Evaluation of the murex hybrid capture cytomegalovirus DNA assay versus plasma PCR and shell vial assay for diagnosis of human cytomegalovirus viremia in immunocompromised patients
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Barrett-Muir, WY
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Royal London Hosp, NHS Trust, Dept Clin Virol, London E1 1BB, EnglandRoyal London Hosp, NHS Trust, Dept Clin Virol, London E1 1BB, England
Barrett-Muir, WY
[1
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Aitken, C
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机构:Royal London Hosp, NHS Trust, Dept Clin Virol, London E1 1BB, England
Aitken, C
Templeton, K
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机构:Royal London Hosp, NHS Trust, Dept Clin Virol, London E1 1BB, England
Templeton, K
Raftery, M
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机构:Royal London Hosp, NHS Trust, Dept Clin Virol, London E1 1BB, England
Raftery, M
Kelsey, SM
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机构:Royal London Hosp, NHS Trust, Dept Clin Virol, London E1 1BB, England
Kelsey, SM
Breuer, J
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机构:Royal London Hosp, NHS Trust, Dept Clin Virol, London E1 1BB, England
Breuer, J
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[1] Royal London Hosp, NHS Trust, Dept Clin Virol, London E1 1BB, England
[2] Royal London Hosp, NHS Trust, Dept Nephrol, London E1 1BB, England
[3] Royal London Hosp, NHS Trust, Dept Haematol, London E1 1BB, England
We evaluated a cytomegalovirus (CMV) 24-hour shell vial assay (SVA), the Murex Hybrid Capture CMV DNA assay (HCA), and a CMV plasma PCR for the detection of CMV viremia in renal and bone marrow transplant recipients and human immunodeficiency virus-infected patients. CMV viremia was detected by at least one method in 125 of 317 evaluable samples (39.4%) from 78 patients and was detected in 19.8% of samples by SVA, 26.8% by HCA, and 32.2% by plasma PCR, There was moderate to substantial agreement between the results of the different tests (kappa coefficient = 0.415 to 0.631). However, HCA and plasma PCR were significantly more sensitive than SVA (P = 0.001 and P < 0.0001, respectively; McNemar's test), and plasma PCR was more sensitive than HCA (P = 0.031; McNemar's test). BCA and plasma PCR were more consistently positive than SVA during viremic episodes (P = 0.0002 and P < 0.0001, respectively; McNemar's test). The use of HCA or plasma PCR may therefore improve the diagnosis and management of CMV disease in susceptible patient groups.
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页码:2554 / 2556
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