Vaccinia virus inoculation in sites of allergic skin inflammation elicits a vigorous cutaneous IL-17 response

Oyoshi, Michiko K.; Elkhal, Abdallah; Kumar, Lalit; Scott, Jordan E.; Koduru, Suresh; He, Rui; Leung, Donald Y.M.; Howell, Michael D.; Oettgen, Hans C.; Murphy, Gëorge F.; Geha, Raif S.

doi:10.1073/pnas.0904021106

Cited by 40 publications

(70 citation statements)

References 27 publications

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“…Two reports suggest that Th17 cells exacerbate dermatitis because increased numbers of Th17 cells were found in the peripheral blood and acute lesional skin of AD patients (31). Kawakami et al (32) also support this idea with their study of NK cell function in AD patients (23). In contrast, two reports suggest that low IL-17 expression or reduced responses to IL-17 in the skin cause AD-like symptoms (24,33).…”

Section: Discussionsupporting

confidence: 51%

“…Proteins (5 mg) were fractionated by 10% SDS-PAGE and transferred onto a Hybond-P polyvinylidene difluoride membrane (GE Healthcare, Buckinghamshire, U.K.). A rabbit polyclonal Ab raised against TRAF3IP2 (anti-Act1 [H-300]) was obtained commercially (Santa Cruz Biotechnology, Santa Cruz, CA) and has been characterized previously (23,24). The Ab was used at a dilution of 1:400.…”

Section: Western Blottingmentioning

confidence: 99%

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An Atopic Dermatitis-Like Skin Disease with Hyper-IgE-emia Develops in Mice Carrying a Spontaneous Recessive Point Mutation in theTraf3ip2(Act1/CIKS) Gene

Matsushima

Kikkawa

Takada

et al. 2010

The Journal of Immunology

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Spontaneous mutant mice that showed high levels of serum IgE and an atopic dermatitis (AD)-like skin disease were found in a colony of the KOR inbred strain that was derived from Japanese wild mice. No segregation was observed between hyper-IgE-emia and dermatitis in (BALB/c × KOR mutant) N2 mice, suggesting that the mutation can be attributed to a single recessive locus, which we designated adjm (atopic dermatitis from Japanese mice). All four adjm congenic strains in different genetic backgrounds showed both hyper-IgE-emia and dermatitis, although the disease severity varied among strains. Linkage analysis using (BALB/c × KOR-adjm/adjm) N2 mice restricted the potential adjm locus to the 940 kb between D10Stm216 and D10Stm238 on chromosome 10. Sequence analysis of genes located in this region revealed that the gene AI429613, which encodes the mouse homologue of the human TNFR-associated factor 3-interacting protein 2 (TRAF3IP2) protein (formerly known as NF-κB activator 1/connection to IκB kinase and stress-activated protein kinase/Jun kinase), carried a single point mutation leading to the substitution of a stop codon for glutamine at amino acid position 214. TRAF3IP2 has been shown to function as an adaptor protein in signaling pathways mediated by the TNFR superfamily members CD40 and B cell-activating factor in epithelial cells and B cells as well as in the IL-17–mediated signaling pathway. Our results suggest that malfunction of the TRAF3IP2 protein causes hyper-IgE-emia through the CD40- and B cell-activating factor-mediated pathway in B cells and causes skin inflammation through the IL-17–mediated pathway. This study demonstrates that the TRAF3IP2 protein plays an important role in AD and suggests the protein as a therapeutic target to treat AD.

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Section: Discussionsupporting

confidence: 51%

Section: Western Blottingmentioning

confidence: 99%

An Atopic Dermatitis-Like Skin Disease with Hyper-IgE-emia Develops in Mice Carrying a Spontaneous Recessive Point Mutation in theTraf3ip2(Act1/CIKS) Gene

Matsushima

Kikkawa

Takada

et al. 2010

The Journal of Immunology

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“…Hou et al [23] reported that Th17 cells promote persistent viral infection in a model of chronic virus infection and IL-17 upregulates anti-apoptotic molecules and consequently increases persistent infection by enhancing the survival of virus-infected cells and blocking target cell destruction by cytotoxic T cells. Also, Oyoshi et al [24] reported that IL-17 contributes to viral replication in a model of disseminated vaccinia infection rather than providing host defense against viral infection.…”

Section: Discussionmentioning

confidence: 99%

T Helper Type 1/T Helper Type 17-Related Cytokines in Chronic Hepatitis C Patients before and after Interferon and Ribavirin Therapy

Fathy

Ahmed²,

Metwally³

et al. 2011

Med Princ Pract

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Objective: This study examined the T helper (Th) 1/Th17-related cytokines, interferon (IFN)-γ and interleukin (IL)-17 in the serum of biopsy-proven chronic hepatitis C patients before and after IFN and ribavirin therapy to address whether or not viral clearance is related to Th1/Th17 cytokines. Subjects and Methods: The serum levels of IFN-γ and IL-17 were assayed by ELISA on 26 patients with chronic hepatitic C virus (HCV) infection before the start and 3 months after treatment with pegylated IFN-α plus ribavarin and compared with sera from 15 normal control subjects. Results: IFN-γ and IL-17 levels are higher in the serum of patients with chronic hepatitis than in normal controls and these elevated levels were not directly correlated (r = –0.01, p = 0.96 for IFN-γ and r = –0.08, p = 0.66 for IL-17) to the viremic state of the HCV infection. In contrast to IL-17, IFN-γ showed significant reduction after 12 weeks of treatment with pegylated IFN plus ribavirin. However, IFN-γ and IL-17 serum levels were not significantly (p = 0.19 and = 0.70, respectively) different among responders and nonresponders for pegylated IFN plus ribavirin therapy. Conclusion: Our findings suggest that the combined treatment with pegylated IFN-α and ribavirin downmodulates the secretion of key cytokine IFN-γ as early as 12 weeks after treatment in infected patients. These findings could encourage new exciting possibilities for immune-based interventions with the aim of restoring functional antiviral T cell responses combined with improved viral clearance.

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“…Virus inoculation at sites of experimentally induced Th2-biased allergic skin inflammation resulted in more severe lesions, higher viral DNA loads in the skin and internal organs and more satellite lesions when compared to inoculation on unsensitized skin [36]. Local expression of IL-17 and ineffective T cell responses may also be involved in the susceptibility of patients with AD to EV [36,37,38]. …”

Section: Discussionmentioning

confidence: 99%

“…A number of animal models of EV have been explored by others to understand the biological and molecular basis for the potentially life-threatening VV dissemination which can be seen in some individuals after vaccination against smallpox [36,37,38]. Virus inoculation at sites of experimentally induced Th2-biased allergic skin inflammation resulted in more severe lesions, higher viral DNA loads in the skin and internal organs and more satellite lesions when compared to inoculation on unsensitized skin [36].…”

Section: Discussionmentioning

confidence: 99%

Susceptibility to Vaccinia Virus Infection and Spread in Mice Is Determined by Age at Infection, Allergen Sensitization and Mast Cell Status

Domenico

Lucas

Fujita

et al. 2012

Int Arch Allergy Immunol

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Background: Patients, especially young children, with atopic dermatitis are at an increased risk of developing eczema vaccinatum, a severe reaction to the smallpox vaccine, either through direct vaccination or indirect contact with a person recently vaccinated. Methods: Using a mouse model of infection, the severity of vaccinia-induced lesions was assessed from their appearance and viral DNA content. The response to vaccinia inoculation was assessed in young and adult mice, allergen-sensitized mice, and in mast cell-deficient mice. Results: Young age, sensitization to an allergen prior to infection, and a mast cell deficit, accomplished by using mast cell-deficient mice, resulted in more severe viral lesions at the site of inoculation, according to lesion appearance and viral DNA content. All three factors combined demonstrated maximal susceptibility, characterized by the severity of primary lesions and the development of secondary (satellite) lesions, as occurs in eczema vaccinatum in humans. Resistance to the appearance of satellite lesions could be restored by adoptive transfer of bone marrow-derived mast cells from either wild-type or cathelicidin-related antimicrobial peptide-deficient mice. Primary lesions were more severe following the latter transfer, indicating that cathelicidin-related antimicrobial peptide does contribute to the protective activity of mast cells against infection. Conclusions: The combination of young age, allergen sensitization and a mast cell deficit resulted in the most severe lesions, including satellite lesions. Understanding the factors determining the relative resistance/sensitivity to vaccinia virus will aid in the development of strategies for preventing and treating adverse reactions which can occur after smallpox vaccination.

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Vaccinia virus inoculation in sites of allergic skin inflammation elicits a vigorous cutaneous IL-17 response

Cited by 40 publications

References 27 publications

An Atopic Dermatitis-Like Skin Disease with Hyper-IgE-emia Develops in Mice Carrying a Spontaneous Recessive Point Mutation in theTraf3ip2(Act1/CIKS) Gene

An Atopic Dermatitis-Like Skin Disease with Hyper-IgE-emia Develops in Mice Carrying a Spontaneous Recessive Point Mutation in theTraf3ip2(Act1/CIKS) Gene

T Helper Type 1/T Helper Type 17-Related Cytokines in Chronic Hepatitis C Patients before and after Interferon and Ribavirin Therapy

Susceptibility to Vaccinia Virus Infection and Spread in Mice Is Determined by Age at Infection, Allergen Sensitization and Mast Cell Status

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