Uncovering the Interplay Between CD8, CD4 and Antibody Responses to Complex Pathogens

Moutaftsi, Magdalini; Tscharke, David C.; Vaughan, Kerrie; Koelle, David M.; Stern, Lawrence J.; Calvo-Calle, Mauricio; Ennis, Francis A.; Terajima, Masanori; Sutter, Gerd; Crotty, Shane; Drexler, Ingo; Franchini, Genoveffa; Yewdell, Jonathan W.; Head, Steven R.; Blum, Janice S.; Peters, Bjoern; Sette, Alessandro

doi:10.2217/fmb.09.110

Cited by 65 publications

(81 citation statements)

References 113 publications

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“…Of these, the arrays detected strong antibody signals against US6/gD (from both HSV-1 and -2) and UL48 of HSV-2, both of which are also CD4 ϩ target antigens. The overlap between the targets of antibody and CD4 ϩ cells, rather than CD8 ϩ cells, is also consistent with recent findings for vaccinia virus antigens (36,59,60). Further investigations of T-cell responses to ID-A-Ags versus ID-S-Ags may be needed to break new ground in our understanding of the protective versus pathogenic immune mechanisms against ocular, orofacial, and genital herpes.…”

Section: Fig 4 Intensities Of Antibody Responses Against Four Immunodsupporting

confidence: 84%

“…The symptomatic and asymptomatic B-cell antigens identified in this study would certainly help speed up the identification of more symptomatic and asymptomatic T-cell antigens by serodiagnosing more symptomatic and asymptomatic individuals. In addition, many HSV and non-HSV antigens tend to contain both B-and T-cell epitopes (36,59,60). It was suggested previously that the most immunodominant B-cell antigens in HSV may be those of envelope proteins, such as the envelope glycoproteins UL27/gB and US6/gD (10).…”

Section: Fig 4 Intensities Of Antibody Responses Against Four Immunodmentioning

confidence: 99%

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Immunodominant “Asymptomatic” Herpes Simplex Virus 1 and 2 Protein Antigens Identified by Probing Whole-ORFome Microarrays with Serum Antibodies from Seropositive Asymptomatic versus Symptomatic Individuals

Dasgupta

Chentoufi

Kalantari

et al. 2012

J Virol

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cHerpes simplex virus 1 (HSV-1) and HSV-2 are medically significant pathogens. The development of an effective HSV vaccine remains a global public health priority. HSV-1 and HSV-2 immunodominant "asymptomatic" antigens (ID-A-Ags), which are strongly recognized by B and T cells from seropositive healthy asymptomatic individuals, may be critical to be included in an effective immunotherapeutic HSV vaccine. In contrast, immunodominant "symptomatic" antigens (ID-S-Ags) may exacerbate herpetic disease and therefore must be excluded from any HSV vaccine. In the present study, proteome microarrays of 88 HSV-1 and 84 HSV-2 open reading frames(ORFs) (ORFomes) were constructed and probed with sera from 32 HSV-1-, 6 HSV-2-, and 5 HSV-1/HSV-2-seropositive individuals and 47 seronegative healthy individuals (negative controls). The proteins detected in both HSV-1 and HSV-2 proteome microarrays were further classified according to their recognition by sera from HSV-seropositive clinically defined symptomatic (n ‫؍‬ 10) and asymptomatic (n ‫؍‬ 10) individuals. We found that (i) serum antibodies recognized an average of 6 ORFs per seropositive individual; (ii) the antibody responses to HSV antigens were diverse among HSV-1-and HSV-2-seropositive individuals; (iii) panels of 21 and 30 immunodominant antigens (ID-Ags) were identified from the HSV-1 and HSV-2 ORFomes, respectively, as being highly and frequently recognized by serum antibodies from seropositive individuals; and (iv) interestingly, four HSV-1 and HSV-2 cross-reactive asymptomatic ID-A-Ags, US4, US11, UL30, and UL42, were strongly and frequently recognized by sera from 10 of 10 asymptomatic patients but not by sera from 10 of 10 symptomatic patients (P < 0.001). In contrast, sera from symptomatic patients preferentially recognized the US10 ID-S-Ag (P < 0.001). We have identified previously unreported immunodominant HSV antigens, among which were 4 ID-A-Ags and 1 ID-S-Ag. These newly identified ID-A-Ags could lead to the development of an efficient "asymptomatic" vaccine against ocular, orofacial, and genital herpes.

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Section: Fig 4 Intensities Of Antibody Responses Against Four Immunodsupporting

confidence: 84%

Section: Fig 4 Intensities Of Antibody Responses Against Four Immunodmentioning

confidence: 99%

Immunodominant “Asymptomatic” Herpes Simplex Virus 1 and 2 Protein Antigens Identified by Probing Whole-ORFome Microarrays with Serum Antibodies from Seropositive Asymptomatic versus Symptomatic Individuals

Dasgupta

Chentoufi

Kalantari

et al. 2012

J Virol

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“…10C. The genes for top-ranked CD8 ϩ T cell antigens are predominantly in the early class, as noted previously (6,8,19). The genes for top-ranked CD4 ϩ T cell and B cell antigens are mostly synthesized after DNA replication but with a higher proportion in the intermediate than the late class (Fig.…”

Section: Discussionsupporting

confidence: 69%

“…A recent review summarized the VACV antigens recognized by CD8 ϩ T cells, CD4 ϩ T cells, and B cells (19). The distribution of these antigenic proteins in different expression classes is shown in Fig.…”

Section: Discussionmentioning

confidence: 99%

Expression Profiling of the Intermediate and Late Stages of Poxvirus Replication

Yang

Reynolds

Martens

et al. 2011

J Virol

118

146

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“…poxvirus infection, the vast majority of peptides that could in principle be recognized by the immune system in any context of immune exposure are not. 34,52 There are multiple aspects influencing immunodominance that impact which epitopes ultimately get recognized, ranging from variables associated with the antigen encoding the epitope (such as its abundance, cellular localization or kinetics of transcription), as well as conservation/cross-reactivity with other immune targets. These are also all relevant in the cancer setting, where expression level of the antigen itself, and the clonality of a mutation within the cancer cell population both impact the likelihood of detecting an immune response against it.…”

Section: Discussionmentioning

confidence: 99%

Predicting T cell recognition of MHC class I restricted neoepitopes

et al. 2018

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Epitopes that arise from a somatic mutation, also called neoepitopes, are now known to play a key role in cancer immunology and immunotherapy. Recent advances in high-throughput sequencing have made it possible to identify all mutations and thereby all potential neoepitope candidates in an individual cancer. However, most of these neoepitope candidates are not recognized by T cells of cancer patients when tested in vivo or in vitro, meaning they are not immunogenic. Especially in patients with a high mutational load, usually hundreds of potential neoepitopes are detected, highlighting the need to further narrow down this candidate list. In our study, we assembled a dataset of known, naturally processed, immunogenic neoepitopes to dissect the properties that make these neoepitopes immunogenic. The tools to use and thresholds to apply for prioritizing neoepitopes have so far been largely based on experience with epitope identification in other settings such as infectious disease and allergy. Here, we performed a detailed analysis on our dataset of curated immunogenic neoepitopes to establish the appropriate tools and thresholds in the cancer setting. To this end, we evaluated different predictors for parameters that play a role in a neoepitope’s immunogenicity and suggest that using binding predictions and length-rescaling yields the best performance in discriminating immunogenic neoepitopes from a background set of mutated peptides. We furthermore show that almost all neoepitopes had strong predicted binding affinities (as expected), but more surprisingly, the corresponding non-mutated peptides had nearly as high affinities. Our results provide a rational basis for parameters in neoepitope filtering approaches that are being commonly used.Abbreviations: SNV: single nucleotide variant; nsSNV: nonsynonymous single nucleotide variant; ROC: receiver operating characteristic; AUC: area under ROC curve; HLA: human leukocyte antigen; MHC: major histocompatibility complex; PD-1: Programmed cell death protein 1; PD-L1 or CTLA-4: cytotoxic T-lymphocyte associated protein 4

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Uncovering the Interplay Between CD8, CD4 and Antibody Responses to Complex Pathogens

Cited by 65 publications

References 113 publications

Immunodominant “Asymptomatic” Herpes Simplex Virus 1 and 2 Protein Antigens Identified by Probing Whole-ORFome Microarrays with Serum Antibodies from Seropositive Asymptomatic versus Symptomatic Individuals

Immunodominant “Asymptomatic” Herpes Simplex Virus 1 and 2 Protein Antigens Identified by Probing Whole-ORFome Microarrays with Serum Antibodies from Seropositive Asymptomatic versus Symptomatic Individuals

Expression Profiling of the Intermediate and Late Stages of Poxvirus Replication

Predicting T cell recognition of MHC class I restricted neoepitopes

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