Polyomavirus BK with rearranged noncoding control region emerge in vivo in renal transplant patients and increase viral replication and cytopathology

Gosert, Rainer; Rinaldo, Christine Hanssen; Funk, Georg A.; Egli, Adrian; Ramos, Emilio; Drachenberg, Cinthia B.; Hirsch, Hans H.

doi:10.1084/jem.20072097

Cited by 187 publications

(246 citation statements)

References 49 publications

(60 reference statements)

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“…This suggests that the susceptibility to BKPyV might be enhanced by the transformed phenotype of cancer host cells, which often involve altered signal transduction and metabolic pathways 54, 55. For our study, we used the well‐characterized BKPyV(Dun) strain, which is derived from the original Gardner strain 56, and replicates similarly to natural variants found in KT patients 16. Also, different donor sources of RPTECs were used with indistinguishable results, suggesting that our results would apply to most KT recipients.…”

Section: Discussionmentioning

confidence: 99%

BK Polyomavirus Replication in Renal Tubular Epithelial Cells Is Inhibited by Sirolimus, but Activated by Tacrolimus Through a Pathway Involving FKBP-12

Hirsch

Yakhontova

et al. 2016

American Journal of Transplantation

105

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BK polyomavirus (BKPyV) replication causes nephropathy and premature kidney transplant failure. Insufficient BKPyV‐specific T cell control is regarded as a key mechanism, but direct effects of immunosuppressive drugs on BKPyV replication might play an additional role. We compared the effects of mammalian target of rapamycin (mTOR)‐ and calcineurin‐inhibitors on BKPyV replication in primary human renal tubular epithelial cells. Sirolimus impaired BKPyV replication with a 90% inhibitory concentration of 4 ng/mL by interfering with mTOR–SP6‐kinase activation. Sirolimus inhibition was rapid and effective up to 24 h postinfection during viral early gene expression, but not thereafter, during viral late gene expression. The mTORC‐1 kinase inhibitor torin‐1 showed a similar inhibition profile, supporting the notion that early steps of BKPyV replication depend on mTOR activity. Cyclosporine A also inhibited BKPyV replication, while tacrolimus activated BKPyV replication and reversed sirolimus inhibition. FK binding protein 12kda (FKBP‐12) siRNA knockdown abrogated sirolimus inhibition and increased BKPyV replication similar to adding tacrolimus. Thus, sirolimus and tacrolimus exert opposite effects on BKPyV replication in renal tubular epithelial cells by a mechanism involving FKBP‐12 as common target. Immunosuppressive drugs may therefore contribute directly to the risk of BKPyV replication and nephropathy besides suppressing T cell functions. The data provide rationales for clinical trials aiming at reducing the risk of BKPyV replication and disease in kidney transplantation.

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Section: Discussionmentioning

confidence: 99%

BK Polyomavirus Replication in Renal Tubular Epithelial Cells Is Inhibited by Sirolimus, but Activated by Tacrolimus Through a Pathway Involving FKBP-12

Hirsch

Yakhontova

et al. 2016

American Journal of Transplantation

105

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“…The variation of NCCRs has been described in renal transplant patients and is associated with an increased replication and the onset of BKVAN [Gosert et al, 2008;Olsen et al, 2006]. In contrast to the architectural rearrangement of NCCRs, the consequences of mutations within the VP1-loop have not been examined in vivo.…”

Section: Discussionmentioning

confidence: 99%

“…The reasons for the reactivation of BKV are not well understood. Among various other discussed risk factors, virus-specific determinants were investigated as well [Smith et al, 1998;Boldorini et al, 2001;Chen et al, 2001;Randhawa et al, 2003;Carr et al, 2006;Gosert et al, 2008]. The polyomavirus genome encodes for the agnoprotein, the capsid proteins VP1-3 and the small and large T-antigen.…”

Section: Introductionmentioning

confidence: 99%

Mutations in the BC‐loop of the BKV VP1 region do not influence viral load in renal transplant patients

Krautkrämer

Klein

Sommerer

et al. 2008

Journal of Medical Virology

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The reactivation and replication of the BK polyomavirus (BKV) leading to BKV-associated nephropathy (BKVAN) is one of the major complications in renal transplantation patients. BKV isolates were classified into four subtypes (I-IV) based on genotype variations within the VP1-coding region. The type-specific amino acid differences cluster within the BC-loop of the major capsid protein VP1. As demonstrated in vitro, mutations in this region also play a role in the infectivity, attachment and stability of viral particles. Therefore, we analyzed the prevalence of BC-loop mutations in isolates of kidney transplant patients and compared their viral load in the urine. The VP1 subtyping regions of BKV isolates obtained from urine samples of 45 renal transplant patients were sequenced. The phylogenetic analysis of these sequences revealed that subtype I (66.67%) is the most prevalent genotype. The remaining isolates belong to subtype IV (33.33%). A high frequency of changes to specific amino acids within the BC-loop was identified among the BKV isolates from renal transplant patients. Patients with BKVAN exhibited a higher viral replication than patients without nephropathy. Although titers of isolates of subtype I were higher than titers of subtype IV isolates, the difference did not reach statistical significance. In addition, amino acid changes in the BC-loop did not influence the viral load and the incidence of BKVAN. These in vivo results demonstrate that high replication rates which serve as a predictive marker for BKVAN are not caused by altered receptor binding or affinity via mutated BC-loops.

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“…The NCCR sequence showed no rearrangements indicating that the pathology of JCPyVAN occurs without rr-NCCR. This is similar to BKPyVAN, which arises with at-NCCR BKPyV that are, however, subsequently replaced by rr-NCCR BKPyV variants as majority species if uncontrolled virus replication has been ongoing for some time (243). The factors permitting relatively high-level replication of the JCPyV archetype in the urinary tract of immunocompetent individuals and causing invasive renal disease in some kidney transplant and HIV patients are currently undefined.…”

Section: Jcpyv Diseasementioning

confidence: 99%

The human JC polyomavirus (JCPyV): virological background and clinical implications

Hirsch

Kardas

Kranz

et al. 2013

APMIS

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138

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JC polyomavirus (JCPyV) was the first of now 12 PyVs detected in humans, when in 1964, PyV particles were revealed by electron microscopy in progressive multifocal leukoencephalopathy (PML) tissues. JCPyV infection is common in 35–70% of the general population, and the virus thereafter persists in the renourinary tract. One third of healthy adults asymptomatically shed JCPyV at approximately 50 000 copies/mL urine. PML is rare having an incidence of <0.3 per 100 000 person years in the general population. This increased to 2.4 per 1000 person years in HIV‐AIDS patients without combination antiretroviral therapy (cART). Recently, PML emerged in multiple sclerosis patients treated with natalizumab to 2.13 cases per 1000 patients. Natalizumab blocks α4‐integrin‐dependent lymphocyte homing to the brain suggesting that not the overall cellular immunodeficiency but local failure of brain immune surveillance is a pivotal factor for PML. Recovering JCPyV‐specific immune control, e.g., by starting cART or discontinuing natalizumab, significantly improves PML survival, but is challenged by the immune reconstitution inflammatory syndrome. Important steps of PML pathogenesis are undefined, and antiviral therapies are lacking. New clues might come from molecular and functional profiling of JCPyV and PML pathology and comparison with other replicative pathologies such as granule cell neuronopathy and (meningo‐)encephalitis, and non‐replicative JCPyV pathology possibly contributing to some malignancies. Given the increasing number of immunologically vulnerable patients, a critical reappraisal of JCPyV infection, replication and disease seems warranted.

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Polyomavirus BK with rearranged noncoding control region emerge in vivo in renal transplant patients and increase viral replication and cytopathology

Cited by 187 publications

References 49 publications

BK Polyomavirus Replication in Renal Tubular Epithelial Cells Is Inhibited by Sirolimus, but Activated by Tacrolimus Through a Pathway Involving FKBP-12

BK Polyomavirus Replication in Renal Tubular Epithelial Cells Is Inhibited by Sirolimus, but Activated by Tacrolimus Through a Pathway Involving FKBP-12

Mutations in the BC‐loop of the BKV VP1 region do not influence viral load in renal transplant patients

The human JC polyomavirus (JCPyV): virological background and clinical implications

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