Histological Evolution of BK Virus–Associated Nephropathy: Importance of Integrating Clinical and Pathological Findings

Drachenberg, Cinthia B.; Chaudhry, M. R.; Ugarte, Richard; Mavanur, M.; Thomas, Beje; Cangro, Charles B.; Costa, Nadiesda; Ramos, Emilio; Weir, Matthew R.; Haririan, Abdolreza

doi:10.1111/ajt.14314

Cited by 78 publications

(124 citation statements)

References 59 publications

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“…Viruria sometimes progresses to viremia (usually after a gap of a few weeks), with a reported incidence of 5–15%. Although the progress to viremia closely mirrors the onset of BKVN, the incidence of biopsy-proven BKVN is reported to be only 1–5%, likely due to the focal nature of BKV disease (9–11). BKVN often leads to renal allograft loss, and a substantial body of literature exists about this association and its management (8, 12).…”

Section: Introductionmentioning

confidence: 99%

Treatment for presumed BK polyomavirus nephropathy and risk of urinary tract cancers among kidney transplant recipients in the United States

Gupta

Kuppachi

Kalil

et al. 2018

American Journal of Transplantation

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Recent case series describe detection of BK polyomavirus (BKV) in urinary tract cancers in kidney transplant recipients, suggesting that BKV could contribute to the development of these cancers. We assessed risk for urinary tract cancers in kidney recipients with or without treatment for presumed BKV nephropathy (tBKVN) using data from the United States Transplant Cancer Match Study (2003-2013). Among 55 697 included recipients, 2015 (3.6%) were reported with tBKVN. Relative to the general population, incidence was similarly elevated (approximately 4.5-fold) for kidney cancer in recipients with or without tBKVN, and incidence was not increased in either group for prostate cancer. In contrast, for invasive bladder cancer, incidence was more strongly elevated in recipients with versus without tBKVN (standardized incidence ratios 4.5 vs. 1.7; N = 48 cases), corresponding to an incidence rate ratio (IRR) of 2.9 (95% confidence interval [CI] 1.0-8.2), adjusted for sex, age, transplant year, and use of polyclonal antibody induction. As a result, recipients with tBKVN had borderline increased incidence for all urothelial cancers combined (renal pelvis, ureter, and bladder cancers: adjusted IRR 2.2, 95% CI 0.9-5.4; N = 89 cases). Together with reports describing BKV detection in tumor tissues, these results support an association between BKV and urothelial carcinogenesis among kidney transplant recipients.

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Section: Introductionmentioning

confidence: 99%

Treatment for presumed BK polyomavirus nephropathy and risk of urinary tract cancers among kidney transplant recipients in the United States

Gupta

Kuppachi

Kalil

et al. 2018

American Journal of Transplantation

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“…In our cohort 18% of kidney transplant recipients were diagnosed with BKPyVAN beyond 1 year post‐transplant; however, since the majority of our cohort was not routinely screened beyond 1 year post‐transplant, this represents a minimum estimate of the frequency of late‐onset BKPyVAN. These findings emphasize the importance of evaluating for BKPyV viremia at all times that a renal graft biopsy is deemed clinically necessary, as is recommended in current guidelines . Notably, the incidence rate of BKPyVAN was similar between SPK recipients and KTR, but SPK recipients were significantly more likely to develop late‐onset BKPyVAN, suggesting that monitoring in SPK recipients should be extended beyond 1 year for this group to optimize the opportunity for earlier detection and intervention.…”

Section: Discussionmentioning

confidence: 81%

“…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 . To verify comparability in BK viral load across assays, the clinically used BKPyV assay in this study was directly compared to the assay used to define the 10 000 BKPyV DNA copies/mL threshold for BKPyVAN, and demonstrated viral load results within 0.1 log BKPyV DNA copies/mL.…”

Section: Methodsmentioning

confidence: 99%

“…This definition of “late‐onset” is problematic both because the mean/median onset of BKPyVAN is often later than 6 months and because all major guidelines recommend routine BKPyV screening up to 1 year post‐transplant. Recent studies have documented the histological evolution of BKPyVAN and have noted isolated late cases occurring >2 years post‐transplantation . Additional data on BKPyVAN occurring beyond 1 year post‐transplant are necessary to identify the incidence and outcomes and to identify potential patient groups in whom longer durations of screening beyond 1 year post‐transplant might be appropriate.…”

Section: Introductionmentioning

confidence: 99%

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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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“…The authors were well positioned to independently revisit the natural histologic and clinical evolution of BKVN under contemporary clinical screening protocols, maintenance immunosuppression, and immunosuppression reduction approaches in cases with viremia and BKVN (2,3). Both articles study kidney transplants with BKVN.…”

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confidence: 99%

BK Virus Nephropathy Revisited

Mengel

2017

American Journal of Transplantation

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More than 20 years after its first description and increased morbidity under powerful immunosuppression, the understanding of the pathogenesis of BK polyomavirus induced-allograft nephropathy (BKVN) has changed clinical practice in renal transplantation. Screening programs were introduced at most transplant centers, causing the prevalence of BKVN to decrease. However, BK viremia is still found in 10-30% of renal allograft recipients, with 1-10% developing BKVN. Once manifested, BKVN represents a serious disease of the renal transplant, causing allograft failure in 15-50% (1).In this issue of AJT, two transplant centers describe results from their comprehensively phenotyped cohorts of renal allograft recipients. The authors were well positioned to independently revisit the natural histologic and clinical evolution of BKVN under contemporary clinical screening protocols, maintenance immunosuppression, and immunosuppression reduction approaches in cases with viremia and BKVN (2,3). Both articles study kidney transplants with BKVN. Drachenberg et al (n = 71) and Nankivell et al (n = 63) discuss patients undergoing sequential biopsies (total number of BKVN biopsies analyzed from both studies, n = 660) and viral load measurements with available long-term follow-up. In the Nankivell study, the BKVN cohort was compared to an equally well-annotated and followed time-matched cohort of renal transplants (n = 490) without BKVN (975 protocol biopsies). Interesting and reassuring is the fact that both studies independently reveal almost identical major findings, discussed below. Early-stage disease (i.e. BKVN without inflammation) was very uncommon at initial clinical presentation, while early prodromal borderline-like interstitial inflammation in SV40-negative biopsies predated a later diagnosis of BKVN in up to 23% of cases with BK viremia. Also, resolving BKVN often featured SV40-negative interstitial inflammation. It is quite likely that in such scenarios the SV40 stain is false negative due to sampling error and/or limited staining sensitivity (4). Accordingly, an inadequate, SV40-negative biopsy in a patient with viremia should trigger early but modest reduction in immunosuppression and close follow-up, since presumptive (SV40-negative; 30% of cases) and definite (SV40-positive; 70% of cases) BKVN presented with an identical clinical course.

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Histological Evolution of BK Virus–Associated Nephropathy: Importance of Integrating Clinical and Pathological Findings

Cited by 78 publications

References 59 publications

Treatment for presumed BK polyomavirus nephropathy and risk of urinary tract cancers among kidney transplant recipients in the United States

Treatment for presumed BK polyomavirus nephropathy and risk of urinary tract cancers among kidney transplant recipients in the United States

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

BK Virus Nephropathy Revisited

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