Different Innate Signatures Induced in Human Monocyte-derived Dendritic Cells by Wild-Type Dengue 3 Virus, Attenuated but Reactogenic Dengue 3 Vaccine Virus, or Attenuated Nonreactogenic Dengue 1-4 Vaccine Virus Strains

Balas, Claire; Kennel, Audrey; Deauvieau, Florence; Sodoyer, Régis; Arnaud-Barbe, Nadège; Lang, Jean; Guy, Bruno

doi:10.1093/infdis/jiq022

Cited by 34 publications

(34 citation statements)

References 15 publications

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“…The data presented here could be of help to enhance understanding of the severe or fatal outcomes observed in several dengue patients, as previously suggested (2). Finally, in view of our data and taking into account previous results by Palmer et al (34) in studies of the deficient activation of T cells by DCs infected with DENV, the high infection and apoptosis levels observed in DENV3/5532-infected mdDCs could impair DENV3 antigen presentation to T lymphocytes, affecting adaptive immune responses.…”

Section: Vol 85 2011 Denv-3 Induces Inflammatory Responses In Mddcssupporting

confidence: 80%

Dengue Virus Type 3 Isolated from a Fatal Case with Visceral Complications Induces Enhanced Proinflammatory Responses and Apoptosis of Human Dendritic Cells

Silveira

Meyer

Delfraro

et al. 2011

J Virol

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. Strain DENV3/5532 was found to display significantly higher replicative ability than DENV3/ 290 in monocyte-derived dendritic cells (mdDCs). In addition, compared to DENV3/290 results, mdDCs exposed to DENV3/5532 showed increased production of proinflammatory cytokines associated with higher rates of programmed cell death, as shown by annexin V staining. The observed phenotype was due to viral replication, and tumor necrosis factor alpha (TNF-␣) appears to exert a protective effect on virus-induced mdDC apoptosis. These results suggest that the DENV3/5532 strain isolated from the fatal case replicates within human dendritic cells, modulating cell survival and synthesis of inflammatory mediators.

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Section: Vol 85 2011 Denv-3 Induces Inflammatory Responses In Mddcssupporting

confidence: 80%

Dengue Virus Type 3 Isolated from a Fatal Case with Visceral Complications Induces Enhanced Proinflammatory Responses and Apoptosis of Human Dendritic Cells

Silveira

Meyer

Delfraro

et al. 2011

J Virol

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“…In general, the gene expression results were consistent with the degree of toxic effects observed in more traditional assays, such as the abnormal toxicity test and the leukopenic toxicity test (72)(73)(74). More recently, the systems vaccinology approach describes using the genome-wide gene expression underlying the host responses to vaccination (75)(76)(77)(78). In these studies, blood signature genes associated with B cell or T cell response were flagged as potential biomarkers to help differentiate vaccine efficacy or immunogenicity.…”

Section: Safetysupporting

confidence: 56%

Strategic Applications of Gene Expression: From Drug Discovery/Development to Bedside

Bai

Alekseyenko

Statnikov

et al. 2013

AAPS J

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ABSTRACT. Gene expression is useful for identifying the molecular signature of a disease and for correlating a pharmacodynamic marker with the dose-dependent cellular responses to exposure of a drug. Gene expression offers utility to guide drug discovery by illustrating engagement of the desired cellular pathways/networks, as well as avoidance of acting on the toxicological pathways. Successful employment of gene-expression signatures in the later stages of drug development depends on their linkage to clinically meaningful phenotypic characteristics and requires a biologically meaningful mechanism combined with a stringent statistical rigor. Much of the success in clinical drug development is hinged on predefining the signature genes for their fitness for purposes of application. Specific examples are highlighted to illustrate the breadth and depth of the potential utility of gene-expression signatures in drug discovery and clinical development to targeted therapeutics at the bedside.

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“…However, gene expression profiles indirectly measure the antibody response, not the specificity of antibody reactivity. In the case of attenuated dengue fever vaccines, gene expression profiles were identical for different serotypes (21) and are not descriptive of the adverse response of vaccination with the wrong serotypes of virus (22,23). Immunosignatures should provide a valuable addition to systems vaccinology, and at times may alone be sufficient for evaluation.…”

Section: Discussionmentioning

confidence: 99%

Immunosignatures can predict vaccine efficacy

Legutki

Johnston

2013

Proc. Natl. Acad. Sci. U.S.A.

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The development of new vaccines would be greatly facilitated by having effective methods to predict vaccine performance. Such methods could also be helpful in monitoring individual vaccine responses to existing vaccines. We have developed "immunosignaturing" as a simple, comprehensive, chip-based method to display the antibody diversity in an individual on peptide arrays. Here we examined whether this technology could be used to develop correlates for predicting vaccine effectiveness. By using a mouse influenza infection, we show that the immunosignaturing of a natural infection can be used to discriminate a protective from nonprotective vaccine. Further, we demonstrate that an immunosignature can determine which mice receiving the same vaccine will survive. Finally, we show that the peptides comprising the correlate signatures of protection can be used to identify possible epitopes in the influenza virus proteome that are correlates of protection.peptide microarray | systems vaccinology | epitope prediction | antibody repertoire | immune profile

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Different Innate Signatures Induced in Human Monocyte-derived Dendritic Cells by Wild-Type Dengue 3 Virus, Attenuated but Reactogenic Dengue 3 Vaccine Virus, or Attenuated Nonreactogenic Dengue 1-4 Vaccine Virus Strains

Cited by 34 publications

References 15 publications

Dengue Virus Type 3 Isolated from a Fatal Case with Visceral Complications Induces Enhanced Proinflammatory Responses and Apoptosis of Human Dendritic Cells

Dengue Virus Type 3 Isolated from a Fatal Case with Visceral Complications Induces Enhanced Proinflammatory Responses and Apoptosis of Human Dendritic Cells

Strategic Applications of Gene Expression: From Drug Discovery/Development to Bedside

Immunosignatures can predict vaccine efficacy

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