Screening for BK virus nephropathy in kidney transplant recipients: comparison of diagnostic tests

Pinto, Gabriel Godinho; Poloni, José Antônio Tesser; Rotta, Liane Nanci; Razonable, Raymund R.; Pasqualotto, Alessandro C.

doi:10.5935/0101-2800.20160054

Cited by 6 publications

(10 citation statements)

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“…The study was retrospective and single center and these results should therefore be confirmed at other centers using different immunosuppression and other clinical protocols. The majority of BKPyVAN cases were presumptively diagnosed based on viral load threshold rather than by biopsy, but a well‐validated virologic threshold was used for diagnosis, and the characteristics and outcomes of those with presumptive and proven BKPyVAN were similar (Table ). The inclusion of both presumptive and biopsy‐proven cases allowed an analysis reflective of the full clinical spectrum of BKPyVAN and avoided inappropriate misclassification of cases with false negative biopsies .…”

Section: Discussionmentioning

confidence: 99%

“…Biopsy‐proven BKPyVAN was diagnosed by renal allograft biopsy that demonstrated typical viral inclusions that were positive for SV40 antigen as described previously . Presumptive BKPyVAN was defined as a plasma BKPyV load >10 000 BKPyV DNA copies/mL, a well‐validated, sensitive, and specific threshold for biopsy‐proven BKPyVAN, as previously described . Proven and presumed cases were pooled for analysis to reflect the entire spectrum of clinical BKPyVAN, to include true cases of BKPyVAN that might have been missed because of a falsely negative biopsy, and because these clinical entities have been shown to have a generally similar histologic and clinical course .…”

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Clinical characteristics and outcomes of late‐onset BK virus nephropathy in kidney and kidney‐pancreas transplant recipients

Imlay

Whitaker

Fisher

et al. 2018

Transplant Infectious Dis

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Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Clinical characteristics and outcomes of late‐onset BK virus nephropathy in kidney and kidney‐pancreas transplant recipients

Imlay

Whitaker

Fisher

et al. 2018

Transplant Infectious Dis

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“…1,2 NAT in urine, in the absence of an elevated BKPyV plasma load is not associated with an increased risk for BKPyVAN. Pinto et al 7 concluded that positive BKPyV in two or more urine samples was helpful to predict BKPyV viremia with 100% sensitivity, 94% specificity and a PPV of 50% and NPV of 100%. Plasma NAT has the best PPV for BKPyVAN and has been used for most transplant centers for BKPyV screening; the sensitivity to predict BKPyVAN was 60-100%, specificity was 33-100%, and PPV was 72-100%.…”

Section: Analysis Of Diagnostic Methods As a Screening Test To Detectmentioning

confidence: 99%

“…As reported by Pinto et al, the different techniques limit the comparison between quantitative NATs and there is a need for standardization for BKPyV-related tests. 7 PCRs with primers and probes targeting the variable regions of the genome, like the NCCR or VP1 regions, may give false negative results or incorrect viral loads when samples contain rare genotypes. 10 In addition, urine "decoy cells" detection presents a considerable pre-analytical logistics and an analytical laboratory expertise; the exam should be performed in fresh urine, and inconclusive results are frequent during the first months post-transplant due the high urinary sediment.…”

Section: Analysis Of Diagnostic Methods As a Screening Test To Detectmentioning

confidence: 99%

“…that directly compared the analytical performance of screening methods to predict the diagnosis of BKPyVAN proven by histopathology. 7 From 707 potential articles initially identified, only 12 met inclusion criteria and were included in the final analysis, representing the paucity of data in the literature regarding this issue and the lack of quality data. The authors have demonstrated a better diagnostic performance of quantitative NAT than urine cytopathology for the detection of BKPyVAN.…”

Section: Analysis Of Diagnostic Methods As a Screening Test To Detectmentioning

confidence: 99%

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Analysis of diagnostic methods as a screening test to detect BK virus nephropathy in kidney transplant patients

Nihei

Pierrotti

David‐Neto

2016

Jornal Brasileiro De Nefrologia

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Presence of decoy cells for 6 months on urine cytology efficiently predicts BK virus nephropathy in renal transplant recipients

Sekito¹,

Araki²,

Yoshinaga³

et al. 2021

Int J of Urology

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Objectives: To investigate the association between duration of consecutive presence of decoy cells on urine cytology and BK virus nephropathy after kidney transplantation. Methods: In total, 121 kidney transplant recipients were retrospectively evaluated. The best duration of consecutive presence of decoy cells that could be used to predict BK virus nephropathy was analyzed using the area under the curve for each duration, and recipients were divided into two groups based on the best predictive performance. The effectiveness of SV40 immunostaining on urinary cytology was also analyzed. Results: In total, 2534 urine specimens as well as SV40 immunostaining in 2241 urine specimens were analyzed. Six consecutive months of decoy cell positivity had the best predictive performance for BK virus nephropathy (area under the curve = 0.832). The incidence of BK virus nephropathy in recipients with positive decoy cells for 6 months or more consecutive months (5/44) was significantly higher than in those who had positive decoy cells for less than 6 months (0/77; P = 0.005). Decoy cell positivity had a sensitivity, specificity, positive predictive value, and negative predictive value for BK virus nephropathy of 100%, 66%, 11%, and 100% respectively. SV40 immunostaining provided slightly better specificity (68%) and positive predictive value (12%). Conclusions: The detection of decoy cells at 6 months or more on urine cytology had high predictive value for BK virus nephropathy in kidney transplant recipients. SV40 immunostaining on urine cytology added minimal diagnostic accuracy.

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Screening for BK virus nephropathy in kidney transplant recipients: comparison of diagnostic tests

Cited by 6 publications

References 0 publications

Clinical characteristics and outcomes of late‐onset BK virus nephropathy in kidney and kidney‐pancreas transplant recipients

Clinical characteristics and outcomes of late‐onset BK virus nephropathy in kidney and kidney‐pancreas transplant recipients

Analysis of diagnostic methods as a screening test to detect BK virus nephropathy in kidney transplant patients

Presence of decoy cells for 6 months on urine cytology efficiently predicts BK virus nephropathy in renal transplant recipients

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