Abstract

It is well known that during and following resuscitation from hemorrhagic shock (HS), the vasculature becomes hyporeactive to vasoconstricting agents, and subtle changes in endothelial cell structure and function occur. Although nitric oxide (NO) clearly contributes to the genesis and maintenance of such vasodysregulation, the molecular and cellular basis of vascular pathology in HS remains unclear. The active or allosteric sites of most known bioregulatory targets for NO (and its secondary reaction products) contain thiols and/or iron. In this project, we suggest that in HS an alternative but critical target for NO is zinc sulfur clusters. After iron, zinc (Zc) is the most abundant intracellular metal. Zn metalloproteins comprise >1% of the entire human genome and are critical components of all classes of enzymes as well as many other proteins (e.g., transcription factors). Although Zn itself is redox, insert, its major intracellular binding partner metallothionein (MT) is readily nitrosylated by NO and thus we hypothesize that MT acts a molecular switch linking sensing of NO with a potential component of its transduction (labile zinc). Preliminary data regarding sensitivity of MT null mutant mice to HS and NO-dependent phenotypic changes in vasomoter regulation of resistance vessels of MT- /- mice underscores this hypothesis. According, the specific aims are to: I. Identify the role of MT in affecting the vascular response to hemorrhagic shock and vasomotor regulation of isolated mesenteric vessels in MT null mutant and transgenic mice. II. Study the physiology of zinc homeostasis in isolated cultured murine endothelial (and vascular smooth muscle) cells including use of a novel GTP-MT construct, FRET, and Zn-sensitive fluorophores. III. Determine the mechanism by which zinc contributes to: a) oxidant induced necrosis; or b) NO-mediated inhibition of LPS-induced apoptosis in cultured murine endothelial cells. IV. Determine the molecular mechanisms by which NO-mediated zinc release affects myogenic reflex in mouse mesenteric artery including calcium sparks and spontaneous transient outward currents.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Specialized Center (P50)
Project #
5P50GM053789-06
Application #
6607074
Study Section
Special Emphasis Panel (ZGM1)
Project Start
2002-07-01
Project End
2003-06-30
Budget Start
Budget End
Support Year
6
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Type
DUNS #
053785812
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
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
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
Yang, Yong; Zhang, Peng; Zhao, Yanfeng et al. (2016) Decreased MicroRNA-26a expression causes cisplatin resistance in human non-small cell lung cancer. Cancer Biol Ther 17:515-25
Yang, Weng-Lang; Sharma, Archna; Wang, Zhimin et al. (2016) Cold-inducible RNA-binding protein causes endothelial dysfunction via activation of Nlrp3 inflammasome. Sci Rep 6:26571
Vodovotz, Yoram (2016) Reverse Engineering the Inflammatory ""Clock"": From Computational Modeling to Rational Resetting. Drug Discov Today Dis Models 22:57-63
Yang, Jie; Zhao, Yanfeng; Zhang, Peng et al. (2016) Hemorrhagic shock primes for lung vascular endothelial cell pyroptosis: role in pulmonary inflammation following LPS. Cell Death Dis 7:e2363
Namas, Rami A; Almahmoud, Khalid; Mi, Qi et al. (2016) Individual-specific principal component analysis of circulating inflammatory mediators predicts early organ dysfunction in trauma patients. J Crit Care 36:146-153

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