BK viremia and polyomavirus nephropathy in 352 kidney transplants; risk factors and potential role of mTOR inhibition

Jacobi, Johannes; Prignitz, Antonina; Büttner, Maike; Korn, Klaus; Weidemann, Alexander; Hilgers, Karl F.; Heller, Katharina; Velden, Joachim; Knöll, Antje; Wullich, Bernd; May, Christoph; Eckardt, Kai‐Uwe; Amann, Kerstin

doi:10.1186/1471-2369-14-207

Cited by 51 publications

(60 citation statements)

References 38 publications

(37 reference statements)

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“…In patients with negative screening for BKPyV, the authors observed an improved renal allograft function within the first year after transplantation compared to patients with BKPyV viremia and/or PyVAN. However, the patients with BKPyV viremia were not subdivided into groups based on quantified BKPyV viral load in serum . In the current study, patients with BKPyV viremia were subdivided according to their maximal detected BKPyV load in serum until 24 months after transplantation.…”

Section: Discussionmentioning

confidence: 97%

“…The impact of serum BKPyV viremia ≤10 4 copies/mL was not previously evaluated in the literature. A retrospective study by Jacobi et al observed an impact of the BKPyV viremia on the graft function. In patients with negative screening for BKPyV, the authors observed an improved renal allograft function within the first year after transplantation compared to patients with BKPyV viremia and/or PyVAN.…”

Section: Discussionmentioning

confidence: 99%

“…However, graft function was not described separately for patients with low‐level BKPyV viremia . These findings could be used in clinical praxis, as there seems to be no need for reduction of immunosuppression in patients with low‐level viremia in contrast to patients with high‐level viremia …”

Section: Discussionmentioning

confidence: 99%

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Impact of low‐level BK polyomavirus viremia on intermediate‐term renal allograft function

Korth

Widera²,

Dolff³

et al. 2018

Transplant Infectious Dis

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Section: Discussionmentioning

confidence: 97%

Section: Discussionmentioning

confidence: 99%

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Impact of low‐level BK polyomavirus viremia on intermediate‐term renal allograft function

Korth

Widera²,

Dolff³

et al. 2018

Transplant Infectious Dis

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“…Moreover, they are associated with lesser CMV viremia [69], and everolimus was shown to be superior to MMF in that aspect in a pooled analysis of three clinical trials [70]. Additionally, mTOR-I showed favourable effect in BK viremia/BK associated nephropathy [71,72] and post-transplant encapsulating peritoneal sclerosis [73][74][75].…”

Section: Introduction and Overview Of Immunosuppressant In Kidney Tramentioning

confidence: 99%

m-TOR Inhibitors in Kidney Transplantation: A Comprehensive Review

M¹,

Jm²,

Sharma³

et al. 2017

J Kidney

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Mammalian target of rapamaycin inhibitors (mTOR-I) has been in use in kidney transplantation for over two decades. Since their introduction, they have been used in different combination immunosuppressant for low risk group renal transplantation. They have been in use in the various (Calcineurin inhibitors) CNI-free protocols, either as De novo regiments, or by conversion from CNIs at a later stage. Many of these studies reported comparable graft rejection rate and a better kidney function (eGFR) compared to standard CNI protocols. Also mTOR-I when used in combination with CNIs, facilitated the use of lower doses of CNIs with the resultant reduction of CNI related side effects, without seriously compromising graft outcome. They are of particular interest among certain group of renal transplant recipients, including those with malignancy, post-transplant encapsulating peritoneal scelorosis, CMV and BK virus infections. Moreover, protocols containing mTOR-I showed comparable results to standard protocols among recipients of kidneys from extended-criteria transplantation. However, only few reports studied their use in high risk group renal transplantation, with variable outcomes. There is a noticeable drop in their popularity in the recent years, and their use was associated with multiple adverse events, in addition to a recent concern of their link to increased mortality. Also, a high discontinuation rate was demonstrated across many of the studies available to date. More studies are still needed to clarify the above-mentioned concerns.

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“…The issue has become more important in recent years, as several new immunosuppressant agents have been introduced for treating renal transplant recipients. PVAN is an aggressively destructive disease occurring in up to 8% of kidney allograft recipients [3], with one-year graft-loss rate ranging from 30% to 65% [4]. PVAN has become an important cause of allograft loss in renal transplantation, but only limited information is available regarding its pathogenesis.…”

Section: Introductionmentioning

confidence: 99%

Clinical and Pathological Study of Polyomavirus-Associated Nephropathy after Renal Transplantation

Ji¹,

Xie²,

Chen³

et al. 2014

J Transplant Technol Res

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Polyomavirus infection has emerged as an important cause of polyomavirus-associated nephropathy (PVAN) leading to allograft dysfunction and loss. The aim of this study is to investigate pathological features and clinical characteristics of PVAN. We prospectively investigated 351 renal allografts performed in Jinling Hospital. PVAN was diagnosed by light microscopic examination and a positive immunohistochemistry staining of anti-SV40 large T antibody in a biopsy specimen. 31 patients were diagnosed with PVAN (8.8%). The patients with PVAN typically presented as allograft dysfunction with an asymptomatic rise in serum creatinine about 3 to 39 months posttransplant. Urinary decoy cells were positive in 4 patients (12.9%). The histologic changes of PVAN are not pathognomonic and can be mistaken for allograft rejection, i.e. tubulointerstitial nephritis with varying degrees of inflammatory infiltrates, tubulitis, tubular atrophy and fibrosis. Typical findings on histology are focal interstitial mononuclear inflammatory cell infiltrates, presence of plasma cells, necrotic tubular epithelium, and presence of homogenous intranuclear inclusion bodies. Immunohistochemistry with SV40 staining is positive in allograft. CD3, CD4, CD8, CD68 positive cells are increased in PVAN group than the non-PVAN group, but none of HLA-DR and IL-2R expression is positive in PVAN patients. MPA AUC 0-12 and TAC trough levels are increased in PVAN group than non-PVAN group at biopsy. We have treated 31 patients with biopsy-proven PVAN with leflunomide. Increased intensity of immunosuppression appears to increase the likelihood of PVAN. The definitive diagnosis of PVAN requires renal biopsy. Immunohistochemistry with SV40 staining has been used as an indirect method to document the presence of PVAN.

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BK viremia and polyomavirus nephropathy in 352 kidney transplants; risk factors and potential role of mTOR inhibition

Cited by 51 publications

References 38 publications

Impact of low‐level BK polyomavirus viremia on intermediate‐term renal allograft function

Impact of low‐level BK polyomavirus viremia on intermediate‐term renal allograft function

m-TOR Inhibitors in Kidney Transplantation: A Comprehensive Review

Clinical and Pathological Study of Polyomavirus-Associated Nephropathy after Renal Transplantation

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