Abstract

The goal of this work is the development of an optical instrument and method for measuring in real time, and with site-specificity, the absolute concentrations of drugs or other compounds in tissue. New computational methods, incorporating Mie theory into a Monte Carlo transport code, for modeling of photon transport in tissue, will for the first time allow determination of the effective path histories of photons over varying distances in tissue. Analysis of the optical spectra will enable the separation of the optical scattering and absorption co-efficients of the tissue, and permit determination of the drug concentrations. Fiber-optic probes will permit such measurements to be conducted directly or through endoscopes. The concentrations and kinetics of drugs at specific tissue locations in the body are generally difficult to determine, given only the administered dosage or blood serum measurements. For chemotherapy, it is the difference between the dose-response curves of normal tissue and tumor tissue that must be exploited during treatment. The ability to rapidly, quantitatively and non-invasively measure the concentration of specific drugs and other compounds, especially chemotherapy agents, at specific organ sites, would provide succinct benefits to the study of pharmacokinetics and to clinical pharmacology in general. There does not currently exits a non-invasive method of measuring drug concentrations in the target tissue, and even invasive methods, such as microdialysis, have limited application. We will demonstrate an instrument and a diagnostic method which invokes elastic scattering spectroscopy for measurements through fiber-optic probes, over a broad range of wavelengths from the near-ultraviolet to the near-infrared. Improved spectrometers will be assembled, and the computational codes will be used to model the photon transport, enabling improved designs of fiber-optic probes. The algorithms to analyze the spectra and deduce drug concentrations will be refined. The instrumentation will be applied to pharmacokinetic studies of selected chemotherapy and photodynamic-therapy agents in laboratory animals. Optical measurements will be compared with standard invasive assay results, generally HPLC, for purposes of calibration.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
7R01CA082104-03
Application #
6362718
Study Section
Diagnostic Imaging Study Section (DMG)
Program Officer
Hagan, Ann A
Project Start
1999-03-15
Project End
2003-02-28
Budget Start
2001-05-18
Budget End
2003-02-28
Support Year
3
Fiscal Year
2001
Total Cost
$395,629
Indirect Cost

  Institution

Name
Boston University
Department
Engineering (All Types)
Type
Schools of Engineering
DUNS #
042250712
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Chen, J; Weiss, W A (2015) Alternative splicing in cancer: implications for biology and therapy. Oncogene 34:1-14
Jahangiri, Arman; Weiss, William A (2013) It takes two to tango: Dual inhibition of PI3K and MAPK in rhabdomyosarcoma. Clin Cancer Res 19:5811-3
Ergin, Aysegul; Wang, Mei; Zhang, Jane Y et al. (2012) The feasibility of real-time in vivo optical detection of blood-brain barrier disruption with indocyanine green. J Neurooncol 106:551-60
Ergin, Aysegul; Wang, Mei; Zhang, Jane et al. (2012) Noninvasive in vivo optical assessment of blood brain barrier permeability and brain tissue drug deposition in rabbits. J Biomed Opt 17:057008
Joshi, Shailendra; Ergin, Aysegul; Wang, Mei et al. (2011) Inconsistent blood brain barrier disruption by intraarterial mannitol in rabbits: implications for chemotherapy. J Neurooncol 104:11-9
Joshi, Shailendra; Reif, Roberto; Wang, Mei et al. (2011) Intra-arterial mitoxantrone delivery in rabbits: an optical pharmacokinetic study. Neurosurgery 69:706-12; discussion 712