Torque teno virus viremia and QuantiFERON(®)-CMV assay in prediction of cytomegalovirus reactivation in R+ kidney transplant recipients

INTRODUCTION: Cytomegalovirus (CMV) is the most frequent infectious complication following solid organ transplantation. Torque teno viruses (TTV) viremia has been proposed as a biomarker of functional immunity in the management of kidney transplant recipients (KTR). The QuantiFERON(®)-CMV (QF-CMV) i...

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Autores principales: Mafi, Sarah, Essig, Marie, Rerolle, Jean-Philippe, Lagathu, Gisèle, Crochette, Romain, Brodard, Véronique, Schvartz, Betoul, Gouarin, Stephanie, Bouvier, Nicolas, Engelmann, Ilka, Garstka, Antoine, Bressollette-Bodin, Céline, Cantarovitch, Diego, Germi, Raphaële, Janbon, Benedicte, Archimbaut, Christine, Heng, Anne-Elizabeth, Garnier, Françoise, Gomes-Mayeras, Melissa, Labrunie, Anaïs, Hantz, Sébastien, Alain, Sophie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Medicine
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10323437/
https://www.ncbi.nlm.nih.gov/pubmed/37425298
http://dx.doi.org/10.3389/fmed.2023.1180769
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author Mafi, Sarah
Essig, Marie
Rerolle, Jean-Philippe
Lagathu, Gisèle
Crochette, Romain
Brodard, Véronique
Schvartz, Betoul
Gouarin, Stephanie
Bouvier, Nicolas
Engelmann, Ilka
Garstka, Antoine
Bressollette-Bodin, Céline
Cantarovitch, Diego
Germi, Raphaële
Janbon, Benedicte
Archimbaut, Christine
Heng, Anne-Elizabeth
Garnier, Françoise
Gomes-Mayeras, Melissa
Labrunie, Anaïs
Hantz, Sébastien
Alain, Sophie
author_facet Mafi, Sarah
Essig, Marie
Rerolle, Jean-Philippe
Lagathu, Gisèle
Crochette, Romain
Brodard, Véronique
Schvartz, Betoul
Gouarin, Stephanie
Bouvier, Nicolas
Engelmann, Ilka
Garstka, Antoine
Bressollette-Bodin, Céline
Cantarovitch, Diego
Germi, Raphaële
Janbon, Benedicte
Archimbaut, Christine
Heng, Anne-Elizabeth
Garnier, Françoise
Gomes-Mayeras, Melissa
Labrunie, Anaïs
Hantz, Sébastien
Alain, Sophie
author_sort Mafi, Sarah
collection PubMed
description INTRODUCTION: Cytomegalovirus (CMV) is the most frequent infectious complication following solid organ transplantation. Torque teno viruses (TTV) viremia has been proposed as a biomarker of functional immunity in the management of kidney transplant recipients (KTR). The QuantiFERON(®)-CMV (QF-CMV) is a commercially available assay that allows the assessment of CD8(+) T-cell responses in routine diagnostic laboratories. METHODS: In a prospective national multicenter cohort of 64 CMV-seropositive (R+) KTR, we analyzed the value of TTV load and the two markers of the QF-CMV assay [QF-Ag (CMV-specific T-cell responses) and QF-Mg (overall T-cell responses)], alone and in combination, in prediction of CMV reactivation (≥3 log(10) IU/ ml) in the first post-transplant year. We compared previously published cut-offs and specific cut-offs optimized from ROC curves for our population. RESULTS: Using the conventional cut-off (3.45 log(10) copies/ml), TTV load at D0 [inclusion visit on the day of transplantation before induction (D0)], or at M1 (1-month post-transplant visit) perform better in predicting CMV viremia control than CMV reactivation. Survival analyses suggest a better performance of our optimized TTV cut-offs (3.78 log(10) copies/ml at D0 and 4.23 log(10) copies/ml at M1) for risk stratification of CMV reactivation in our R+ KTR cohort. The QF-CMV (QF-Ag = 0.2 IU/ml, and QF-Mg = 0.5 IU/ml) also appears to better predict CMV viremia control than CMV reactivation. Moreover, survival analyses suggest that the QF-Mg would perform better than the QF-Ag in stratifying the risk of CMV reactivation. The use of our optimized QF-Mg cut-off (1.27 IU/ml) at M1 further improved risk stratification of CMV reactivation. Using conventional cut-offs, the combination of TTV load and QF-Ag or TTV load and QF-Mg did not improve prediction of CMV viremia control compared to separate analysis of each marker but resulted in an increase of positive predictive values. The use of our cut-offs slightly improved risk prediction of CMV reactivation. CONCLUSION: The combination of TTV load and QF-Ag or TTV load and QF-Mg could be useful in stratifying the risk of CMV reactivation in R+ KTR during the first post-transplant year and thereby have an impact on the duration of prophylaxis in these patients. CLINICAL TRIAL REGISTRATION: ClinicalTrials.gov registry, identifier NCT02064699.
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spelling pubmed-103234372023-07-07 Torque teno virus viremia and QuantiFERON(®)-CMV assay in prediction of cytomegalovirus reactivation in R+ kidney transplant recipients Mafi, Sarah Essig, Marie Rerolle, Jean-Philippe Lagathu, Gisèle Crochette, Romain Brodard, Véronique Schvartz, Betoul Gouarin, Stephanie Bouvier, Nicolas Engelmann, Ilka Garstka, Antoine Bressollette-Bodin, Céline Cantarovitch, Diego Germi, Raphaële Janbon, Benedicte Archimbaut, Christine Heng, Anne-Elizabeth Garnier, Françoise Gomes-Mayeras, Melissa Labrunie, Anaïs Hantz, Sébastien Alain, Sophie Front Med (Lausanne) Medicine INTRODUCTION: Cytomegalovirus (CMV) is the most frequent infectious complication following solid organ transplantation. Torque teno viruses (TTV) viremia has been proposed as a biomarker of functional immunity in the management of kidney transplant recipients (KTR). The QuantiFERON(®)-CMV (QF-CMV) is a commercially available assay that allows the assessment of CD8(+) T-cell responses in routine diagnostic laboratories. METHODS: In a prospective national multicenter cohort of 64 CMV-seropositive (R+) KTR, we analyzed the value of TTV load and the two markers of the QF-CMV assay [QF-Ag (CMV-specific T-cell responses) and QF-Mg (overall T-cell responses)], alone and in combination, in prediction of CMV reactivation (≥3 log(10) IU/ ml) in the first post-transplant year. We compared previously published cut-offs and specific cut-offs optimized from ROC curves for our population. RESULTS: Using the conventional cut-off (3.45 log(10) copies/ml), TTV load at D0 [inclusion visit on the day of transplantation before induction (D0)], or at M1 (1-month post-transplant visit) perform better in predicting CMV viremia control than CMV reactivation. Survival analyses suggest a better performance of our optimized TTV cut-offs (3.78 log(10) copies/ml at D0 and 4.23 log(10) copies/ml at M1) for risk stratification of CMV reactivation in our R+ KTR cohort. The QF-CMV (QF-Ag = 0.2 IU/ml, and QF-Mg = 0.5 IU/ml) also appears to better predict CMV viremia control than CMV reactivation. Moreover, survival analyses suggest that the QF-Mg would perform better than the QF-Ag in stratifying the risk of CMV reactivation. The use of our optimized QF-Mg cut-off (1.27 IU/ml) at M1 further improved risk stratification of CMV reactivation. Using conventional cut-offs, the combination of TTV load and QF-Ag or TTV load and QF-Mg did not improve prediction of CMV viremia control compared to separate analysis of each marker but resulted in an increase of positive predictive values. The use of our cut-offs slightly improved risk prediction of CMV reactivation. CONCLUSION: The combination of TTV load and QF-Ag or TTV load and QF-Mg could be useful in stratifying the risk of CMV reactivation in R+ KTR during the first post-transplant year and thereby have an impact on the duration of prophylaxis in these patients. CLINICAL TRIAL REGISTRATION: ClinicalTrials.gov registry, identifier NCT02064699. Frontiers Media S.A. 2023-06-22 /pmc/articles/PMC10323437/ /pubmed/37425298 http://dx.doi.org/10.3389/fmed.2023.1180769 Text en Copyright © 2023 Mafi, Essig, Rerolle, Lagathu, Crochette, Brodard, Schvartz, Gouarin, Bouvier, Engelmann, Garstka, Bressollette-Bodin, Cantarovitch, Germi, Janbon, Archimbaut, Heng, Garnier, Gomes-Mayeras, Labrunie, Hantz and Alain. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Medicine
Mafi, Sarah
Essig, Marie
Rerolle, Jean-Philippe
Lagathu, Gisèle
Crochette, Romain
Brodard, Véronique
Schvartz, Betoul
Gouarin, Stephanie
Bouvier, Nicolas
Engelmann, Ilka
Garstka, Antoine
Bressollette-Bodin, Céline
Cantarovitch, Diego
Germi, Raphaële
Janbon, Benedicte
Archimbaut, Christine
Heng, Anne-Elizabeth
Garnier, Françoise
Gomes-Mayeras, Melissa
Labrunie, Anaïs
Hantz, Sébastien
Alain, Sophie
Torque teno virus viremia and QuantiFERON(®)-CMV assay in prediction of cytomegalovirus reactivation in R+ kidney transplant recipients
title Torque teno virus viremia and QuantiFERON(®)-CMV assay in prediction of cytomegalovirus reactivation in R+ kidney transplant recipients
title_full Torque teno virus viremia and QuantiFERON(®)-CMV assay in prediction of cytomegalovirus reactivation in R+ kidney transplant recipients
title_fullStr Torque teno virus viremia and QuantiFERON(®)-CMV assay in prediction of cytomegalovirus reactivation in R+ kidney transplant recipients
title_full_unstemmed Torque teno virus viremia and QuantiFERON(®)-CMV assay in prediction of cytomegalovirus reactivation in R+ kidney transplant recipients
title_short Torque teno virus viremia and QuantiFERON(®)-CMV assay in prediction of cytomegalovirus reactivation in R+ kidney transplant recipients
title_sort torque teno virus viremia and quantiferon(®)-cmv assay in prediction of cytomegalovirus reactivation in r+ kidney transplant recipients
topic Medicine
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10323437/
https://www.ncbi.nlm.nih.gov/pubmed/37425298
http://dx.doi.org/10.3389/fmed.2023.1180769
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