AI Article Synopsis

  • The study aimed to analyze imaging anomalies in black African children with developmental delays, focusing on those aged 1 month to 6 years who underwent brain scans.
  • About 94 children participated, with a significant portion having experienced perinatal asphyxia, and imaging tests showed high rates of abnormal findings, especially cerebral atrophy.
  • The research highlighted that while a majority had imaging abnormalities linked to hypoxic-ischemic events, there was no direct correlation between the severity of developmental delays and the occurrence of these anomalies.

Article Abstract

Background: The purpose of this study was to describe the anomalies observed on imaging for developmental delay in black African children.

Methods: It was a descriptive cross-sectional study, which included children aged between 1 month to 6 years with developmental delay and had done a brain MRI and/or CT scan.

Results: We included 94 children, 60.6% of whom were males. The mean age was 32.5 ± 6.8 months. A history of perinatal asphyxia found in 55.3% of cases. According to the Denver developmental II scale, profound developmental delay observed in 35.1% of cases, and severe developmental delay in 25.5%. DD was isolated in 2.1% of cases and associated with cerebral palsy, pyramidal syndrome, and microcephaly in respectively 83%, 79.8%, and 46.8% of cases. Brain CT scan and MRI accounted for 85.1% and 14.9% respectively. The tests were abnormal in 78.7% of the cases, and cerebral atrophy was the preponderant anomaly (cortical atrophy = 80%, subcortical atrophy = 69.3%). Epileptic patients were 4 times more likely to have abnormal brain imaging (OR = 4.12 and p = 0.05),. We did not find a link between the severity of psychomotor delay and the presence of significant anomalies in imaging.

Conclusion: In our context, there is a high prevalence of organic anomalies in the imaging of psychomotor delay, which were dominated by cerebral atrophy secondary to hypoxic ischemic events.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10398464PMC
http://dx.doi.org/10.4314/ahs.v23i1.73DOI Listing

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