Monitoring low cytomegalovirus viremia in transplanted patients by a real-time PCR on plasma

Until recently, human cytomegalovirus (hCMV) infection and anti‐CMV treatment in transplanted patients have been monitored essentially by pp65 antigenemia, which is time‐consuming and requires experienced operators. For the last two years, pp65 antigenemia levels have tended to be lower than previou...

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Bibliographic Details
Published in:Journal of medical virology 2005-05, Vol.76 (1), p.76-81
Main Authors: Schvoerer, Evelyne, Henriot, Sylvie, Zachary, Pierre, Freitag, Rachel, Fuchs, Anne, Fritsch, Sandrine, Risch, Simone, Meyer, Nicolas, Caillard, Sophie, Lioure, Bruno, Stoll-Keller, Françoise
Format: Article
Language:English
Subjects:
Adult
Aged
Antigens, Viral
Antigens, Viral - blood
Biological and medical sciences
Biomarkers
Biomarkers - blood
Bone Marrow Transplantation
Cytomegalovirus
Cytomegalovirus - genetics
Cytomegalovirus - immunology
Cytomegalovirus - isolation & purification
Cytomegalovirus Infections
Cytomegalovirus Infections - blood
Cytomegalovirus Infections - diagnosis
DNA, Viral
DNA, Viral - blood
Female
Fundamental and applied biological sciences. Psychology
HCMV
Human health and pathology
Human viral diseases
Humans
Infectious diseases
Kidney Transplantation
Life Sciences
LightCycler
Male
Medical sciences
Microbiology
Microbiology and Parasitology
Middle Aged
Miscellaneous
Phosphoproteins
Phosphoproteins - blood
plasma CMV DNA
Polymerase Chain Reaction
Polymerase Chain Reaction - methods
Postoperative Complications
Postoperative Complications - diagnosis
pp65 antigenemia
Time Factors
transplantation
Viral diseases
Viral Matrix Proteins
Viral Matrix Proteins - blood
Virology
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Summary:Until recently, human cytomegalovirus (hCMV) infection and anti‐CMV treatment in transplanted patients have been monitored essentially by pp65 antigenemia, which is time‐consuming and requires experienced operators. For the last two years, pp65 antigenemia levels have tended to be lower than previously in our laboratory, which could be due to better monitoring of CMV‐related risk. Results obtained by real‐time PCR with a LightCycler instrument or by pp65 antigen assay were compared on 145 serial samples from bone marrow or kidney transplant recipients under the usual conditions of our laboratory. CMV DNA was extracted from plasma and quantified by using primers and probes directed to HXFL4 gene. The plasma CMV DNA load was measured by using a standard curve constructed with a commercially available quantified CMV DNA suspension. Among the 145 samples, 139 showed a pp65 antigen which was negative or lower than 20 positively stained cells per 200,000 leukocytes. In the patients with positive pp65 antigenemia, the corresponding values of CMV DNA copy number/ml were significantly higher than those observed in patients without antigenemia (P 
ISSN:0146-6615
1096-9071
DOI:10.1002/jmv.20326