Young-Seon Lee
Postdoctoral Associate
Department of Biomedical Sciences
Cornell University
Ithaca, NY 14853
Email: yl422@cornell.edu
Phone: (607) 253-3075
    Education
    • March 2006 - Current, Postdoctoral training, Biomedical Sciences,  Cornell University, Ithaca, NY
    • May 2006 , Ph.D., Mathematics,  University of Utah, Salt Lake City, UT
    • August 1990, M.S., Mathematics,  Korea University, Seoul, South Korea
    • February 1988, B.Sc., Mathematics,  Korea University, Seoul, South Korea

    CV
    Publication

    Research Area: Ca2+ signaling in cardiac cells

    My current goal in research is to understand the underlying mechanisms by which electrical excitation is coupled with mechanical contraction, EC coupling, via Ca2+ signaling in cardiac cells. Since abnormality in Ca2+ release and cycling has been suggested as the primary cause of cardiac arrhythmia, it is important to study Ca2+ release mechanism in detail. First example is Ca2+ alternans, characterized by a beat-to-beat alternation in the amplitude of the intracellular Ca2+ transient at a constant rate of electrical stimulus. I have explored possible mechanisms of  Ca2+ alternans using mathematical modeling and experimental approach. Second example is Ca2+ wave phenomenon, which is usually found from cells with Ca2+ overload. A typical behavior of Ca2+ wave manifests by wave propagation. I have looked for the roles of Ca2+ wave propagation and mechanisms of its genesis. Lastly, I have studied about kinetic mechanism of ryanodine receptor (RyR) channel complex including RyR, triadin/junctin and calsequestrin (CSQ). RyR is  the primary  Ca2+  release channel  on the surface of SR membrane. Because its co-localised location between the sarcoelmma and the SR, understanding of RyR channel gating is complex. I have focused on the role of CSQ in the regulation of RyR kinetics based on recent experimental evidences.

    Cardiac cell image (Lee 2007)



    1.  Ca2+signaling in cardiac Purkinje cells
     The Purkinje network is believed to contribute importantly to the genesis of ventricular arrhythmias through a variety of mechanisms, including the generation of period-doubling bifurcations (Gilmour et al.,1997). Despite of  its important role in cardiac arrhythmogenesis, not much information is known about EC coupling in Purkinje cells. Therefore I study how electrical stimulation activates Ca2+ release, how Ca2+ wave propagates in Ca2+ overload, and how Ca2+ alternans arises.  


    2.  Ca2+ wave propagation
     Calcium (Ca2+) waves in cardiac cells are usually found under Ca2+ overload conditions and might cause cardiac arrhythmias. Ca2+ waves are initiated at local discrete Ca2+ channels on the sarcoplasmic reticulum and spread to neighboring channels mediated by the regenerative process of Ca2+-induced Ca2+ release. To understand the roles of Ca2+ waves, we simulated one-dimensional reaction-diffusion model of Ca2+-induced Ca2+ release. This model showed that alternating patterns of Ca2+ wave propagation can occur with periodic Ca2+ stimulation under condition of Ca2+ load above a threshold level. The follwoing figure shows an alternating pattern of Ca2+ wave propagation.

    Simulation result of CICR model (Lee and keener)


    3. Mechanism of  alternans Ca2+
     With periodic stimulations cardiac cell shows the corresponding electrical (action potential), chemical (Ca2+ concentration), mechanical (contraction) rhythms. Low-frequency stimulation leads to a uniform patterns of these three rhythms, but high-rate stimulation can induce an alternating shape of each rhythm. This is called cardiac alternans, which was first introduced by Trube in 1872. Since then, cardiac alternans have become an important problem because these phenomena are often observed in heart diseases before these are tranferred to cardiac arrhythmias. Despite its importance of the problem, the underlying mechanism of cardiac alternans is not well understood.To understand the underlying mechanism of alternans, we constructed a mathematical model by an assumption that fractional SR Ca2+ release is a steeply increasing function of SR Ca2+ content, based on the data of Shannon et al 2004. This model shows that a reduced SR Ca2+ release increases the SR content unitl it reaches the threshold level, and then Ca2+ cycling becomes unstable. The following figure illustrates that period-doubling (alternans) becomes chaotic as the slope of the steepness of SR Ca2+ release increases.

    Period-doubling bifurcation of discrete model (Lee and keener)


    4. Regulation of RyR channel
    We developed a kinetic model of RyR which has three binding sites two cytosolic sites for Ca2+ activation and inactivation, and one SR luminal site for CSQ binding. The RyR kinetic model was incorporated into a local CICR model that has both a diadic space and junctional SR (jSR). This model suggests that CSQ plays an inhibitory role of RyR gating at low jSR load through more CSQs binding to RyR. In addition, this local CICR model produces a nonlinear fractional relation of jSR Ca2+ release on jSR load. The following figure describes local CICR model based on the idea of Rice et al 1999.


    Local control CICR model adapted from Rice et al 1999