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Cytomegalovirus-RNA accurately predicts the need for preemptive therapy in children undergoing liver transplantation: a proof-of-concept study
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  • Emanuele Nicastro,
  • Eleonora Severi,
  • Ilaria Passera,
  • Michele Totaro,
  • Lorenza Matarazzo,
  • Laura Fornataro,
  • Francesco Morotti,
  • Alessandra Tebaldi,
  • Ezio Bonanomi,
  • Michela Bravi,
  • Angelo Di Giorgio,
  • Samuele Covini,
  • Marta Dolci,
  • Domenico Pinelli,
  • Marco Arosio,
  • Lorenzo D'Antiga
Emanuele Nicastro
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII

Corresponding Author:enicastro@asst-pg23.it

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Eleonora Severi
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Ilaria Passera
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Michele Totaro
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Lorenza Matarazzo
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Laura Fornataro
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Francesco Morotti
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Alessandra Tebaldi
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Ezio Bonanomi
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Michela Bravi
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Angelo Di Giorgio
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Samuele Covini
Universita degli Studi di Milano-Bicocca Dipartimento di Medicina e Chirurgia
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Marta Dolci
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Domenico Pinelli
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Marco Arosio
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Lorenzo D'Antiga
Aziende Socio Sanitarie Territoriale Papa Giovanni XXIII
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Abstract

Preemptive therapy (PET) is safe and effective in controlling Cytomegalovirus (CMV) infection after pediatric liver transplantation (LT) and allows to observe the kinetics of quatitative CMV-DNA viral load till it reaches the treatment thresholds. While an early detection of low-to-moderate CMV-DNA levels may not indicate active viral replication, awaiting the viral load to exceed the treatment threshold may lead to viremic breakthroughs and CMV disease. We assessed the capacity of quantitative CMV-RNA (UL21.5 mRNA) to identify active viral replication, and its accuracy in predicting the need for PET in LT children. One-hundred and forty-four comparative quantitative CMV-RNA and CMV-DNA determinations were obtained from 12 children followed prospectically for 6 months after LT. Of 52 CMV-DNA-positive specimens, 17 (32%) were also CMV-RNA-positive, while CMV-RNA was undetectable in CMV-DNA-negative specimens. All children needing PET or treated for CMV disease had early detectable CMV-RNA, peaking simultaneously to CMV-DNA (median CMV-DNA: 65,906 cp/mL; median CMV-RNA: 767 cp/mL); conversely, none of those with persistently low DNAemia proved CMV-RNA-positive. In this first pilot study, CMV-RNA had 100% sensitivity and specificity in predicting the need for PET after pediatric LT. The early detection of CMV-RNA marks significant CMV infection/reactivation, thus allowing to avoid unnecessary antiviral treatment.
30 Nov 2024Submitted to Journal of Medical Virology
03 Dec 2024Submission Checks Completed
03 Dec 2024Assigned to Editor
03 Dec 2024Review(s) Completed, Editorial Evaluation Pending
04 Dec 2024Reviewer(s) Assigned