Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) risk

Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) risk

<strong>Background</strong>. BKV infection usually occurs in early childhood through the respiratory tract.The virus persists in a latent form in the kidney and it could be reactivated under favorable condition.The most important clinical manifestations affect kidney transplanted in whic...

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Main Authors: Elio De Nisco, Pia Carmen Melillo, Angelo Santopietro, Maria Landi, Raffaele Ariola, Franca Romeo, Anna Todisco
Format: Article
Language:English
Published: PAGEPress Publications 2013-08-01
Series:Microbiologia Medica
Subjects:
BKV,BKV-DNA, Real-Time PCR, PVAN
Online Access:http://www.pagepressjournals.org/index.php/mm/article/view/2252
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spelling doaj-4b936180ecf44833aecc5d71376138ca2020-11-25T01:24:46ZengPAGEPress PublicationsMicrobiologia Medica 2280-64232013-08-0128210.4081/mm.2013.22521511Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) riskElio De Nisco0Pia Carmen Melillo1Angelo Santopietro2Maria Landi3Raffaele Ariola4Franca Romeo5Anna Todisco6Unità Operativa Complessa di Virologia, Dipartimento di Medicina di Laboratorio, “S.G. Moscati”, AvellinoUnità Operativa Complessa di Virologia, Dipartimento di Medicina di Laboratorio, “S.G. Moscati”, AvellinoStruttura Complessa di Chirurgia Generale e Trapianti di rene, A.O.“OO.RR. San Giovanni di Dio e Ruggi d’Aragona”, SalernoUnità Operativa Complessa di Virologia, Dipartimento di Medicina di Laboratorio, “S.G. Moscati”, AvellinoUnità Operativa Complessa di Virologia, Dipartimento di Medicina di Laboratorio, “S.G. Moscati”, AvellinoUnità Operativa Complessa di Virologia, Dipartimento di Medicina di Laboratorio, “S.G. Moscati”, AvellinoUnità Operativa Complessa di Virologia, Dipartimento di Medicina di Laboratorio, “S.G. Moscati”, Avellino<strong>Background</strong>. BKV infection usually occurs in early childhood through the respiratory tract.The virus persists in a latent form in the kidney and it could be reactivated under favorable condition.The most important clinical manifestations affect kidney transplanted in which the BK polyomavirus nephropathy (PVAN) can lead to kidney failure. <strong>Objectives</strong>. The aim of our study was to evaluate the clinical utility of quantification of BKV viruria and especially viremia detected by real-time PCR method to select the patients at risk of PVAN. <strong>Study Design</strong>. We carried out a quantitative (dosing) assay of BKV-DNA in 24 patients transplanted in Salerno’s hospital, or elsewhere, all treated with cyclosporine or tacrolimus and mycophenolate mofetil or Prednisolone. The enrollment was made on the basis of impaired renal function, in particular of the values of serum creatinine (&gt; 25% of baseline level) and / or appearance of proteinuria. The nucleic acid extraction was performed by EXTRAgen kit (Nanogen); the extracts were submitted to quantitative evaluation by BKV Q-PCR Alert Kit indicare regione target in Real Time PCR (Nanogen) using the instrument ABI7300 (Applied Biosystems). <strong>Results</strong>. 16 patients were negative both for viremia and viruria,4 patients showed positive viruria but viremia &lt;10,000 copies / ml, 4 patients showed positive viruria and viremia &gt; 10,000 copies / ml. In the last group, biopsy, performed to diagnose PVAN was positive and immunosuppressive therapy was reformulate leading to the decline, but never to the negativity of viral load. <strong>Conclusions</strong>. The renal impairement combined with the quantification of BKV’s viral load in urine and especially in plasma, can also be effective predictors of PVAN.http://www.pagepressjournals.org/index.php/mm/article/view/2252BKV,BKV-DNA, Real-Time PCR, PVAN
collection DOAJ
language English
format Article
sources DOAJ
author Elio De Nisco
Pia Carmen Melillo
Angelo Santopietro
Maria Landi
Raffaele Ariola
Franca Romeo
Anna Todisco
spellingShingle Elio De Nisco
Pia Carmen Melillo
Angelo Santopietro
Maria Landi
Raffaele Ariola
Franca Romeo
Anna Todisco
Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) risk
Microbiologia Medica
BKV,BKV-DNA, Real-Time PCR, PVAN
author_facet Elio De Nisco
Pia Carmen Melillo
Angelo Santopietro
Maria Landi
Raffaele Ariola
Franca Romeo
Anna Todisco
author_sort Elio De Nisco
title Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) risk
title_short Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) risk
title_full Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) risk
title_fullStr Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) risk
title_full_unstemmed Quantification of BKV in urine and plasma in renal transplant recipients at PVAN (Polyomavirus-associated nephropathy) risk
title_sort quantification of bkv in urine and plasma in renal transplant recipients at pvan (polyomavirus-associated nephropathy) risk
publisher PAGEPress Publications
series Microbiologia Medica
issn 2280-6423
publishDate 2013-08-01
description <strong>Background</strong>. BKV infection usually occurs in early childhood through the respiratory tract.The virus persists in a latent form in the kidney and it could be reactivated under favorable condition.The most important clinical manifestations affect kidney transplanted in which the BK polyomavirus nephropathy (PVAN) can lead to kidney failure. <strong>Objectives</strong>. The aim of our study was to evaluate the clinical utility of quantification of BKV viruria and especially viremia detected by real-time PCR method to select the patients at risk of PVAN. <strong>Study Design</strong>. We carried out a quantitative (dosing) assay of BKV-DNA in 24 patients transplanted in Salerno’s hospital, or elsewhere, all treated with cyclosporine or tacrolimus and mycophenolate mofetil or Prednisolone. The enrollment was made on the basis of impaired renal function, in particular of the values of serum creatinine (&gt; 25% of baseline level) and / or appearance of proteinuria. The nucleic acid extraction was performed by EXTRAgen kit (Nanogen); the extracts were submitted to quantitative evaluation by BKV Q-PCR Alert Kit indicare regione target in Real Time PCR (Nanogen) using the instrument ABI7300 (Applied Biosystems). <strong>Results</strong>. 16 patients were negative both for viremia and viruria,4 patients showed positive viruria but viremia &lt;10,000 copies / ml, 4 patients showed positive viruria and viremia &gt; 10,000 copies / ml. In the last group, biopsy, performed to diagnose PVAN was positive and immunosuppressive therapy was reformulate leading to the decline, but never to the negativity of viral load. <strong>Conclusions</strong>. The renal impairement combined with the quantification of BKV’s viral load in urine and especially in plasma, can also be effective predictors of PVAN.
topic BKV,BKV-DNA, Real-Time PCR, PVAN
url http://www.pagepressjournals.org/index.php/mm/article/view/2252
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