【 摘 要 】

Even though most of the FDA approved drugs currently out in the market and in the process of development are weakly basic drugs, the bioaccumulation and stabilization of these drugs are not well understood. For this purpose, we use a model drug, clofazimine (CFZ), which is an FDA-approved, weakly basic, and poorly soluble drug that has been used worldwide to treat patients with leprosy and tuberculosis diseases, curing over 16 million people in the last twenty years, to investigate its bioaccumulation and stabilization properties. During prolonged oral administration, CFZ accumulates in macrophages of humans and mice as Crystal Like Drug Inclusions (CLDIs), which have been chemically characterized to be composed of hydrochloride salts of CFZ (CFZ-H+Cl-) crystals. However, the mechanism by which the formation and stabilization of these insoluble complexes occur in cells is not known. Thus, to address this gap, we test the following hypothesis in this dissertation: due to the sufficient proton and chloride levels in endolysosomes, we hypothesize that the phase-transition-dependent drug accumulation and stabilization processes are occurring inside intracellular compartments of likely endolysosomal origin, in macrophages of humans as well as mice. To test our hypothesis, we adapt a systems-based mathematical lysosomal ion regulation model, which consists of lysosomal membrane proteins, such as the proton-pump known as Vacuolar ATPase (V-ATPase), Cl-/H+ antiporter known as CLC7, and membrane proton leak, in order to investigate the key lysosomal parameters that play essential role in the physiological, dose-dependent CFZ-H+Cl- crystal bioaccumulation. Furthermore, we examine the stabilizationof the free base (CFZ) versus salt form (CFZ-H+Cl-) of the drug by mathematically fitting an in vitro pH-dependent solubility data of CFZ-H+Cl- crystal obtained at pH ranging between extracellular, cellular, and subcellular pH values, and determining the drug’s solubility properties, which include the apparent pKa, intrinsic free base and salt solubility, pHmax, and Ksp values. Moreover, we model the cellular and subcellular drug transportation and calculate i) the non-membrane and membrane drug accumulation by accounting for the cell-type dependent heterogeneous and asymmetric lipid bilayer of the biological membranes ii) the degree of supersaturation, which is a measure of thermodynamic propensity of precipitation, of both free base CFZ and CFZ-H+Cl- salt using the aforementioned solubility properties. Collectively, our computational results as well as the CFZ-H+Cl- physicochemical properties in relation to the ion contents and pH of the microenvironment suggest that the physiological and preferential phase-transition-dependent accumulation and stabilization mechanisms of CFZ-H+Cl- crystals in macrophages, more specifically in macrophage lysosomes, are primarily determined by the lysosomal V-ATPase. Moreover, we have shown that the alteration of lysosomal physiology due to lysosomal morphological changes induced upon the accumulation of intrinsic and extrinsic materials, such as cholesterol and biocrystal drugs, respectively can be reversed upon V-ATPase upregulation or inhibition of membrane proton permeability. In addition, in terms of characterizing the stabilization of free base CFZ and CFZ-H+Cl- salt, we have found the degree of supersaturation of CFZ-H+Cl- salt to be at least 1000-fold greater than that of free base CFZ in all of the cellular compartments, including the biological membranes; emphasizing the propensity of the formation and stabilization of massive CFZ-H+Cl- salt precipitate in the lysosomal environment even when introducing low (picomolar) total extracellular drug concentration.

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Exploring Drug Bioaccumulation and Stabilization with Respect to Endolysosomal Ion Homeostasis Using a Systems-Based Mathematical Modeling Approach	6860KB	PDF	download