Abstract

Adverse drug reactions (ADRs) are one of the leading causes of hospitalization and death in the United States. ADRs are often associated with unfavorable drug bioavailability or biodistribution profiles. Thus, ADRs could be prevented by optimizing drug transport properties -from the systemic, organ level down to the microscopic, cellular level. To improve the quality of drugs entering clinical trials, a new generation of microscopic imaging instruments -known as """"""""high content screening"""""""" or """"""""HCS"""""""" systems has been developed. HCS instruments can provide preclinical, human cell-based data to complement animal studies in predictive toxicology testing. As a high-throughput platform, HCS systems can be used to screen large collections of small molecules in physiologically-relevant assays. Now the challenge is to incorporate HCS technology into standard biomedical research practice, to facilitate discovery of less toxic drug candidates with improved clinical success rates. To meet this challenge, we propose to develop a cheminformatic and image data management and analysis plan to study the subcellular localization of fluorescent, small molecules -in living cells. Inspired by machine vision approaches currently being used as a tool to analyze the subcellular distribution of proteins on a genome-wide scale (""""""""location proteomics""""""""), we propose that machine vision could also be adopted as a tool to analyze the distribution of small molecule fluorescent drug candidates. In analogy to how protein location is encoded by signal peptides, we hypothesize that subcellular small molecule localization is encoded by """"""""Chemical Address Tags"""""""" to be discovered within the chemical structure of small molecules. To test this hypothesis, we plan to: 1) Develop automated, image analysis and cheminformatic tools to reverse- engineer Chemical Address Tags in an objective, quantitative and high-throughput manner; 2) Develop and compare two quantitative, machine vision approaches to assay the transport properties of mitochondria- targeting molecules; 3) Demonstrate how a cheminformatics-driven, image data management and analysis plan can impact an anticancer drug lead optimization effort. ? ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM078200-01
Application #
7132037
Study Section
Biodata Management and Analysis Study Section (BDMA)
Program Officer
Okita, Richard T
Project Start
2006-07-01
Project End
2011-06-30
Budget Start
2006-07-01
Budget End
2007-06-30
Support Year
1
Fiscal Year
2006
Total Cost
$218,511
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Rzeczycki, Phillip; Yoon, Gi Sang; Keswani, Rahul K et al. (2018) An Expandable Mechanopharmaceutical Device (2): Drug Induced Granulomas Maximize the Cargo Sequestering Capacity of Macrophages in the Liver. Pharm Res 36:3
Murashov, Mikhail D; Diaz-Espinosa, Jennifer; LaLone, Vernon et al. (2018) Synthesis and Characterization of a Biomimetic Formulation of Clofazimine Hydrochloride Microcrystals for Parenteral Administration. Pharmaceutics 10:
Rzeczycki, Phillip; Woldemichael, Tehetina; Willmer, Andrew et al. (2018) An Expandable Mechanopharmaceutical Device (1): Measuring the Cargo Capacity of Macrophages in a Living Organism. Pharm Res 36:12
Woldemichael, Tehetina; Keswani, Rahul K; Rzeczycki, Phillip M et al. (2018) Reverse Engineering the Intracellular Self-Assembly of a Functional Mechanopharmaceutical Device. Sci Rep 8:2934
LaLone, Vernon; Mourão, Márcio A; Standiford, Theodore J et al. (2018) An Expandable Mechanopharmaceutical Device (3): a Versatile Raman Spectral Cytometry Approach to Study the Drug Cargo Capacity of Individual Macrophages. Pharm Res 36:2
Murashov, Mikhail D; LaLone, Vernon; Rzeczycki, Phillip M et al. (2018) The Physicochemical Basis of Clofazimine-Induced Skin Pigmentation. J Invest Dermatol 138:697-703
Rzeczycki, Phillip; Yoon, Gi Sang; Keswani, Rahul K et al. (2017) Detecting ordered small molecule drug aggregates in live macrophages: a multi-parameter microscope image data acquisition and analysis strategy. Biomed Opt Express 8:860-872
Horstman, Elizabeth M; Keswani, Rahul K; Frey, Benjamin A et al. (2017) Elasticity in Macrophage-Synthesized Biocrystals. Angew Chem Int Ed Engl 56:1815-1819
Trexel, Julie; Yoon, Gi S; Keswani, Rahul K et al. (2017) Macrophage-Mediated Clofazimine Sequestration Is Accompanied by a Shift in Host Energy Metabolism. J Pharm Sci 106:1162-1174
Woldemichael, Tehetina; Rosania, Gus R (2017) The physiological determinants of drug-induced lysosomal stress resistance. PLoS One 12:e0187627

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