| Literature DB >> 25598835 |
Kirsten A Donald1, Kathleen G Walker2, Tracy Kilborn3, Henri Carrara4, Nelleke G Langerak5, Brian Eley6, Jo M Wilmshurst2.
Abstract
BACKGROUND: The Human Immune Deficiency Virus (HIV) can manifest neurologically in both adults and children. Early invasion of the central nervous system by the virus, affecting the developing brain, is believed to result in the most common primary HIV-related neurological complication, HIV Encephalopathy (HIVE). In countries such as South Africa where many children have not been initiated on antiretroviral treatment early, HIVE remains a significant clinical problem.Entities:
Keywords: Brain; Children; Developmental delay; HIV encephalopathy; MRI
Year: 2015 PMID: 25598835 PMCID: PMC4297380 DOI: 10.1186/s12981-014-0042-7
Source DB: PubMed Journal: AIDS Res Ther ISSN: 1742-6405 Impact factor: 2.250
Figure 1Study algorithm.
Background information for children with HIVE
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| Gender (n = 87) | ||
| Male | 51 | 59 |
| Female | 36 | 41 |
| Age group at examination (n = 87) | ||
| <2 years | 16 | 18 |
| 2 – 4 years | 24 | 28 |
| 5 – 9 years | 36 | 41 |
| 10 – 14 years | 11 | 13 |
| Age at ART commencement (n = 87) | ||
| <12 months | 38 | 44 |
| 12 – 36months | 33 | 38 |
| >36 months | 14 | 16 |
| Not reported | 2 | 2 |
| Developmental milestone walking (n = 75) | ||
| On time | 15 | 20 |
| Delayed (>18 months) | 60 | 80 |
| Not old enough to tell | 5 | N/A |
| Not reported | 7 | N/A |
| Developmental milestone talking (n = 72) | ||
| On time | 18 | 25 |
| Delayed (>18 months) | 54 | 75 |
| Not old enough to tell | 4 | N/A |
| Not reported | 11 | N/A |
| Home environment (n = 87) | ||
| home | 49 | 56 |
| Institution, orphanage, foster home | 13 | 15 |
| bio foster (adopted by family member) | 20 | 23 |
| other foster | 4 | 5 |
| Not reported | 1 | 1 |
| School (n = 87) | ||
| Mainstream pre-school | 32 | 37 |
| Mainstream school | 35 | 40 |
| Special school/care center | 4 | 5 |
| None | 7 | 8 |
| Not reported | 9 | 10 |
| Repeating grades | ||
| Yes | 37 | 43 |
| No | 27 | 31 |
| Not reported | 23 | 26 |
Clinical findings for children with HIVE
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| Weight | ||
| Normal | 43 | 49 |
| 3rd – 10th centile | 16 | 18 |
| <3rd centile | 28 | 32 |
| Height | ||
| Normal | 24 | 28 |
| 3rd – 10th centile | 20 | 23 |
| <3rd centile | 26 | 30 |
| Not recorded | 17 | 20 |
| Physical exam | ||
| Spastic diplegia/long tract signs | 55 | 63 |
| Microcephaly | 42 | 48 |
| Learning Difficulties | 6 | 7 |
| Peripheral Neuropathy | 1 | 1 |
| Visual impairment | 1 | 1 |
| Hearing impairment | 2 | 2 |
| Ears | ||
| Normal | 36 | 41 |
| Acute otitis media | 7 | 8 |
| Chronic suppurative otitis media | 26 | 30 |
| not examined/recorded | 16 | 18 |
Neuroimaging findings
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| Imaging | ||
| Global Atrophy | 10 | 20 |
| Basal Ganglia Calcifications | 4 | 8 |
| White Matter Signal Change | 9 | 18 |
| White Matter Volume Loss | 12 | 24 |
| Grey Matter Volume Loss | 4 | 8 |
| Thinning of Corpus Callosum | 9 | 18 |
| Other | 6 | 12 |
| Normal | 14 | 29 |
Figure 2Axial CT Brain showing bilateral basal ganglia calcification and cerebral shrinkage in a 1year old child with HIVE.
Figure 3Axial T2 (a) and FLAIR (b) images of an HIV-positive child showing bilateral symmetrical high signal in the periventricular white matter with normal basal ganglia. Prominence of the cerebral sulci implies volume loss.