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Thomas DeCoursey

TitleProfessor
InstitutionRush University, Rush Medical College
DepartmentPhysiology and Biophysics
Address1750 West Harrison St
Chicago IL 60612
ORCID ORCID Icon0000-0002-4263-180X Additional info
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    Collapse Biography 
    Collapse awards and honors
    1974Valedictorian, McPherson College
    1980 - 1981Honorary Research Fellow, University of Glasgow
    2001Co-organizer of First International Proton Channel Meeting , Villars, Switzerland
    2003Invited talk, Stockholm, Sweden, 126th Nobel Symposium
    2005Keynote speaker, Proton Conduction in Diverse Media, Fitzwilliam College, Cambridge University
    2007Chair, Electrochemical Signaling by Membrane Proteins, SOKENDAI International Symposium/36th SERIKEN Conference, Aichi, Japan
    2016Chair-elect, Protons and Membrane Reactions Gordon Research Conference
    2018 - 2023R35 Outstanding Investigator Award, NIH-GM
    2023Co-organizer of “Proton Reactions: From Basic Science to Biomedical Applications", Biophysical Society Conference at Granlibakken in Tahoe CA

    Collapse Overview 
    Collapse overview
    My ORCID is 0000-0002-4263-180X.
    My Scopus ID is 7005381745.
    My NIH COMMONS name is TDECOURSEY.

    Research Areas:
    The properties and biological functions of ion channels are long-term interests of Tom DeCoursey’s laboratory. A major focus in recent years is the voltage-gated proton channel (Hv1). Modulation of the voltage-dependence of this channel by pHo and pHi ensures that it opens only when the electrochemical gradient for H+ is outward (in most species). In other words, when the proton channel opens, it extrudes acid from cells. In a long collaboration with Dr. Vladimir V. Cherny and others, the behavior of proton channels has been explored in alveolar epithelial cells and in white blood cells (human neutrophils and eosinophils). Immune cells engulf (phagocytose) bacteria and kill parasites by secreting reactive oxygen species (e.g., Chlorox). The enzyme responsible for these heroic actions is NADPH oxidase. This enzyme moves electrons across the cell membrane to form superoxide anion near the invading critters. We measure the electron movement directly as an electrical current. For each electron that leaves, one proton stays in the cell. To prevent massive depolarization as well as acidification, protons exit the cell through proton channels. Without H+ efflux, the killing process would be interrupted prematurely. Fortunately, proton channels are activated, relieving the cell of excess acid, and preventing depolarization. The discovery of proton channels has been a great boon to cells, who until this time had to use other, less efficient means of extruding acid. Identification of proton channel genes in 2006 has transformed the field. More functions are described each year, and structure-function studies are appearing. The channel was shown to be a dimer, with conduction pathway in each protomer. The dimer gates cooperatively - both protomers need to move before either conducts. New genes (over a dozen at last count) are appearing at a high rate. The proton channel resists efforts to crystallize it. The first crystal structure was reported in 2014 by Takeshita et al, is likely closed, and is of a chimera with a Voltage-Sensing Phosphatase. Hv1 triggers the flash in bioluminescent dinoflagellates (Smith et al, 2011), which were recently active in Tasmania!

    My Faculty Profile at Rush University Medical Center:
    https://www.rushu.rush.edu/faculty/thomas-decoursey-phd

    My Laboratory:
    https://www.rushu.rush.edu/research/departmental-research/physiology-and-biophysics-research/laboratory-tom-decoursey-phd

    http://www.phys.rush.edu/TomD/physiotd.html

    My NCBI Bibliography:
    https://www.ncbi.nlm.nih.gov/pubmed/?term=DeCoursey+TE

    My Scopus:
    https://www.scopus.com/authid/detail.uri?authorId=7005381745

    My ORCID:
    http://orcid.org/0000-0002-4263-180X

    Education:
    PhD, University of Cincinnati College of Medicine
    BA, McPherson College, Kansas
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