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The Diagnostic Utility of Elevation in Cerebrospinal Fluid B2-Microglobulin in HIV-1 Dementia
Neurol 42:1707-1712, McArthur,J.C.,et al, 1992
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Article Abstract
We measured serum and CSF B2-microglobulin(B2M)levels in HIV-1 seropositive individuals with and without dementia to determine the frequency and diagnostic utility of elevation of CSF B2M.We compared 34 samples from 27 patients with HIV-1 dementia with 110 samples from 54 HIV- 1 seropositive particpiants in the Multicenter AIDS Cohort Study,none of whom had progressive dementia.Neurosyphilis and CNS opportunistic processes were excluded in all subjects.We stratified the nondemented subjects by duration of HIV seropositivity and peripheral blood CD4 count. Compared with the nondemented group,demented subjects had significantly higher CSF total protein,IgG%,and CSF albumin/serum albumin ratios.A highly significant association was found between elevated CSF B2M and reduced CD4 count(p<0.0001).No significant differences were noted between the demented and nondemented groups in CSF WBC count or in the frequency of CSF HIV-1 isolation.The mean CSF B2M was 1.9 mg/l in the nondemented subjects comapred with 4.2 mg/l in those with dementia(p<0.0001).We derived a cutoff of 3.8 mg/l from the distribution of CSF B2M in the nondemented group.The determination of CSF B2M had a sensitivity of 44%, specificity of 90%,and a positive predictive value of 88%for diagnosis of HIV dementia when compared with nondemented subjects with CD4 counts<200. In those without dementia,there was a strong correlation between serum and CSF B2M(r=0.50,p<0.0001),but in demented subjects CSF B2M was elevated independently of serum levels,suggesting that CSF B2M is produced within the brain in HIV dementia.In the absence of CNS opportunistic processes, elevated CSF B2M>3.8 mg/l is a clinically useful marker for HIV dementia.
 
Related Tags
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acquired immunodeficiency syndrome dementia complex
cerebrospinal fluid
cerebrospinal fluid,abnormal
cerebrospinal fluid,B2-microglobulin
dementia
human immunodeficiency virus type 1

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