2019
DOI: 10.1016/j.immuni.2019.02.003
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Human Memory B Cells Harbor Diverse Cross-Neutralizing Antibodies against BK and JC Polyomaviruses

Abstract: Graphical Abstract Highlights d Latent polyomavirus infections generate a potent, neutralizing antibody response d The anti-BKV repertoire is clonally diverse and harbors crossreactive antibodies d Memory IgM B cell receptors are affinity matured and isotype restricted d A monoclonal cross-neutralizing IgG binds a conserved quaternary viral epitope SUMMARY Human polyomaviruses cause a common childhood infection worldwide and typically elicit a neutralizing antibody and cellular immune response, while establish… Show more

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Cited by 51 publications
(73 citation statements)
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“…Refinement of both datasets produced maps at 3.9 Å and 4.2 Å resolution for the A2 and A2-Fab complex, respectively ( Figure 4B and Table S2) (Punjani et al, 2017;Zivanov et al, 2018). In contrast to the 60 epitopes present in the BKPyV:scFv structure (one per asymmetric unit), our complex map revealed density for 360 copies of 8A7H5Fab, corresponding to six copies per asymmetric unit, that is 1 Fab per each VP1 ( Figures S3A and S3B) (Lindner et al, 2019).…”
Section: Cryo Em Reconstruction Of Mupyv Identifies Mechanism Of Vp1 mentioning
confidence: 91%
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“…Refinement of both datasets produced maps at 3.9 Å and 4.2 Å resolution for the A2 and A2-Fab complex, respectively ( Figure 4B and Table S2) (Punjani et al, 2017;Zivanov et al, 2018). In contrast to the 60 epitopes present in the BKPyV:scFv structure (one per asymmetric unit), our complex map revealed density for 360 copies of 8A7H5Fab, corresponding to six copies per asymmetric unit, that is 1 Fab per each VP1 ( Figures S3A and S3B) (Lindner et al, 2019).…”
Section: Cryo Em Reconstruction Of Mupyv Identifies Mechanism Of Vp1 mentioning
confidence: 91%
“…recognized an epitope comprised of residues from VP1 proteins between hexavalent capsomers (Lindner et al, 2019). Thus, mutations may disrupt recognition by antibodies with epitopes distinct from that of 8A7H5.…”
Section: A2v296f Shows Poor Shedding Under Conditions Of Antibody Esmentioning
confidence: 99%
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“…The majority of this antibody’s epitope lies in the EF loop, distant from the receptor binding pocket and sites of PML mutations. However, a portion of the epitope contains several residues in the BC loop in the immediate vicinity of the frequently mutated L54 residue [ 126 ]. JCPyV mAbs generated from a natalizumab-treated PML patient provide evidence for a dominant nAb target in VP1 [ 127 ].…”
Section: Vp1 Mutations: Facilitating Immune Evasionmentioning
confidence: 99%
“…The tissue, cell type(s), and mechanisms responsible for generating VP1 mutations are not known; for JCPyV, kidney epithelia and certain glia have been suggested as possible locations [ 67 , 84 ]. PyV antibody-escape mutants can arise by serial passage in epithelial cells, indicating that these cells are capable of generating VP1 mutations [ 106 , 126 ]. Human glia engrafted in Mbps shi/shi Rag2 −/− mice also generate VP1 point mutations in JCPyV [ 67 ].…”
Section: How Do Vp1 Mutations Arise?mentioning
confidence: 99%