Activation of the innate immune response against DENV in normal non-transformed human fibroblasts

Activation of the innate immune response against DENV in normal non-transformed human fibroblasts

When mosquitoes infected with DENV are feeding, the proboscis must traverse the epidermis several times ("probing") before reaching a blood vessel in the dermis. During this process, the salivary glands release the virus, which is likely to interact first with cells of the various epiderma...

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Veröffentlicht in:PLoS neglected tropical diseases 2011-12, Vol.5 (12), p.e1420-e1420
Hauptverfasser: Bustos-Arriaga, José, García-Machorro, Jazmín, León-Juárez, Moisés, García-Cordero, Julio, Santos-Argumedo, Leopoldo, Flores-Romo, Leopoldo, Méndez-Cruz, A René, Juárez-Delgado, Francisco J, Cedillo-Barrón, Leticia
Format: Artikel
Sprache:eng
Schlagworte:
beta-Defensins - immunology
beta-Defensins - metabolism
Biology
Cells, Cultured
Dengue
Dengue Virus - immunology
Epidermis
Fibroblasts
Fibroblasts - immunology
Fibroblasts - virology
Flow Cytometry
Gene Expression Profiling
Genetic aspects
Health aspects
Humans
Immune response
Immune system
Immunity, Innate
Infections
Interferons - immunology
Interferons - metabolism
Medicine
Microscopy, Fluorescence
Physiological aspects
Prevention
Proteins
Receptors, Immunologic - immunology
Receptors, Immunologic - metabolism
Reverse Transcriptase Polymerase Chain Reaction
Risk factors
Signal Transduction
Skin - cytology
Studies
Translocation
Tropical diseases
Tumor Necrosis Factor-alpha - immunology
Tumor Necrosis Factor-alpha - metabolism
Viral Plaque Assay
Virus Replication
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Zusammenfassung:When mosquitoes infected with DENV are feeding, the proboscis must traverse the epidermis several times ("probing") before reaching a blood vessel in the dermis. During this process, the salivary glands release the virus, which is likely to interact first with cells of the various epidermal and dermal layers, cells which could be physiologically relevant to DENV infection and replication in humans. However, important questions are whether more abundant non-hematopoietic cells such as fibroblasts become infected, and whether they play any role in antiviral innate immunity in the very early stages of infection, or even if they might be used by DENV as primary replication cells. Fibroblasts freshly released from healthy skin and infected 12 hours after their isolation show a positive signal for DENV. In addition, when primary skin fibroblast cultures were established and subsequently infected, we showed DENV-2 antigen-positive intracellular signal at 24 hours and 48 hours post-infection. Moreover, the fibroblasts showed productive infection in a conventional plaque assay. The skin fibroblasts infected with DENV-2 underwent potent signaling through both TLR3 and RIG- 1, but not Mda5, triggering up-regulation of IFNβ, TNFα, defensin 5 (HB5) and β defensin 2 (HβD2). In addition, DENV infected fibroblasts showed increased nuclear translocation of interferon (IFN) regulatory factor 3 (IRF3), but not interferon regulatory factor 7 (IRF7), when compared with mock-infected fibroblasts. In this work, we demonstrated the high susceptibility to DENV infection by primary fibroblasts from normal human skin, both in situ and in vitro. Our results suggest that these cells may contribute to the pro-inflammatory and anti-viral microenvironment in the early stages of interaction with DENV-2. Furthermore, the data suggest that fibroblast may also be used as a primary site of DENV replication and provide viral particles that may contribute to subsequent viral dissemination.
ISSN:1935-2735
1935-2727
1935-2735
DOI:10.1371/journal.pntd.0001420