Abstract

Hemorrhagic Shock (HS) combined with tissue trauma act together to initiate a cascade of signaling events that culminate in inflammation and end-organ damage and dysfunction. The molecular basis for the activation of inflammatory signaling cascades following injury are poorly understood. It has been the premise of our research that understanding how injury induced inflammation is initiated, amplified and then propagated will lead to resuscitation strategies that will control both the early hyperinflammation and the delayed immunocompromised state that develops in trauma patients. It is our hypothesis that signaling events begin almost immediately after injury, and that multiple overlapping pathways are activated that act in concert to amplify and propagate the systemic inflammatory response. We have accumulated data demonstrating that MAP kinases are activated early following the induction of HS in response to hypoxia and circulating hormones. This is followed by the upregulation of the transcriptional factor early growth response gene-1, (Egr-1), and the expression of the inducible NO synthase (iNOS) also during HS and prior to resuscitation. Furthermore, we have evidence showing that both Egr-1 and iNOS participate in the post-resuscitation inflammatory response. We now propose two aims to determine the regulatory relationships between reactive oxygen species, MAP kinases (JNK and ERK), Egr-1, and iNOS during shock and the functional roles of these pathways in controlling post-resuscitation inflammation.
The aims are as follows:
AIM I : To determine the pathways to MAPK activation and Egr-1 and iNOS upregulation following trauma and shock. Under this aim we will explore the role of reactive oxygen species to the upregulafion of MAP kinases, Egr-1 and iNOS. In addition, we will determine whether there is a dependent sequence in the activation of the three pathways.
AIM II : To determine the mechanistic relationships between MAP kinase activation, and Egr-1 and iNOS upregulation to the post-resuscitation intlammation and organ damage. Experiments under Aim II will take advantage of the regulatory information gained in Aim I to determine the role of MAP kinases, Egr-1 and iNOS in controlling the post-resuscitation inflammatory response. With the completion of our two aims we will have established the molecular relationship between these pathways and their individual as well as synergistic roles controlling post-resuscitation inflammation. Each pathway represents a potential target for the further development of therapeutic strategies designed to attenuate the magnitude of the systemic inflammatory response following injury.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Specialized Center (P50)
Project #
2P50GM053789-08
Application #
6829215
Study Section
Special Emphasis Panel (ZGM1-TB-6 (04))
Project Start
2004-07-01
Project End
2009-06-30
Budget Start
2004-07-01
Budget End
2005-06-30
Support Year
8
Fiscal Year
2004
Total Cost
$222,062
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Type
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Schimunek, Lukas; Namas, Rami A; Yin, Jinling et al. (2018) An Enrichment Strategy Yields Seven Novel Single Nucleotide Polymorphisms Associated With Mortality and Altered Th17 Responses Following Blunt Trauma. Shock 49:259-268
Zettel, Kent; Korff, Sebastian; Zamora, Ruben et al. (2017) Toll-Like Receptor 4 on both Myeloid Cells and Dendritic Cells Is Required for Systemic Inflammation and Organ Damage after Hemorrhagic Shock with Tissue Trauma in Mice. Front Immunol 8:1672
Sun, Qian; Loughran, Patricia; Shapiro, Richard et al. (2017) Redox-dependent regulation of hepatocyte absent in melanoma 2 inflammasome activation in sterile liver injury in mice. Hepatology 65:253-268
Zettel, Kent R; Dyer, Mitchell; Raval, Jay S et al. (2017) Aged Human Stored Red Blood Cell Supernatant Inhibits Macrophage Phagocytosis in an HMGB1 Dependent Manner After Trauma in a Murine Model. Shock 47:217-224
Moore, Frederick A; Moore, Ernest E; Billiar, Timothy R et al. (2017) The role of NIGMS P50 sponsored team science in our understanding of multiple organ failure. J Trauma Acute Care Surg 83:520-531
He, Xingying; Qian, Yongbing; Li, Zhigang et al. (2016) TLR4-Upregulated IL-1? and IL-1RI Promote Alveolar Macrophage Pyroptosis and Lung Inflammation through an Autocrine Mechanism. Sci Rep 6:31663
Abboud, Andrew; Namas, Rami A; Ramadan, Mostafa et al. (2016) Computational Analysis Supports an Early, Type 17 Cell-Associated Divergence of Blunt Trauma Survival and Mortality. Crit Care Med 44:e1074-e1081
Vogel, Sebastian; Rath, Dominik; Borst, Oliver et al. (2016) Platelet-derived high-mobility group box 1 promotes recruitment and suppresses apoptosis of monocytes. Biochem Biophys Res Commun 478:143-148
Kassab, Ghassan S; An, Gary; Sander, Edward A et al. (2016) Augmenting Surgery via Multi-scale Modeling and Translational Systems Biology in the Era of Precision Medicine: A Multidisciplinary Perspective. Ann Biomed Eng 44:2611-25
Abboud, Andrew; Mi, Qi; Puccio, Ava et al. (2016) Inflammation Following Traumatic Brain Injury in Humans: Insights from Data-Driven and Mechanistic Models into Survival and Death. Front Pharmacol 7:342

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