Febrile-Range Hyperthermia Augments Neutrophil Accumulation and Enhances Lung Injury in Experimental Gram-Negative Bacterial Pneumonia

Rice, Penelope A.; Martin, Erica L.; He, Ju; Frank, Mariah; DeTolla, Louis J.; Hester, Lisa; O’Neill, Timothy Michael; Manka, Cheu; Benjamin, Ivor J.; Nagarsekar, Ashish; Singh, Ishwar; Hasday, Jeffrey D.

doi:10.4049/jimmunol.174.6.3676

Cited by 99 publications

(123 citation statements)

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“…A computerassisted analysis of CXC chemokine promoters showed that almost every member of this family of neutrophil chemotaxins contains HSEs within their promoter sequences, suggesting these genes may be a newly recognized class of HSF-1-regulated genes (Nagarsekar et al 2005). In further support of the link between febrile-range temperatures and genes-regulating neutrophil recruitment, we found that exposure to febrile-range hyperthermia (core temperature 39.5°C) increases expression of CXC chemokines, augments neutrophil recruitment, and increases tissue injury in mouse models of lung injury (Hasday et al 2003;Rice et al 2005); however, augmentation of CXC chemokine expression did not occur in HSF-1-null mice ). These data demonstrate how activation of HS pathways at febrile-range temperatures has effects beyond HSP expression that may have important consequences in the febrile host.…”

Section: Discussionsupporting

confidence: 58%

“…We and others have demonstrated that elements of the HS response are activated at febrile-range temperatures and regulate genes involved in inflammation and the innate immune response, including tumor necrosis factor α (Ostberg et al 2000;Singh et al 2002Singh et al , 2000, interleukin (IL)-1β (Cahill et al 1996;Fairchild et al 2000), IL-8, and granulocyte macrophage colony-stimulating factor (Rice et al 2005;Singh et al 2008), as well as HSPs. A computerassisted analysis of CXC chemokine promoters showed that almost every member of this family of neutrophil chemotaxins contains HSEs within their promoter sequences, suggesting these genes may be a newly recognized class of HSF-1-regulated genes (Nagarsekar et al 2005).…”

Section: Discussionmentioning

confidence: 99%

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Hyperthermia in the febrile range induces HSP72 expression proportional to exposure temperature but not to HSF-1 DNA-binding activity in human lung epithelial A549 cells

Tulapurkar

Asiegbu

Singh

et al. 2009

Cell Stress and Chaperones

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Expression of heat shock proteins (HSPs) is classically activated at temperatures above the physiologic range (≥42°C) via activation of the stress-activated transcription factor, heat shock factor-1 (HSF-1). Several studies suggest that less extreme hyperthermia, especially within the febrile range, as occurs during fever and exertional/environmental hyperthemia, can also activate HSF-1 and enhance HSP expression. We compared HSP72 protein and mRNA expression in human A549 lung epithelial cells continuously exposed to 38.5°C, 39.5°C, or 41°C or exposed to a classic heat shock (42°C for 2 h). We found that expression of HSP72 protein and mRNA increased linearly as incubation temperature was increased from 37°C to 41°C, but increased abruptly when the incubation temperature was raised to 42°C. A similar response in luciferase activity was observed using A549 cells stably transfected with an HSF-1-responsive luciferase reporter plasmid. However, activation of intranuclear HSF-1 DNA-binding activity was comparable at 38.5°C, 39.5°C, and 41°C and only modestly greater at 42°C but the mobility of HSF1 protein on a denaturing gel was altered with increasing exposure temperature and was distinctly different at 42°C. These findings indicate that the proportional changes in HSF-1-dependent HSP72 expression at febrile-range temperatures are dependent upon exposure time and temperature but not on the degree of HSF-1 DNA-binding activity. Instead, HSF-1-mediated HSP expression following hyperthermia and heat shock appears to be mediated, in addition to HSF-1 activation, by posttranslational modifications of HSF-1 protein.

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Section: Discussionsupporting

confidence: 58%

Section: Discussionmentioning

confidence: 99%

Hyperthermia in the febrile range induces HSP72 expression proportional to exposure temperature but not to HSF-1 DNA-binding activity in human lung epithelial A549 cells

Tulapurkar

Asiegbu

Singh

et al. 2009

Cell Stress and Chaperones

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“…Neutrophils play an important role in the clearance of virus from the infected lungs. Neutrophils also play an important role in the pathophysiology of influenza as they cause narrowing of terminal bronchi and bronchioli (29), and they are a significant source of tissue injury during the innate immune response (46). Consequently, a fine balance exists between the ability of the host immune system to clear the virus and the damage that this immune response causes to the delicate architecture of the lung.…”

Section: Discussionmentioning

confidence: 99%

Contrasting Effects of Cyclooxygenase-1 (COX-1) and COX-2 Deficiency on the Host Response to Influenza A Viral Infection

Carey¹,

Bradbury²,

Seubert³

et al. 2005

The Journal of Immunology

103

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Influenza is a significant cause of morbidity and mortality worldwide despite extensive research and vaccine availability. The cyclooxygenase (COX) pathway is important in modulating immune responses and is also a major target of nonsteroidal anti-inflammatory drugs (NSAIDs) and the newer COX-2 inhibitors. The purpose of the present study was to examine the effect of deficiency of COX-1 or COX-2 on the host response to influenza. We used an influenza A viral infection model in wild type (WT), COX-1−/−, and COX-2−/− mice. Infection induced less severe illness in COX-2−/− mice in comparison to WT and COX-1−/− mice as evidenced by body weight and body temperature changes. Mortality was significantly reduced in COX-2−/− mice. COX-1−/− mice had enhanced inflammation and earlier appearance of proinflammatory cytokines in the BAL fluid, whereas the inflammatory and cytokine responses were blunted in COX-2−/− mice. However, lung viral titers were markedly elevated in COX-2−/− mice relative to WT and COX-1−/− mice on day 4 of infection. Levels of PGE2 were reduced in COX-1−/− airways whereas cysteinyl leukotrienes were elevated in COX-2−/− airways following infection. Thus, deficiency of COX-1 and COX-2 leads to contrasting effects in the host response to influenza infection, and these differences are associated with altered production of prostaglandins and leukotrienes following infection. COX-1 deficiency is detrimental whereas COX-2 deficiency is beneficial to the host during influenza viral infection.

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“…For LPS instillation, the mice were briefly anesthetized with isoflurane, and 50 g of LPS in 50 l of PBS was administered into the posterior pharynx with the tongue retracted until aspiration was witnessed. Twenty-four hours later, the mice were euthanized by isoflurane inhalation and cervical dislocation, and either lungs were resected and frozen in liquid nitrogen for homogenization in radioimmune precipitation assay buffer or lung lavage was performed with a total of 2 ml of PBS as we have previously described (33,35,36).…”

Section: Methodsmentioning

confidence: 99%

Toll-like Receptor Agonists and Febrile Range Hyperthermia Synergize to Induce Heat Shock Protein 70 Expression and Extracellular Release

Gupta¹,

Cooper²,

Tulapurkar³

et al. 2013

Journal of Biological Chemistry

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Febrile-Range Hyperthermia Augments Neutrophil Accumulation and Enhances Lung Injury in Experimental Gram-Negative Bacterial Pneumonia

Cited by 99 publications

References 50 publications

Hyperthermia in the febrile range induces HSP72 expression proportional to exposure temperature but not to HSF-1 DNA-binding activity in human lung epithelial A549 cells

Hyperthermia in the febrile range induces HSP72 expression proportional to exposure temperature but not to HSF-1 DNA-binding activity in human lung epithelial A549 cells

Contrasting Effects of Cyclooxygenase-1 (COX-1) and COX-2 Deficiency on the Host Response to Influenza A Viral Infection

Toll-like Receptor Agonists and Febrile Range Hyperthermia Synergize to Induce Heat Shock Protein 70 Expression and Extracellular Release

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