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Prevalence of long-term BK and JC excretion in HIV-infected adults and lack of correlation with serological markers

✍ Scribed by Knowles, W.A.; Pillay, D.; Johnson, M.A.; Hand, J.F.; Brown, D.W.G.


Publisher
John Wiley and Sons
Year
1999
Tongue
English
Weight
82 KB
Volume
59
Category
Article
ISSN
0146-6615

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✦ Synopsis


The natural history of polyomavirus infection, and sensitivity of diagnostic assays remain unclear. A stratified group of 94 human immunodeficiency virus (HIV)-infected patients was studied for both virological and serological markers of active infection with both JC virus and BK virus. JC DNA was detected in the urine of 18 of 81 (22%) patients and BK DNA in 30 (37%) patients. Whilst patients with a low CD 4 cell count (P = .009), CD 4 /CD 8 ratio (P = .031) and ␤2M concentration (P = .042) were significantly more likely to be excreting BK, JC excretion did not correlate with any of the immunological markers measured. Furthermore, when all the immunological factors were taken into account, there was no association between either BK or JC excretion and age of the patient (P = .149 for BK, P = 0.891 for JC). BK IgM antibody was detected in only 3 of 30 (10%) BK excretors. JC IgM was detected in 5 of 18 (27.7%) JC excretors but also in 11 of 63 (17.5%) patients without demonstrable JC excretion. Therefore IgM was a very poor indicator of viruria. One year follow-up on a subset of patients showed that both DNA detection in urine and IgM antibody remain stable over many months despite falling CD 4 cell counts, and would indicate that events leading to enhanced viral production probably occur early after HIV infection. Replication of JC virus in the brain leading to the onset of progressive multifocal leukoencephalopathy (PML) could not be predicted using any of the markers studied.