART for at least two years and a comparison group of HIV-negative children, aged 8–16 years and frequency-matched by age and sex, were recruited from HIV clinics and local schools in the same catchment area, in Harare, Zimbabwe. BA was assessed from non-dominant hand-wrist radiographs using the Tanner Whitehouse 3 method. Negative SMD values correspond to delayed development, i.e., BA younger than CA. Multivariable linear regression models determined factors associated with SMD overall, and in children with HIV.
Results: in total, 534 participants (54% males) were included; by design CA was similar in males and females, whether living with or without HIV. Mean (SD) SMD was more negative in CWH than in HIV-negative children in both males [-1.4(1.4) vs. -0.4(1.1) years] and females [-1.1(1.3) vs. -0.0(1.2) years]. HIV infection and weight-for-age Z-score<-2 were associated with more negative SMD in both males and females after adjusting for socio-economic status, orphanhood, pubertal stage, and calcium intake. Age at ART initiation was associated with SMD in both males and females with those starting ART later more delayed: starting ART aged 4–8 years 1.14 (-1.84, -0.43), or over 8 years 1.47 (-2.30, -0.65) (p-value for trend < 0.001). Similar non-significant trends were seen in males. TDF exposure TDF exposure whether < 4years or ≥ 4 years was not associated with delayed development.
Conclusion: perinatally-acquired HIV infection and being underweight were independently associated with delayed skeletal maturation in both males and females. Starting ART later was independently associated with skeletal maturation delay in CWH. Given the known effects of delayed development on later health, it is important to find interventions to ensure healthy weight gain through early years and in CWH to initiate ART as early as possible.
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s12887-024-04965-y
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Accepted/In Press date: 24 July 2024
e-pub ahead of print date: 27 July 2024
Keywords:
Adolescent, Age Determination by Skeleton, Anti-HIV Agents/therapeutic use, Bone Development/drug effects, Case-Control Studies, Child, Cross-Sectional Studies, Female, HIV Infections/drug therapy, Humans, Male, Risk Factors, Tenofovir/therapeutic use, Zimbabwe/epidemiology, Adolescence, Puberty, Africa, HIV, Bone age, Children
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Local EPrints ID: 493019
URI: http://eprints.soton.ac.uk/id/eprint/493019
ISSN: 1471-2431
PURE UUID: 2c212c5e-197e-4fe2-b618-e4051d978bcb
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Date deposited: 21 Aug 2024 17:16
Last modified: 22 Aug 2024 01:47
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Contributors
Author:
Farirayi Kowo-Nyakoko
Author:
Celia L. Gregson
Author:
Leo D. Westbury
Author:
Tafadzwa Madanhire
Author:
Amaka C. Offiah
Author:
Lisa K. Micklesfield
Author:
Rashida Abbas Ferrand
Author:
Andrea M. Rehman
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