Abstract

Trauma is the major cause of death and disability in modern armed conflict as well as in almost every terrorist attack. Less well known, trauma is the most common cause of civilian death below age 45. Between birth and age 36, trauma exceeds all other causes of death combined. Many patients survive injury initially only to suffer prolonged critical illness or die later when trauma and shock trigger neutrophil (PMN) inflammation and dysfunction that leads to organ failure or sepsis. Thus PMN-mediated inflammation after shock is a key national defense as well as public health problem. During our last grant support period, we showed that inflammation after trauma reflects aberrant regulation of calcium ion (Ca2+) entry from the environment into PMN. These pathways depend in part on the agonist-initiated emptying of cell Ca2+ stores and are therefore generally termed store-operated calcium entry (SOCE). We further showed that in PMN, SOCE is mediated by cellular synthesis of a lipid second messenger, sphingosine 1-phosphate (S1P) in response to Ca2+ store emptying. Related lipids act similarly, and can stimulate PMN activation whether produced intra- or extra-cellular. We have also demonstrated that PMN SOCE occurs through a complex system of Ca2+ entry channels which are composed of """"""""Transient Receptor Potential"""""""" channel proteins (TRPC). Since SOCE is a key regulator of PMN Ca2+ and is abnormally regulated in PMN after injury, these findings suggested the hypothesis that pharmacologic modulation of both S1P synthesis and SOCE-specific Ca2+ channels might prevent PMN-mediated inflammatory sequellae of shock and trauma. Further work has now shown that inhibition of SOCE by a variety of strategies can act to diminish PMN-mediated inflammation and lung injury in complex animal models mimicking clinically relevant trauma and shock treatment scenarios. The present proposal seeks to extend our prior work from the stage of a clinical promising application of our prior basic molecular biologic observations, to the stage of a well-understood treatment strategy ready for clinical implementation both on the battlefield and in civilian trauma practice. We propose to do this by achieving the four following Specific Aims: 1. Determine how to use SOCE inhibition to prevent organ injury after traumatic shock 2. Determine the side effects and complications of SOCE inhibition after shock. 3. Determine the effects of injury on intracellular S1P/SOCE signaling 4. Determine the mechanisms by which circulating S1P activates PMN after trauma. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM059179-08
Application #
7426385
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Somers, Scott D
Project Start
2000-07-01
Project End
2010-02-28
Budget Start
2008-03-01
Budget End
2009-02-28
Support Year
8
Fiscal Year
2008
Total Cost
$390,887
Indirect Cost

  Institution

Name
Beth Israel Deaconess Medical Center
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Itagaki, Kiyoshi; Adibnia, Yasaman; Sun, Shiqin et al. (2011) Bacterial DNA induces pulmonary damage via TLR-9 through cross-talk with neutrophils. Shock 36:548-52
Hauser, Carl J; Sursal, Tolga; Rodriguez, Edward K et al. (2010) Mitochondrial damage associated molecular patterns from femoral reamings activate neutrophils through formyl peptide receptors and P44/42 MAP kinase. J Orthop Trauma 24:534-8
Itagaki, Kiyoshi; Zhang, Qin; Hauser, Carl J (2010) Sphingosine kinase inhibition alleviates endothelial permeability induced by thrombin and activated neutrophils. Shock 33:381-6
Zhang, Qin; Raoof, Mustafa; Chen, Yu et al. (2010) Circulating mitochondrial DAMPs cause inflammatory responses to injury. Nature 464:104-7
Doucet, Danielle R; Bonitz, R Paul; Feinman, Rena et al. (2010) Estrogenic hormone modulation abrogates changes in red blood cell deformability and neutrophil activation in trauma hemorrhagic shock. J Trauma 68:35-41
Itagaki, Kiyoshi; Menconi, Michael; Antoniu, Bozena et al. (2010) Dexamethasone stimulates store-operated calcium entry and protein degradation in cultured L6 myotubes through a phospholipase A(2)-dependent mechanism. Am J Physiol Cell Physiol 298:C1127-39
Zhang, Qin; Itagaki, Kiyoshi; Hauser, Carl J (2010) Mitochondrial DNA is released by shock and activates neutrophils via p38 map kinase. Shock 34:55-9
Lee, Cindy; Xu, Da-Zhong; Feketeova, Eleonora et al. (2008) Calcium entry inhibition during resuscitation from shock attenuates inflammatory lung injury. Shock 30:29-35
Itagaki, Kiyoshi; Yun, Jong K; Hengst, Jeremy A et al. (2007) Sphingosine 1-phosphate has dual functions in the regulation of endothelial cell permeability and Ca2+ metabolism. J Pharmacol Exp Ther 323:186-91
Kannan, Kolenkode B; Barlos, Dimitrios; Hauser, Carl J (2007) Free cholesterol alters lipid raft structure and function regulating neutrophil Ca2+ entry and respiratory burst: correlations with calcium channel raft trafficking. J Immunol 178:5253-61

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