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You have engineered a drug to combat cardiovascular disease by activating a key target protein inside cells within atherosclerotic plaque. The drug, which is absent
You have engineered a drug to combat cardiovascular disease by activating a key target
protein inside cells within atherosclerotic plaque. The drug, which is absent from the body
initially, is consistently supplied to the bloodstream at Rnmo The drug leaves the
bloodstream through the kidneys; this process is quantitatively described with first order rate
constant It also passively enters the cells of interest. The rate of this process is proportional to
the concentration of drug in the bloodstream. There is no mechanism for the drug to leave the
cell to reenter the bloodstream. Instead, the drug can reversibly bind the target in a monovalent
manner. The number of targets per cells is denoted and can be assumed to be in significant
excess relative to the delivered drug. The drug can also be degraded via a firstorder process
with the rate constant Denote the bloodstream volume by and intracellular volume of all
targeted cells by
a Derive an expression for the dynamic concentration of drug in the bloodstream.
b What is the steadystate concentration of the drug in the bloodstream?
c What is the steadystate fraction of target proteins that are complexed?
d Derive an expression for the dynamic concentration of drugreceptor complex in the cells in
the atherosclerotic plaque. You can approximate that binding and unbinding are rapidly
equilibrate relative to pharmacokinetic transport.
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