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1. Context‐specific anti‐inflammatory roles of type III interferon signaling in the lung in nonviral injuries.

Author

Feng, Jingjing, Kim, Jooyoung, Wang, Victoria D., Chang, De, Liu, Hongbo, Bain, William G., Robinson, Keven M., Jie, Zhijun, Kotenko, Sergei V., Dela Cruz, Charles S., and Sharma, Lokesh

Subjects
LUNG injuries, INTERFERONS, PULMONARY fibrosis, KNOCKOUT mice, BLEOMYCIN
Abstract

Type III interferons (λ1, λ2, and λ3) are potent antiviral cytokines in the lung. However, their roles in nonviral lung injuries are less well understood. This study investigates the activation of type III interferon signaling in three distinct models of lung injuries caused by diverse stimuli: the bacterial pathogen Pseudomonas aeruginosa, bacterial endotoxin LPS, and the chemotherapeutic agent bleomycin. Our data show that, despite inducing a potent inflammatory response, Pseudomonas and LPS did not increase IFNλ secretion. In contrast, bleomycin instillation increased secretion of IFNλ in the airways at both early and late time points. Consistent with limited secretion, type III interferon signaling had a minimal role in the host response to both Pseudomonas and LPS, as measured by pathogen burden, inflammatory response, and lung injury. Conversely, a deficiency in type III interferon signaling led to increased inflammatory signaling and elevated acute lung injury in the bleomycin model on day 3. This elevated early injury resulted in impaired recovery in IFNLR1 knockout mice, as evidenced by their recovery from bleomycin‐induced weight loss. Taken together, these data suggest a context‐specific activation of type III interferon signaling, where it plays an anti‐inflammatory role in the lung. [ABSTRACT FROM AUTHOR]

Published
2024
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3. Lung microvascular occlusion by platelet-rich neutrophil-platelet aggregates promotes cigarette smoke–induced severe flu

Author

Kaminski, Tomasz W., primary, Brzoska, Tomasz, additional, Li, Xiuying, additional, Vats, Ravi, additional, Katoch, Omika, additional, Dubey, Rikesh K., additional, Bagale, Kamal, additional, Watkins, Simon C., additional, McVerry, Bryan J., additional, Pradhan-Sundd, Tirthadipa, additional, Zhang, Lianghui, additional, Robinson, Keven M., additional, Nyunoya, Toru, additional, and Sundd, Prithu, additional

Published
2024
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15. IL-33-mediated IL-13 secretion by ST2+ Treg controls inflammation after lung injury

Author

Liu, Quan, primary, Dwyer, Gaelen K., additional, Zhao, Yifei, additional, Li, Huihua, additional, Mathews, Lisa R., additional, Chakka, Anish Bhaswanth, additional, Chandran, Uma R., additional, Demetris, Jake A., additional, Alcorn, John F., additional, Robinson, Keven M., additional, Ortiz, Luis A., additional, Pitt, Bruce, additional, Thomson, Angus W., additional, Fan, Ming-Hui, additional, Billiar, Timothy R., additional, and Turnquist, Heth R., additional

Published
2019
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16. STAT2 Signaling Regulates Macrophage Phenotype During Influenza and Bacterial Super-Infection

Author

Gopal, Radha, primary, Lee, Benjamin, additional, McHugh, Kevin J., additional, Rich, Helen E., additional, Ramanan, Krishnaveni, additional, Mandalapu, Sivanarayana, additional, Clay, Michelle E., additional, Seger, Philip J., additional, Enelow, Richard I., additional, Manni, Michelle L., additional, Robinson, Keven M., additional, Rangel-Moreno, Javier, additional, and Alcorn, John F., additional

Published
2018
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25. Influenza-induced type I interferon enhances susceptibility to gram-negative and gram-positive bacterial pneumonia in mice

Author

Lee, Benjamin, primary, Robinson, Keven M., additional, McHugh, Kevin J., additional, Scheller, Erich V., additional, Mandalapu, Sivanarayana, additional, Chen, Chen, additional, Di, Y. Peter, additional, Clay, Michelle E., additional, Enelow, Richard I., additional, Dubin, Patricia J., additional, and Alcorn, John F., additional

Published
2015
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28. Effect of aerosolized antipseudomonals on Pseudomonas positivity and bronchiolitis obliterans syndrome after lung transplantation.

Author

Moore, Cody A., Pilewski, Joseph M., Venkataramanan, Raman, Robinson, Keven M., Morrell, Matthew R., Wisniewski, Stephen R., Zeevi, Adriana, McDyer, John F., and Ensor, Christopher R.

Subjects
PSEUDOMONAS diseases, LUNG transplantation, HOMOGRAFTS, GRAFT rejection -- Risk factors, PROPORTIONAL hazards models, PREVENTION, PATIENTS
Abstract

Purpose To describe the effects of aerosolized antipseudomonals (AAPs) on Pseudomonas ( PS) culture positivity, bronchiolitis obliterans syndrome ( BOS), and acute cellular rejection ( ACR) in lung transplant recipients ( LTRs). Methods Single-center, retrospective cohort study was performed of adult LTRs treated with either AAP for ≥28 days vs no AAP therapy or AAP therapy <28 days, indexed to a matched median date post lung transplantation ( LT). Primary outcome was freedom from PS positivity by positive bronchoalveolar lavage or bronchial wash at 1 year. Secondary outcomes were freedom from BOS or BOS progression and ACR burden (defined by the novel composite rejection standardized score. Normality was assessed, and univariate and multivariate parametric and non-parametric statistical tests were used to assess baseline characteristics and outcomes, where appropriate. Freedom from events was compared using the Kaplan-Meier method with log-rank conversion and risk was assigned using multivariable Cox proportional hazards ( PH) modeling. Results In total, 293 LTRs (105 with AAP, 188 with no AAP) were included. Median ages in AAP and control cohorts were 51 (30-63) and 62 (54-67) years ( P<.01). Median AAP duration was 198 (interquartile range 94-395) days. Time to median positive PS culture was similar between AAP (median 1.02 [95% confidence interval { CI} 0.74-1.22] years) and control (median 0.96 [95% CI 0.72-1.21] years). Log-rank test for time-to- PS positivity was similar for both groups (log-rank P=.26). Incidence of PS culture positivity at 1 year was similar in APP vs controls (59.0% vs 54.8%, P=.48). In the non-cystic fibrosis ( CF) subgroup, AAP use was protective against PS recurrence on univariate Cox PH model (hazard ratio [ HR] 0.55, 95% CI 0.38-0.83) and on multivariate Cox PH adjusting for age and induction ( HR 0.56, 95% CI 0.38-0.83). Incidence of new-onset BOS or BOS progression in APP vs control at 1 (17.1% vs 14.9%, P=.61) and 3 (38.1% vs 37.8%, P=.96) years was similar. CRSS was similar in APP vs control group at 1 year (0.42 vs 0.33, P=.41). Conclusion AAP use was not associated with less PS positivity, BOS, or ACR in all LTRs. In the non- CF subgroup analysis, treatment with AAPS was associated with protection against recurrent PS. Limitations include retrospective design, heterogeneous AAP therapy among LTRs, and potential convenience sampling of LTRs receiving AAPs for >28 days at our center. Larger assessments and better controlled analyses are required to further define efficacy of AAPs after LT. [ABSTRACT FROM AUTHOR]

Published
2017
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38. Clinical Consequences of Targeting IL-17 and TH17 in Autoimmune and Allergic Disorders.

Author

Robinson, Keven M., Manni, Michelle L., Biswas, Partha S., and Alcorn, John F.

Abstract

The T H17 lineage of T cells and its canonical cytokine IL-17 have been the focus of many recent studies in autoimmune, allergic, and infectious disease. In this review, we will briefly discuss the current knowledge about the role of these cells and IL-17 in a spectrum of disorders. It is clear that IL-17 plays pathogenic roles in certain conditions while the same pathway is critically important to immunity in others. Targeting of T H17 cells or IL-17 therapeutically may impart many benefits, but this approach is not without potentially serious implications regarding host defense. These issues will be discussed herein as we evaluate pharmacological approaches targeting this pathway that are just beginning to be fully tested in human disease. [ABSTRACT FROM AUTHOR]

Published
2013
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39. Role of artificial intelligence in early diagnosis and treatment of infectious diseases.

Author

Srivastava, Vartika, Kumar, Ravinder, Wani, Mohmmad Younus, Robinson, Keven, and Ahmad, Aijaz

Abstract

AbstractInfectious diseases remain a global health challenge, necessitating innovative approaches for their early diagnosis and effective treatment. Artificial Intelligence (AI) has emerged as a transformative force in healthcare, offering promising solutions to address this challenge. This review article provides a comprehensive overview of the pivotal role AI can play in the early diagnosis and treatment of infectious diseases. It explores how AI-driven diagnostic tools, including machine learning algorithms, deep learning, and image recognition systems, enhance the accuracy and efficiency of disease detection and surveillance. Furthermore, it delves into the potential of AI to predict disease outbreaks, optimise treatment strategies, and personalise interventions based on individual patient data and how AI can be used to gear up the drug discovery and development (D3) process.The ethical considerations, challenges, and limitations associated with the integration of AI in infectious disease management are also examined. By harnessing the capabilities of AI, healthcare systems can significantly improve their preparedness, responsiveness, and outcomes in the battle against infectious diseases. [ABSTRACT FROM AUTHOR]

Published
2024
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40. Restoration of Type 17 immune signaling is not sufficient for protection during influenza-associated pulmonary aspergillosis.

Author

Ahmad A, Singh RB, Nickolich K, Pilewski M, Ngeow C, Frempong-Manso K, and Robinson K

Abstract

Influenza-associated pulmonary aspergillosis (IAPA) is a severe complication of influenza infection that occurs in critically ill patients and results in higher mortality compared to influenza infection alone. Interleukin-17 (IL-17) and the Type 17 immune signaling pathway cytokine family are recognized for their pivotal role in fostering protective immunity against various pathogens. In this study, we investigate the role of IL-17 and Type 17 immune signaling components during IAPA. Wild-type mice were challenged with influenza A H1N1 (Flu) and then exposed to Aspergillus fumigatus ATCC42202 resting conidia on day 6 post-influenza infection, followed by the quantification of cytokines and chemokines at 48 hours post-fungal infection. Gene and protein expression levels revealed that IL-17 and Type 17 immune cytokines and antimicrobial peptides are downregulated during IAPA compared to mice singularly infected solely with A. fumigatus . Restoration of Type 17 immunity was not sufficient to provide protection against the increased fungal burden observed during IAPA. These findings contrast those observed during post-influenza bacterial super-infection, in which restoration of Type 17 immune signaling protects against exacerbation seen during super-infection. Our study highlights the need for future studies to understand the immune mechanisms that increase susceptibility to fungal infection., Competing Interests: DECLARATION OF INTEREST The authors have no conflict of interest with any organization or entity with a financial interest in the subject matters or materials discussed in this manuscript.

Published
2024
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41. COVID-19 and the Early-Career Physician-Scientist. Fostering Resilience beyond the Pandemic.

Author

Kliment CR, Barbash IJ, Brenner JS, Chandra D, Courtright K, Gauthier MC, Robinson KM, Scheunemann LP, Shah FA, Christie JD, and Morris A

Abstract

The coronavirus disease (COVID-19) pandemic has created significant stressors for the academic and scientific community, with unique challenges for early-career physician-scientists. The pandemic-related disruptions have significantly affected research productivity, access to mentoring, professional development and networking opportunities, funding, and personal wellness. This is especially true for pulmonary and critical care medicine faculty because of the burden of specialized clinical care responsibilities that the COVID-19 pandemic has demanded. Departmental, institutional, and national leadership should foster open dialogue to identify and mitigate these challenges to promote ongoing career development of early-career physician-scientists. Implementation of thoughtful interventions to address these challenges will provide essential support for junior faculty and help retain a generation of physician-scientists., (Copyright © 2021 by the American Thoracic Society.)

Published
2020
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42. Influenza-induced type I interferon enhances susceptibility to gram-negative and gram-positive bacterial pneumonia in mice.

Author

Lee B, Robinson KM, McHugh KJ, Scheller EV, Mandalapu S, Chen C, Di YP, Clay ME, Enelow RI, Dubin PJ, and Alcorn JF

Subjects
Animals, Antimicrobial Cationic Peptides metabolism, Coinfection immunology, Coinfection microbiology, Coinfection virology, Disease Susceptibility, Escherichia coli immunology, Escherichia coli pathogenicity, Escherichia coli Infections immunology, Escherichia coli Infections virology, Influenza A virus immunology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Orthomyxoviridae Infections immunology, Orthomyxoviridae Infections virology, Pneumonia immunology, Pneumonia virology, Pneumonia, Bacterial immunology, Pneumonia, Bacterial virology, Staphylococcal Infections immunology, Staphylococcal Infections virology, Staphylococcus aureus immunology, Staphylococcus aureus pathogenicity, Escherichia coli Infections microbiology, Influenza A virus pathogenicity, Orthomyxoviridae Infections microbiology, Pneumonia microbiology, Pneumonia, Bacterial microbiology, Receptor, Interferon alpha-beta physiology, Staphylococcal Infections microbiology
Abstract

Suppression of type 17 immunity by type I interferon (IFN) during influenza A infection has been shown to enhance susceptibility to secondary bacterial pneumonia. Although this mechanism has been described in coinfection with gram-positive bacteria, it is unclear whether similar mechanisms may impair lung defense against gram-negative infections. Furthermore, precise delineation of the duration of type I IFN-associated susceptibility to bacterial infection remains underexplored. Therefore, we investigated the effects of preceding influenza A virus infection on subsequent challenge with the gram-negative bacteria Escherichia coli or Pseudomonas aeruginosa and the temporal association between IFN expression with susceptibility to Staphylococcus aureus challenge in a mouse model of influenza and bacterial coinfection. Here we demonstrate that preceding influenza A virus led to increased lung E. coli and P. aeruginosa bacterial burden, which was associated with suppression of type 17 immunity and attenuation of antimicrobial peptide expression. Enhanced susceptibility to S. aureus coinfection ceased at day 14 of influenza infection, when influenza-associated type I IFN levels had returned to baseline levels, further suggesting a key role for type I IFN in coinfection pathogenesis. These findings further implicate type I IFN-associated suppression of type 17 immunity and antimicrobial peptide production as a conserved mechanism for enhanced susceptibility to both gram-positive and gram-negative bacterial coinfection during influenza infection., (Copyright © 2015 the American Physiological Society.)

Published
2015
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