Monitoring of Cytomegalovirus Infection in Solid-Organ Transplant Recipients by an Ultrasensitive Plasma PCR Assay

Hadaya, Karine; Wunderli, Werner; Deffernez, Christelle; Martin, Pierre-Yves; Mentha, Gilles; Binet, Isabelle; Perrin, Luc; Kaiser, Laurent

doi:10.1128/jcm.41.8.3757-3764.2003

Cited by 40 publications

(31 citation statements)

References 35 publications

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“…In our study, the levels of viral DNAemia were those actually detected prior to the start of preemptive therapy, which prevented consistently HCMV disease and, thus, were verified as safe clinically. Cutoffs proposed by another group taking care of the patient clinical outcome were more similar to those calculated in the present study [Hadaya et al, 2003].…”

Section: Discussionsupporting

confidence: 52%

Clinically‐based determination of safe DNAemia cutoff levels for preemptive therapy or human cytomegalovirus infections in solid organ and hematopoietic stem cell transplant recipients

Lilleri¹,

Baldanti²,

Gatti³

et al. 2004

Journal of Medical Virology

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Transplantation Centers using human cytomegalovirus (HCMV) antigenemia-based preemptive therapy will need to replace in the near future the antigenemia assay with a more standardized and automatable assay, such as a molecular assay quantifying HCMV DNA in blood (DNAemia). Thus, in view of replacing antigenemia with clinically safe cutoff values, DNAemia levels corresponding to antigenemia cutoffs guiding HCMV preemptive therapy were determined retrospectively in solid organ and hematopoietic stem cell transplant recipients (HSCTR) using an "in-house" quantitative PCR (QPCR) method. Since preemptive therapy had prevented appearance of HCMV disease in all patients tested, DNA cutoffs determined retrospectively had to be considered as safe clinically as antigenemia cutoffs used prospectively. However, in solid organ transplant recipients (SOTR), initiating preemptive therapy upon an antigenemia cutoff of 100 pp65-positive leukocytes, a DNAemia cutoff of 300,000 copies/ml blood had positive and negative predictive values of >90%, indicating that a DNAemia cutoff could achieve, in terms of prevention of HCMV disease, the same clinical results as the antigenemia cutoff. In HSCTR, initiating preemptive therapy upon first antigenemia positivity, a DNAemia cutoff of 10,000 copies/ml blood had a positive predictive value of >90%, indicating that the great majority of patients treated under the antigenemia guidance would have been treated also using this DNA cutoff. On the other hand, the negative predictive value of 28.6% indicated that two out of three HSCTR had been treated under the antigenemia guidance having the same levels of viral DNA as the untreated patients. The data suggest that a quantitative cutoff could be adopted as a guiding criterion for preemptive therapy also in HSCTR. Regression analysis allowed to determine the DNAemia (corresponding to QPCR) cutoff values for two commercial assays tested both in solid organ and HSCTR. Retrospective DNAemia cutoff values will be verified for safety in prospective trials.

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Section: Discussionsupporting

confidence: 52%

Clinically‐based determination of safe DNAemia cutoff levels for preemptive therapy or human cytomegalovirus infections in solid organ and hematopoietic stem cell transplant recipients

Lilleri¹,

Baldanti²,

Gatti³

et al. 2004

Journal of Medical Virology

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“…Other studies, however, have reported a significantly lower sensitivity of antigenemia testing than those of molecular tests (80,88,(94)(95)(96)(97)(98)(99). In one study, the sensitivity of pp65 antigenemia was lower (39%) than that of an ultrasensitive PCR-based assay performed on plasma (67%) (96). Moreover, the LDT plasma PCR assay detected CMV infection 12 days earlier than the antigenemia test (96).…”

Section: Antigen Testingmentioning

confidence: 83%

“…One of these studies reported a strong correlation between pp65 antigenemia and CMV PCR performed on whole-blood specimens by use of an in-house laboratory-developed test (LDT) (91). Other studies, however, have reported a significantly lower sensitivity of antigenemia testing than those of molecular tests (80,88,(94)(95)(96)(97)(98)(99). In one study, the sensitivity of pp65 antigenemia was lower (39%) than that of an ultrasensitive PCR-based assay performed on plasma (67%) (96).…”

Section: Antigen Testingmentioning

confidence: 99%

“…In one study, the sensitivity of pp65 antigenemia was lower (39%) than that of an ultrasensitive PCR-based assay performed on plasma (67%) (96). Moreover, the LDT plasma PCR assay detected CMV infection 12 days earlier than the antigenemia test (96). Another study reported a significantly lower sensitivity (26%) of pp65 antigenemia testing than those of two PCR-based assays (COBAS Amplicor CMV Monitor test [48.6%] and an inhouse LDT [performed on a LightCycler] [54%]) (98).…”

Section: Antigen Testingmentioning

confidence: 99%

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Clinical Utility of Viral Load in Management of Cytomegalovirus Infection after Solid Organ Transplantation

2013

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SUMMARY The negative impact of cytomegalovirus (CMV) infection on transplant outcomes warrants efforts toward improving its prevention, diagnosis, and treatment. During the last 2 decades, significant breakthroughs in diagnostic virology have facilitated remarkable improvements in CMV disease management. During this period, CMV nucleic acid amplification testing (NAT) evolved to become one of the most commonly performed tests in clinical virology laboratories. NAT provides a means for rapid and sensitive diagnosis of CMV infection in transplant recipients. Viral quantification also introduced several principles of CMV disease management. Specifically, viral load has been utilized (i) for prognostication of CMV disease, (ii) to guide preemptive therapy, (iii) to assess the efficacy of antiviral treatment, (iv) to guide the duration of treatment, and (v) to indicate the risk of clinical relapse or antiviral drug resistance. However, there remain important limitations that require further optimization, including the interassay variability in viral load reporting, which has limited the generation of standardized viral load thresholds for various clinical indications. The recent introduction of an international reference standard should advance the major goal of uniform viral load reporting and interpretation. However, it has also become apparent that other aspects of NAT should be standardized, including sample selection, nucleic acid extraction, amplification, detection, and calibration, among others. This review article synthesizes the vast amount of information on CMV NAT and provides a timely review of the clinical utility of viral load testing in the management of CMV in solid organ transplant recipients. Current limitations are highlighted, and avenues for further research are suggested to optimize the clinical application of NAT in the management of CMV after transplantation.

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“…Both methods have been previously described. 18,19 Preemptive ganciclovir therapy was given at a dose of 5 mg/kg intravenously twice a day for 14 days and then 5 mg/kg daily for 2 weeks. In patients with neutropenia, foscarnet at a dose 90 mg/kg intravenously twice a day for 2 weeks and then 90 mg/kg daily 2 weeks was used.…”

Section: CMVmentioning

confidence: 99%

Pretransplantation CMV-specific T cells protect recipients of T-cell-depleted grafts against CMV-related complications

Chalandon¹,

Degermann²,

Villard³

et al. 2005

Blood

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Monitoring of Cytomegalovirus Infection in Solid-Organ Transplant Recipients by an Ultrasensitive Plasma PCR Assay

Cited by 40 publications

References 35 publications

Clinically‐based determination of safe DNAemia cutoff levels for preemptive therapy or human cytomegalovirus infections in solid organ and hematopoietic stem cell transplant recipients

Clinically‐based determination of safe DNAemia cutoff levels for preemptive therapy or human cytomegalovirus infections in solid organ and hematopoietic stem cell transplant recipients

Clinical Utility of Viral Load in Management of Cytomegalovirus Infection after Solid Organ Transplantation

Pretransplantation CMV-specific T cells protect recipients of T-cell-depleted grafts against CMV-related complications

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