Variations in BK Polyomavirus Immunodominant Large Tumor Antigen-Specific 9mer CD8 T-Cell Epitopes Predict Altered HLA-Presentation and Immune Failure

Leuzinger, Karoline; Kaur, Amandeep; Wilhelm, Maud; Hirsch, Hans H.

doi:10.3390/v12121476

Cited by 6 publications

(12 citation statements)

References 51 publications

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“…Thus, BKPyV replication after allogeneic HCT may result from (1) reactivation and high-level viruria of the recipient BKPyV during the allogeneic HCT immune gap; (2) exposure to immunosuppressive drugs for GVHD prophylaxis [ 9 , 43 ]; (3) impaired serotype Vp1 antibody and corresponding LTag genotype-specific T-cell control; and (4) viral variants escaping T-cell control [ 24 ]. Based on the findings of this study, prospective clinical studies can be designed to investigate the diagnostic and functional role as well as the prevalence and magnitude of these steps and may help to optimize antiviral strategies as well as vaccination and adoptive transfer of nAbs and T cells [ 41 , 44 , 45 ].…”

Section: Discussionmentioning

confidence: 99%

“…Single immunodominant 9mers are presented by several HLA types such as HLA-B7, HLA-B8, and HLA-B51 linked to protection from BKPyV replication [ 22 , 23 ]. Analyzing publicly available BKPyV genome sequences has revealed non-synonymous amino acid exchanges in immunodominant LTag 9mers, which significantly reduced HLA-A/HLA-B binding and reduced or abrogated 9mer-specific CD8 T-cell responses [ 24 ]. Based on these findings, we conducted a detailed molecular characterization of urine and plasma BKPyV loads in our allogeneic HCT patients [ 25 ].…”

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confidence: 99%

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Molecular Characterization of BK Polyomavirus Replication in Allogeneic Hematopoietic Cell Transplantation Patients

Leuzinger

Kaur

Wilhelm

et al. 2022

The Journal of Infectious Diseases

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Background High-level BK polyomavirus (BKPyV) replication in allogeneic hematopoietic cell transplantation (HCT) predicts failing immune control and BKPyV-associated hemorrhagic cystitis (BKPyV-HC). Methods To identify molecular markers of BKPyV-replication and disease, we scrutinized BKPyV-DNA loads in longitudinal urine and plasma pairs from 20 HCT-patients using quantitative nucleic-acid-testing (QNAT), DNase-I treatment prior to QNAT, next-generation-sequencing (NGS) and tested cell-mediated immunity. Results We found that larger QNAT amplicons led to under-quantification and false-negatives results (p < 0.001). DNase-I reduced urine and plasma BKPyV-loads by >90% (p < 0.001) indicating non-encapsidated BKPyV-genomes. DNase-resistant urine BKPyV-loads remained infectious in cell culture. BKPyV-genome fragmentation of ≤250 bp impaired NGS-coverage of genetic variation using 1000 bp and 5000 bp targets. Conversely, 250bp-amplicons captured viral minority variants. We identified genotype-specific and genotype-independent changes in capsid-Vp1 or large T-antigen predicted to escape from antibody neutralization or HLA-presentation to CD8 T-cells, respectively. Genotype-specific changes in immunodominant 9mers were associated with reduced or absent CD8 T-cell responses. Thus, failure to control BKPyV-replication in HCT-patients may involve insufficient genotype-specific cytotoxic CD8 T-cell responses potentially predictable by low neutralizing antibodies as well as genotype-independent immune escape of variants. Conclusion Our results provide new insights for patient evaluation and for designing immune protection through neutralizing antibodies, adoptive T-cell therapy or vaccines.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

Molecular Characterization of BK Polyomavirus Replication in Allogeneic Hematopoietic Cell Transplantation Patients

Leuzinger

Kaur

Wilhelm

et al. 2022

The Journal of Infectious Diseases

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“…The characterisation of the underlying molecular pathogenesis is highly relevant for effective treatment approaches in conjunction with HPyV-specific immunity. Although lasting immune control is the ultimate goal of antiviral therapy, be it by reconstitution, adoptive transfer or vaccination, [22][23][24] we focus here on small-molecule drugs and compounds potentially bridging this gap and disregard immune therapies. Antiviral treatment is needed for treating replicative HPyV diseases such as PyVAN and PyVHC, whereas specific inhibitors blocking the oncogenic activity of small T-antigen (sTag) or large T-antigen (LTag) may be needed for treating hyperproliferative and transforming activities seen HPyVassociated diseases and outright cancers.…”

Section: Human Polyomaviruses and Associated Diseasesmentioning

confidence: 99%

“…Approximately 10% of healthy BKPyV-seropositive blood donors asymptomatically shed BKPyV in urine, 19 indicating regular escape from immune control, despite specific neutralizing antibodies and T-cells. 22,24,27 PyVAN occurs in 1%-15% of kidney transplant patients. 25 Uncontrolled BKPyV replication in renal tubule epithelial cells causes progressive cytopathology, denudation, interstitial and tubular inflammation, interstitial fibrosis, and eventually tubular atrophy (Figure 1), thereby leading to irreversible loss of allograft function and premature return to renal replacement therapy.…”

Section: Bkpyv-associated Diseasesmentioning

confidence: 99%

Antivirals against human polyomaviruses: Leaving no stone unturned

Hirsch

2021

Reviews in Medical Virology

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Human polyomaviruses (HPyVs) encompass more than 10 species infecting 30%-90% of the human population without significant illness. Proven HPyV diseases with documented histopathology affect primarily immunocompromised hosts with manifestations in brain, skin and renourinary tract such as polyomavirus-associated nephropathy (PyVAN), polyomavirus-associated haemorrhagic cystitis (PyVHC), polyomavirus-associated urothelial cancer (PyVUC), progressive multifocal leukoencephalopathy (PML), Merkel cell carcinoma (MCC), Trichodysplasia spinulosa (TS) and pruritic hyperproliferative keratinopathy. Although virus-specific immune control is the eventual goal of therapy and lasting cure, antiviral treatments are urgently needed in order to reduce or prevent HPyV diseases and thereby bridging the time needed to establish virus-specific immunity. However, the small dsDNA genome of only 5 kb of the non-enveloped HPyVs only encodes 5-7 viral proteins. Thus, HPyV replication relies heavily on host cell factors, thereby limiting both, number and type of specific virus-encoded antiviral targets. Lack of cost-effective high-throughput screening systems and relevant small animal models complicates the preclinical development. Current clinical studies are limited by small case

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“…Since there are no effective antiviral drugs for treatment or prevention of BKPyV replication and associated diseases (9), current clinical management relies on reconstituting BKPyV-specific humoral and cellular immunity. However, our earlier work has identified significant changes in 9mer epitopes which were associated with failure of CD8 T cells to activate polyfunctional responses, to kill and to proliferate (10)(11)(12).…”

Section: Introductionmentioning

confidence: 97%

Structural implications of BK polyomavirus sequence variations in the major viral capsid protein Vp1 and large T-antigen: a computational study

Durairaj,

Follonier,

Leuzinger

et al. 2023

Preprint

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BK polyomavirus (BKPyV) is a double-stranded DNA virus causing nephropathy, hemorrhagic cystitis, and urothelial cancer in transplant patients. The BKPyV-encoded capsid protein Vp1 and large T-antigen (LTag) are key targets of neutralizing antibodies and cytotoxic T-cells, respectively. Our single-center data suggested that variability in Vp1 and LTag may contribute to failing BKPyV-specific immune control, and impact vaccine design. We therefore analyzed all available entries in GenBank (1516VP1; 742LTAG)and explored potential structural effects using computational approaches. BKPyV-genotype (gt)1 was found in 71.18% of entries, followed by BKPyV-gt4 (19.26%), BKPyV-gt2 (8.11%) and BKPyV-gt3 (1.45%), but rates differed according to country and specimen type. Vp1-mutations matched a serotype different than the assigned one or were serotype-independent in 43%, 18% affected more than one amino acid. Notable Vp1-mutations altered antibody-binding domains, interactions with sialic acid receptors, or were predicted to change conformation. LTag-sequences were more conserved, with only 16 mutations detectable in more than one entry and without significant effects on LTag-structure or interaction domains. However, LTag changes were predicted to affect HLA-class I presentation of immunodominant 9mers to cytotoxic T-cells. These global data strengthen single center observations and specifically our earlier findings revealing mutant 9mer epitopes conferring immune escape from HLA-I cytotoxic T cells. We conclude that variability of BKPyV-Vp1 and LTag may have important implications for diagnostic assays assessing BKPyV-specific immune control and for vaccine design.IMPORTANCEType and rate of amino acid variations in BKPyV may provide important insights into BKPyV diversity in human populations and an important step towards defining determinants of BKPyV-specific immunity needed to protect vulnerable patients from BKPyV diseases. Our analysis of BKPyV sequences obtained from human specimens reveals an unexpectedly high genetic variability for this double-stranded DNA virus that strongly relies on host cell DNA replication machinery with its proof reading and error correction mechanisms. BKPyV variability and immune escape should be taken into account when designing further approaches to antivirals, monoclonal antibodies and vaccines for patients at risk of BKPyV diseases.

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Variations in BK Polyomavirus Immunodominant Large Tumor Antigen-Specific 9mer CD8 T-Cell Epitopes Predict Altered HLA-Presentation and Immune Failure

Cited by 6 publications

References 51 publications

Molecular Characterization of BK Polyomavirus Replication in Allogeneic Hematopoietic Cell Transplantation Patients

Molecular Characterization of BK Polyomavirus Replication in Allogeneic Hematopoietic Cell Transplantation Patients

Antivirals against human polyomaviruses: Leaving no stone unturned

Structural implications of BK polyomavirus sequence variations in the major viral capsid protein Vp1 and large T-antigen: a computational study

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