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7. Development and Progression of Radiologic Abnormalities in Individuals at Risk for Familial Interstitial Lung Disease

Author

Salisbury, Margaret L., primary, Hewlett, Justin C., additional, Ding, Guixiao, additional, Markin, Cheryl R., additional, Douglas, Katrina, additional, Mason, Wendi, additional, Guttentag, Adam, additional, Phillips, John A., additional, Cogan, Joy D., additional, Reiss, Sara, additional, Mitchell, Daphne B., additional, Wu, Pingsheng, additional, Young, Lisa R., additional, Lancaster, Lisa H., additional, Loyd, James E., additional, Humphries, Stephen M., additional, Lynch, David A., additional, Kropski, Jonathan A., additional, and Blackwell, Timothy S., additional

Published
2020
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8. Glucagon-like peptide 1 signaling inhibits allergen-induced lung IL-33 release and reduces group 2 innate lymphoid cell (ILC2) cytokine production in vivo

Author

Toki, Shinji, Goleniewska, Kasia, Reiss, Sara, Zhang, Jian, Bloodworth, Melissa H., Stier, Matthew T., Zhou, Weisong, Newcomb, Dawn C., Ware, Lorraine B., Stanwood, Gregg D., Galli, Aurelio, Boyd, Kelli L., Niswender, Kevin D., and Peebles, R. Stokes

Subjects
Mice, Inbred BALB C, Dermatophagoides pteronyssinus, Alternaria, Mice, Transgenic, Allergens, Interleukin-33, Article, Asthma, Glucagon-Like Peptide-1 Receptor, Immunity, Innate, Mucus, Glucagon-Like Peptide 1, Eosinophilia, Animals, Cytokines, Female, Lymphocytes, Lung, Signal Transduction
Abstract

BACKGROUND: IL-33 is one of the most consistently associated gene candidates for asthma identified by GWAS. Studies in mice and in human cells have confirmed the importance of IL-33 in inducing type-2 cytokine production from both group 2 innate lymphoid cells (ILC2) and Th2 cells. However, there are no pharmacologic agents known to inhibit IL-33 release from airway cells. OBJECTIVE: To determine the effect of glucagon like peptide receptor-1 GLP-1R signaling on aeroallergen-induced airway IL-33 production and release and on innate type-2 airway inflammation. METHODS: BALB/c mice were challenged intranasally with Alternaria extract for 4 consecutive days. GLP-1R agonist or the vehicle was administered starting either 2 days before the first Alternaria extract-challenge or 1 day after the first Alternaria extract-challenge. RESULTS: GLP-1R agonist treatment starting 2 days before the first Alternaria extract-challenge decreased IL-33 release in the BAL fluid and DUOX1 mRNA expression 1 h after the first Alternaria extract-challenge, and IL-33 expression in lung epithelial cells 24 h after the last Alternaria extract-challenge. Further, GLP-1R agonist significantly decreased the number of ILC2 expressing IL-5 and IL-13, the lung protein expression of type-2 cytokines and chemokines, the number of perivascular eosinophils, mucus production, and airway responsiveness compared with vehicle treatment. GLP-1R agonist treatment starting one day after the first Alternaria extract-challenge also significantly decreased eosinophilia and type-2 cytokine and chemokine expression in the airway after 4 days of Alternaria extract-challenge. CONCLUSION: These results reveal that GLP-1R signaling may be a potential therapy to reduce IL-33 release and inhibit the ILC2 response to protease-containing aeroallergens, such as Alternaria.

Published
2018

9. Glucagon-like peptide 1 signaling inhibits allergen-induced lung IL-33 release and reduces group 2 innate lymphoid cell cytokine production in vivo

Author

Toki, Shinji, primary, Goleniewska, Kasia, additional, Reiss, Sara, additional, Zhang, Jian, additional, Bloodworth, Melissa H., additional, Stier, Matthew T., additional, Zhou, Weisong, additional, Newcomb, Dawn C., additional, Ware, Lorraine B., additional, Stanwood, Gregg D., additional, Galli, Aurelio, additional, Boyd, Kelli L., additional, Niswender, Kevin D., additional, and Peebles, R. Stokes, additional

Published
2018
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11. Glucagon-like Peptide 1 Receptor (GLP-1R) Signaling Inhibits Aeroallergen-Induced IL-33 Release and Reduces Group 2 Innate Lymphoid Cell (ILC2) Activation In Vivo

Author

Toki, Shinji, primary, Goleniewska, Kasia, additional, Reiss, Sara, additional, Zhang, Jian, additional, Bloodworth, Melissa H., additional, Stier, Matt T., additional, Zhou, Weisong, additional, Newcomb, Dawn C., additional, Boyd, Kelli L., additional, Niswender, Kevin D., additional, and Peebles, Stokes, additional

Published
2017
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12. Additional file 2: of β2-Adrenergic receptor promoter haplotype influences the severity of acute viral respiratory tract infection during infancy: a prospective cohort study

Author

Pingsheng Wu, Larkin, Emma, Reiss, Sara, Carroll, Kecia, Summar, Marshall, Minton, Patricia, Woodward, Kimberly, Zhouwen Liu, Islam, Jessica, Hartert, Tina, and Moore, Paul

Abstract

BSS distribution stratified by copy number of coding block haplotype GG and separated by race. The scatter plots and the box-and-whisker plots of BSS across 0, 1, and 2 copies of coding block haplotype GG for both Caucasian and African American infants. P values were obtained from multivariable regression model adjusted for infant age at enrollment, gender, daycare exposure, secondhand smoke exposure, any prior history of breastfeeding, any siblings at home, and enrollment season. (PDF 11 kb)

Published
2015
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13. Additional file 6: of β2-Adrenergic receptor promoter haplotype influences the severity of acute viral respiratory tract infection during infancy: a prospective cohort study

Author

Pingsheng Wu, Larkin, Emma, Reiss, Sara, Carroll, Kecia, Summar, Marshall, Minton, Patricia, Woodward, Kimberly, Zhouwen Liu, Islam, Jessica, Hartert, Tina, and Moore, Paul

Abstract

BSS distribution stratified by copy number of combined haplotype TTGGC and separated by race. The scatter plots and the box-and-whisker plots of BSS across 0, 1, and 2 copies of combined haplotype TTGGC for both Caucasian and African American infants. P values were obtained from multivariable regression model adjusted for infant age at enrollment, gender, daycare exposure, secondhand smoke exposure, any prior history of breastfeeding, any siblings at home, and enrollment season. (PDF 11 kb)

Published
2015
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14. Additional file 1: of β2-Adrenergic receptor promoter haplotype influences the severity of acute viral respiratory tract infection during infancy: a prospective cohort study

Author

Pingsheng Wu, Larkin, Emma, Reiss, Sara, Carroll, Kecia, Summar, Marshall, Minton, Patricia, Woodward, Kimberly, Zhouwen Liu, Islam, Jessica, Hartert, Tina, and Moore, Paul

Abstract

BSS distribution by copy number of promoter haplotype TTG and stratified by race. The scatter plots and the box-and-whisker plots of BSS across 0, 1, and 2 copies of promoter haplotype TTG for both Caucasian and African American infants. P values were obtained from multivariable regression model adjusted for infant age at enrollment, gender, daycare exposure, secondhand smoke exposure, any prior history of breastfeeding, any siblings at home, and enrollment season. (PDF 17 kb)

Published
2015
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15. Additional file 5: of β2-Adrenergic receptor promoter haplotype influences the severity of acute viral respiratory tract infection during infancy: a prospective cohort study

Author

Pingsheng Wu, Larkin, Emma, Reiss, Sara, Carroll, Kecia, Summar, Marshall, Minton, Patricia, Woodward, Kimberly, Zhouwen Liu, Islam, Jessica, Hartert, Tina, and Moore, Paul

Abstract

BSS distribution stratified by copy number of combined haplotype TTGAC and separated by race. The scatter plots and the box-and-whisker plots of BSS across 0, 1, and 2 copies of combined haplotype TTGAC for both Caucasian and African American infants. P values were obtained from multivariable regression model adjusted for infant age at enrollment, gender, daycare exposure, secondhand smoke exposure, any prior history of breastfeeding, any siblings at home, and enrollment season. (PDF 11 kb)

Published
2015
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16. Additional file 4: of β2-Adrenergic receptor promoter haplotype influences the severity of acute viral respiratory tract infection during infancy: a prospective cohort study

Author

Pingsheng Wu, Larkin, Emma, Reiss, Sara, Carroll, Kecia, Summar, Marshall, Minton, Patricia, Woodward, Kimberly, Zhouwen Liu, Islam, Jessica, Hartert, Tina, and Moore, Paul

Abstract

BSS distribution stratified by copy number of coding block haplotype GC and separated by race. The scatter plots and the box-and-whisker plots of BSS across 0, 1, and 2 copies of coding block haplotype GC for both Caucasian and African American infants. P values were obtained from multivariable regression model adjusted for infant age at enrollment, gender, daycare exposure, secondhand smoke exposure, any prior history of breastfeeding, any siblings at home, and enrollment season. (PDF 11 kb)

Published
2015
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17. The histone deacetylase inhibitor trichostatin A suppresses murine innate allergic inflammation by blocking group 2 innate lymphoid cell (ILC2) activation

Author

Toki, Shinji, primary, Goleniewska, Kasia, additional, Reiss, Sara, additional, Zhou, Weisong, additional, Newcomb, Dawn C, additional, Bloodworth, Melissa H, additional, Stier, Matthew T, additional, Boyd, Kelli L, additional, Polosukhin, Vasiliy V, additional, Subramaniam, Sriram, additional, and Peebles, R Stokes, additional

Published
2016
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18. The Histone Deacetylase Inhibitor Trichostatin a (TSA) Suppresses Alternaria Extract-Induced Murine Innate Allergic Inflammation By Blocking Group 2 Innate Lymphoid Cell (ILC2) Activation

Author

Toki, Shinji, primary, Goleniewska, Kasia, additional, Reiss, Sara, additional, Zhou, Weisong, additional, Newcomb, Dawn C., additional, Bloodworth, Melissa H., additional, Stier, Matthew T., additional, Boyd, Kelli L., additional, Polosukhin, Vasiliy V., additional, Subramaniam, Sriram, additional, and Peebles, R. Stokes, additional

Published
2016
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19. IL-17A inhibits airway reactivity induced by RSV infection during allergic airway inflammation

Author

Newcomb, Dawn C, Boswell, Madison G, Reiss, Sara, Zhou, Weisong, Goleniewska, Kasia, Toki, Shinji, Harintho, Melissa T, Lukacs, Nicholas W., Kolls, Jay K, and Peebles, R. Stokes

Subjects
Inflammation, Mice, Knockout, Mice, Inbred BALB C, Interleukin-17, Enzyme-Linked Immunosorbent Assay, Respiratory Syncytial Virus Infections, Real-Time Polymerase Chain Reaction, Article, Asthma, Disease Models, Animal, Mice, Animals, Cytokines, Female, RNA, Messenger, Bronchoalveolar Lavage Fluid
Abstract

Viral infections are the most frequent cause of asthma exacerbations and are linked to increased airway reactivity (AR) and inflammation. Mice infected with respiratory syncytial virus (RSV) during ovalbumin (OVA)-induced allergic airway inflammation (OVA/RSV) had increased AR compared with OVA or RSV mice alone. Furthermore, interleukin 17A (IL-17A) was only increased in OVA/RSV mice.To determine whether IL-17A increases AR and inflammation in the OVA/RSV model.Wild-type (WT) BALB/c and IL-17A knockout (KO) mice underwent mock, RSV, OVA or OVA/RSV protocols. Lungs, bronchoalveolar lavage (BAL) fluid and/or mediastinal lymph nodes (MLNs) were harvested after infection. Cytokine expression was determined by ELISA in the lungs or BAL fluid. MLNs were restimulated with either OVA (323-229) peptide or RSV M2 (127-135) peptide and IL-17A protein expression was analysed. AR was determined by methacholine challenge.RSV increased IL-17A protein expression by OVA-specific T cells 6 days after infection. OVA/RSV mice had decreased interferon-β protein expression compared with RSV mice. OVA/RSV mice had increased IL-23p19 mRNA expression in lung homogenates compared with mock, OVA or RSV mice. Unexpectedly, IL-17A KO OVA/RSV mice had increased AR compared with WT OVA/RSV mice. Furthermore, IL-17A KO OVA/RSV mice had increased eosinophils, lymphocytes and IL-13 protein expression in BAL fluid compared with WT OVA/RSV mice.IL-17A negatively regulated AR and airway inflammation in OVA/RSV mice. This finding is important because IL-17A has been identified as a potential therapeutic target in asthma, and inhibiting IL-17A in the setting of virally-induced asthma exacerbations may have adverse consequences.

Published
2013

20. β2-Adrenergic receptor promoter haplotype influences the severity of acute viral respiratory tract infection during infancy: a prospective cohort study

Author

Wu, Pingsheng, primary, Larkin, Emma K, additional, Reiss, Sara S, additional, Carroll, Kecia N, additional, Summar, Marshall L, additional, Minton, Patricia A, additional, Woodward, Kimberly B, additional, Liu, Zhouwen, additional, Islam, Jessica Y, additional, Hartert, Tina V, additional, and Moore, Paul E, additional

Published
2015
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24. Allergic Airway Inflammation Decreases Lung Bacterial Burden following Acute Klebsiella pneumoniae Infection in a Neutrophil- and CCL8-Dependent Manner

Author

Dulek, Daniel E., primary, Newcomb, Dawn C., additional, Goleniewska, Kasia, additional, Cephus, Jaqueline, additional, Zhou, Weisong, additional, Reiss, Sara, additional, Toki, Shinji, additional, Ye, Fei, additional, Zaynagetdinov, Rinat, additional, Sherrill, Taylor P., additional, Blackwell, Timothy S., additional, Moore, Martin L., additional, Boyd, Kelli L., additional, Kolls, Jay K., additional, and Peebles, R. Stokes, additional

Published
2014
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26. Cat neuturing, continued

Author

Reiss, Sara and Sandry, Adele

Subjects
Disease transmission, Cats
Abstract

COUNTRYSIDE: This is in regards to Michelle Milbanks' "No cat neutering on this homestead" (Sept/Oct 2007). I am sorry to hear that she was unable to adopt a cat from […]

Published
2007

31. The histone deacetylase inhibitor trichostatin A suppresses murine innate allergic inflammation by blocking group 2 innate lymphoid cell (ILC2) activation.

Author

Shinji Toki, Goleniewska, Kasia, Reiss, Sara, Weisong Zhou, Newcomb, Dawn C., Bloodworth, Melissa H., Stier, Matthew T., Boyd, Kelli L., Polosukhin, Vasiliy V., Subramaniam, Sriram, Peebles Jr, R. Stokes, Toki, Shinji, Zhou, Weisong, and Peebles, R Stokes Jr

Subjects
INTERLEUKIN-5, HISTONE deacetylase, TRICHOSTATIN A, IMMUNE response, INFLAMMATION, ALLERGENS, ANIMAL experimentation, ASTHMA, BRONCHOALVEOLAR lavage, CYTOKINES, ENZYME inhibitors, FUNGI, IMMUNITY, INTERLEUKINS, LUNGS, LYMPHOCYTES, MICE, RESEARCH funding, HYDROXY acids, PHARMACODYNAMICS
Abstract

Background: Group 2 innate lymphoid cells (ILC2) are an important source of the type 2 cytokines interleukin (IL)-5 and IL-13 that are critical to the allergic airway phenotype. Previous studies reported that histone deacetylase (HDAC) inhibition by trichostatin A (TSA) downregulated adaptive allergic immune responses; however, the effect of HDAC inhibition on the early innate allergic immune response is unknown. Therefore, we investigated the effect of TSA on innate airway inflammation mediated by ILC2 activation.Methods: BALB/c mice were challenged intranasally with Alternaria extract, exogenous recombinant mouse IL-33 (rmIL-33) or the respective vehicles for four consecutive days following TSA or vehicle treatment. Bronchoalveolar lavage (BAL) fluids and lungs were harvested 24 h after the last challenge.Results: We found that TSA treatment significantly decreased the number of ILC2 expressing IL-5 and IL-13 in the lungs challenged with Alternaria extract or rmIL-33 compared with vehicle treatment (p<0.05). TSA treatment significantly decreased protein expression of IL-5, IL-13, CCL11 and CCL24 in the lung homogenates from Alternaria extract-challenged mice or rmIL-33-challenged mice compared with vehicle treatment (p<0.05). Further, TSA treatment significantly decreased the number of perivascular eosinophils and mucus production in the large airways that are critical components of the asthma phenotype (p<0.05). TSA did not change early IL-33 release in the BAL fluids; however, TSA decreased lung IL-33 expression from epithelial cells 24 h after last Alternaria extract challenge compared with vehicle treatment (p<0.05).Conclusions: These results reveal that TSA reduces allergen-induced ILC2 activation and the early innate immune responses to an inhaled protease-containing aeroallergen. [ABSTRACT FROM AUTHOR]

Published
2016
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33. β2-Adrenergic receptor promoter haplotype influences the severity of acute viral respiratory tract infection during infancy: a prospective cohort study.

Author

Pingsheng Wu, Larkin, Emma K., Reiss, Sara S., Carroll, Kecia N., Summar, Marshall L., Minton, Patricia A., Woodward, Kimberly B., Zhouwen Liu, Islam, Jessica Y., Hartert, Tina V., and Moore, Paul E.

Subjects
BETA adrenoceptors, RESPIRATORY infections in children, HAPLOTYPES, MEDICAL genetics, GENETICS
Abstract

Background: Despite the significant interest in β2-Adrenergic receptor (ADRB2) polymorphisms related to asthma, whether ADRB2 genetic variants are similarly associated with acute respiratory tract infections have not been studied. We hypothesized that genetic variants in ADRB2 associated with a response to asthma therapy during an asthma exacerbation were also associated with severity of acute respiratory tract infections. Methods: To test this hypothesis, we genotyped 5 common polymorphisms in the promoter region and coding block of the ADRB2 gene (loci -2387, -2274, -1343, +46, and +79) from 374 Caucasian and African American term infants who were enrolled at the time of acute respiratory illness over four respiratory viral seasons. Severity of respiratory tract infections was measured using a bronchiolitis severity score (BSS; range = 0-12, clinically significant difference = 0.5) with a higher score indicating more severe disease. We assigned the promoter, coding and combined promoter and coding haplotypes to the unphased genotype data. The associations between each of these five single-nucleotide polymorphisms (SNPs) as well as the haplotypes and infant BSS were analyzed using nonparametric univariate analysis and multivariable proportional odds model separately in Caucasians and African Americans. Results: There was no significant association between infant BSS and each of the SNPs in both Caucasians and African Americans. However, promoter haplotype CCA was associated with a decreased BSS in African Americans in a dose dependent manner. The median (interquartile range) BSS of infants with no copies of the CCA haplotype, one copy, and two copies of the CCA haplotype were 5.5 (2.0, 8.0), 4.0 (1.0, 7.5), and 3.0 (1.0, 4.0), respectively. This dose dependent relationship persisted after adjusting for infant age, gender, daycare exposure, secondhand smoke exposure, prior history of breastfeeding, siblings at home, and enrollment season (adjusted odds ratio: 0.59, 95 % confidence interval: 0.36, 0.98). There was no similar protective relationship of haplotype CCA on severity of respiratory tract infections identified in Caucasians. Conclusions: ADRB2 genotype may be predictive of severity of acute respiratory tract infections in African Americans, and potentially identify a subset of infants who may respond to beta-agonist therapy. [ABSTRACT FROM AUTHOR]

Published
2015
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34. Allergic Airway Inflammation Decreases Lung Bacterial Burden following Acute Klebsiella pneumoniaeInfection in a Neutrophil- and CCL8-Dependent Manner

Author

Dulek, Daniel E., Newcomb, Dawn C., Goleniewska, Kasia, Cephus, Jaqueline, Zhou, Weisong, Reiss, Sara, Toki, Shinji, Ye, Fei, Zaynagetdinov, Rinat, Sherrill, Taylor P., Blackwell, Timothy S., Moore, Martin L., Boyd, Kelli L., Kolls, Jay K., and Peebles, R. Stokes

Abstract

ABSTRACTThe Th17 cytokines interleukin-17A (IL-17A), IL-17F, and IL-22 are critical for the lung immune response to a variety of bacterial pathogens, including Klebsiella pneumoniae. Th2 cytokine expression in the airways is a characteristic feature of asthma and allergic airway inflammation. The Th2 cytokines IL-4 and IL-13 diminish ex vivoand in vivoIL-17A protein expression by Th17 cells. To determine the effect of IL-4 and IL-13 on IL-17-dependent lung immune responses to acute bacterial infection, we developed a combined model in which allergic airway inflammation and lung IL-4 and IL-13 expression were induced by ovalbumin sensitization and challenge prior to acute lung infection with K. pneumoniae. We hypothesized that preexisting allergic airway inflammation decreases lung IL-17A expression and airway neutrophil recruitment in response to acute K. pneumoniaeinfection and thereby increases the lung K. pneumoniaeburden. As hypothesized, we found that allergic airway inflammation decreased the number of K. pneumoniae-induced airway neutrophils and lung IL-17A, IL-17F, and IL-22 expression. Despite the marked reduction in postinfection airway neutrophilia and lung expression of Th17 cytokines, allergic airway inflammation significantly decreased the lung K. pneumoniaeburden and postinfection mortality. We showed that the decreased lung K. pneumoniaeburden was independent of IL-4, IL-5, and IL-17A and partially dependent on IL-13 and STAT6. Additionally, we demonstrated that the decreased lung K. pneumoniaeburden associated with allergic airway inflammation was both neutrophil and CCL8 dependent. These findings suggest a novel role for CCL8 in lung antibacterial immunity against K. pneumoniaeand suggest new mechanisms of orchestrating lung antibacterial immunity.

Published
2014
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35. Country conversation & feedback.

Author

Blank, F., Bakehouse, Jon, Strong, Paul, Nevada, Carrie, Garner, Alfred, Reusser, Judy, Mimranek, Jim, Bright, John, Kehm, George, Forsyth, Cynthia, Barbara, Pollard, Fred, Seigreid, Lynn, Lemm, Teri, Goss Jr., ]effery, Mimranek, Judy, Alexa, Tennessee, Alexa, Brand, Barbara, and Reiss, Sara

Subjects
LETTERS to the editor, ANTS, PEONIES, EDIBLE wild plants, DISCOUNT houses (Retail trade)
Abstract

Several letters to the editor are presented in response to articles in previous issues of "Countryside & Small Stock Journal," including an article in the September/October 2007 issue about ants and peonies, "Wild Plants--Winter Food," in the September/October 2007 issue and the stigma attached to dollar stores.

Published
2007

38. STAT4 Deficiency Fails To Induce Lung Th2 or Th17 Immunity following Primary or Secondary Respiratory Syncytial Virus (RSV) Challenge but Enhances the Lung RSV-Specific CD8+ T Cell Immune Response to Secondary Challenge.

Author

Dulek, Daniel E., Newcomb, Dawn C., Shinji Toki, Goliniewska, Kasia, Cephus, Jacqueline, Reiss, Sara, Bates, John T., Crowe Jr., James E., Boyd, Kelli L., Moore, Martin L., Weisong Zhou, and Peebles Jr., R. Stokes

Subjects
*VIRUS diseases, *IMMUNE response, *RESPIRATORY syncytial virus, *CD80 antigen, *T cells, *RESPIRATORY diseases, *INTERFERONS
Abstract

Immune-mediated lung injury is a hallmark of lower respiratory tract illness caused by respiratory syncytial virus (RSV). STAT4 plays a critical role in CD4+ Th1 lineage differentiation and gamma interferon (IFN-γ) protein expression by CD4+ T cells. As CD4+ Th1 differentiation is associated with negative regulation of CD4+ Th2 and Th17 differentiation, we hypothesized that RSV infection of STAT4-/- mice would result in enhanced lung Th2 and Th17 inflammation and impaired lung Th1 inflammation compared to wild-type (WT) mice. We performed primary and secondary RSV challenges in WT and STAT4-/- mice and used STAT4-/- mice as a positive control for the development of RSV-specific lung Th2 and Th17 inflammation during primary challenge. Primary RSV challenge of STAT4-/- mice resulted in decreased T-bet and IFN-γ expression levels in CD4+ T cells compared to those of WT mice. Lung Th2 and Th17 inflammation did not develop in primary RSV-challenged STAT4/ mice. Decreased IFN-γ expression by NK cells, CD4+ T cells, and CD4+ T cells was associated with attenuated weight loss and enhanced viral clearance with primary challenge in STAT4-/- mice compared to WT mice. Following secondary challenge, WT and STAT4-/- mice also did not develop lung Th2 or Th17 inflammation. In contrast to primary challenge, secondary RSV challenge of STAT4-/- mice resulted in enhanced weight loss, an increased lung IFN-γ expression level, and an increased lung RSV-specific CD4+ T cell response compared to those of WT mice. These data demonstrate that STAT4 regulates the RSV-specific CD4+ T cell response to secondary infection but does not independently regulate lung Th2 or Th17 immune responses to RSV challenge. [ABSTRACT FROM AUTHOR]

Published
2014
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39. Endogenous PGI 2 signaling through IP inhibits neutrophilic lung inflammation in LPS-induced acute lung injury mice model.

Author

Toki S, Zhou W, Goleniewska K, Reiss S, Dulek DE, Newcomb DC, Lawson WE, and Peebles RS Jr

Subjects
Acute Lung Injury chemically induced, Acute Lung Injury pathology, Animals, Disease Models, Animal, Epoprostenol genetics, Mice, Mice, Knockout, Neutrophils pathology, Acute Lung Injury metabolism, Epoprostenol metabolism, Lipopolysaccharides toxicity, Neutrophil Infiltration, Neutrophils metabolism, Signal Transduction
Abstract

Endogenous prostaglandin I 2 (PGI 2 ) has inhibitory effects on immune responses against pathogens or allergens; however, the immunomodulatory activity of endogenous PGI 2 signaling in endotoxin-induced inflammation is unknown. To test the hypothesis that endogenous PGI 2 down-regulates endotoxin-induced lung inflammation, C57BL/6 wild type (WT) and PGI 2 receptor (IP) KO mice were challenged intranasally with LPS. Urine 6-keto-PGF , a stable metabolite of PGI 2, was significantly increased following the LPS-challenge, suggesting that endogenous PGI 2 signaling modulates the host response to LPS-challenge. IPKO mice had a significant increase in neutrophils in the BAL fluid as well as increased proteins of KC, LIX, and TNF-α in lung homogenates compared with WT mice. In contrast, IL-10 was decreased in LPS-challenged IPKO mice compared with WT mice. The PGI 2 analog cicaprost significantly decreased LPS-induced KC, and TNF-α, but increased IL-10 and AREG in bone marrow-derived dendritic cells (BMDCs) and bone marrow-derived macrophages (BMMs) compared with vehicle-treatment. These results indicated that endogenous PGI 2 signaling attenuated neutrophilic lung inflammation through the reduced inflammatory cytokine and chemokine and enhanced IL-10., (Published by Elsevier Inc.)

Published
2018
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40. STAT4 deficiency fails to induce lung Th2 or Th17 immunity following primary or secondary respiratory syncytial virus (RSV) challenge but enhances the lung RSV-specific CD8+ T cell immune response to secondary challenge.

Author

Dulek DE, Newcomb DC, Toki S, Goliniewska K, Cephus J, Reiss S, Bates JT, Crowe JE Jr, Boyd KL, Moore ML, Zhou W, and Peebles RS Jr

Subjects
Animals, Disease Models, Animal, Female, Lung pathology, Mice, Inbred BALB C, Mice, Knockout, STAT4 Transcription Factor deficiency, CD8-Positive T-Lymphocytes immunology, Lung immunology, Respiratory Syncytial Virus Infections immunology, Respiratory Syncytial Viruses immunology, STAT4 Transcription Factor immunology, Th17 Cells immunology, Th2 Cells immunology
Abstract

Unlabelled: Immune-mediated lung injury is a hallmark of lower respiratory tract illness caused by respiratory syncytial virus (RSV). STAT4 plays a critical role in CD4+ Th1 lineage differentiation and gamma interferon (IFN-γ) protein expression by CD4+ T cells. As CD4+ Th1 differentiation is associated with negative regulation of CD4+ Th2 and Th17 differentiation, we hypothesized that RSV infection of STAT4-/- mice would result in enhanced lung Th2 and Th17 inflammation and impaired lung Th1 inflammation compared to wild-type (WT) mice. We performed primary and secondary RSV challenges in WT and STAT4-/- mice and used STAT1-/- mice as a positive control for the development of RSV-specific lung Th2 and Th17 inflammation during primary challenge. Primary RSV challenge of STAT4-/- mice resulted in decreased T-bet and IFN-γ expression levels in CD4+ T cells compared to those of WT mice. Lung Th2 and Th17 inflammation did not develop in primary RSV-challenged STAT4-/- mice. Decreased IFN-γ expression by NK cells, CD4+ T cells, and CD8+ T cells was associated with attenuated weight loss and enhanced viral clearance with primary challenge in STAT4-/- mice compared to WT mice. Following secondary challenge, WT and STAT4-/- mice also did not develop lung Th2 or Th17 inflammation. In contrast to primary challenge, secondary RSV challenge of STAT4-/- mice resulted in enhanced weight loss, an increased lung IFN-γ expression level, and an increased lung RSV-specific CD8+ T cell response compared to those of WT mice. These data demonstrate that STAT4 regulates the RSV-specific CD8+ T cell response to secondary infection but does not independently regulate lung Th2 or Th17 immune responses to RSV challenge., Importance: STAT4 is a protein critical for both innate and adaptive immune responses to viral infection. Our results show that STAT4 regulates the immune response to primary and secondary challenge with RSV but does not restrain RSV-induced lung Th2 or Th17 immune responses. These findings suggest that STAT4 expression may influence lung immunity and severity of illness following primary and secondary RSV infections., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published
2014
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