Abstract

The overall objective of the Technical Core is to develop a range of techniques and instruments and to supply these to the clinical trials, pre-clinical and basic research projects. These include PDT treatment light sources and delivery systems, fiber-optic based in vivo dosimetry devices, assays of photosensitizer concentration in ex vivo human and animal tissue samples, tissue sectioning with standard or special (immuno) histological staining, and optical imaging and image analysis tools. Additionally, it will provide its expertise in these various techniques and technologies techniques as required in each project. A special focus is to help drive the translation of lab-based techniques/technologies and procedures via the pre-clinical studies to the clinical trials. The technical core acts as a central resource for all project leaders and personnel on the program grant. The technical core has the following 5 specific aims: 1. to provide analysis of ex vivo tissue samples for absolute photosensitizer quantification, and (semi) quantitative confocal microscopy to determine extent of necrosis, apoptosis and protein expression in PDT-treated tissues, and primarily provides 'routine' services to the Program, with a limited developmental component. 2. To develop and transfer new treatment and dosimetry procedures to human trials and animal models, including dedicated instrumentation for fluorescence-guided resection, in vivo photosensitizer measurements by diffuse reflectance spectroscopy, multitasking probes, and light sources/delivery systems for acute and metronomic intracranial PDT treatments. This is primarily developmental work. 3. To provide inter-site cross calibrations of light sources and dosimetry instruments and maintain all dosimetric and fluorescence guided resection systems provided to projects 1 and 2, and is a central element of quality assurance across the Program. 4. To develop image analysis techniques for confocal fluorescence microscopy and fluorescence guided resection imaging, and is developmental, but with rapid transfer to the other projects. 5. To fully implement, enhance and maintain the Program Web site which serves the communication between all projects, recruiting efforts of the clinical trials, and information to the general public.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA043892-15
Application #
7063443
Study Section
Subcommittee G - Education (NCI)
Project Start
Project End
Budget Start
2005-01-01
Budget End
2005-12-31
Support Year
15
Fiscal Year
2005
Total Cost
$96,569
Indirect Cost

  Institution

Name
Healthone Alliance
Department
Type
DUNS #
098407869
City
Denver
State
CO
Country
United States
Zip Code
80203

  Publications

Wang, Luo-Wei; Huang, Zheng; Lin, Han et al. (2013) Effect of Photofrin-mediated photocytotoxicity on a panel of human pancreatic cancer cells. Photodiagnosis Photodyn Ther 10:244-251
Lei, Tim C; Pendyala, Srinivas; Scherrer, Larry et al. (2013) Optical profiles of cathode ray tube and liquid crystal display monitors: implication in cutaneous phototoxicity in photodynamic therapy. Appl Opt 52:2711-7
Weston, Mark A; Patterson, Michael S (2011) Calculation of singlet oxygen dose using explicit and implicit dose metrics during benzoporphyrin derivative monoacid ring A (BPD-MA)-PDT in vitro and correlation with MLL cell survival. Photochem Photobiol 87:1129-37
Santra, Manoranjan; Zheng, Xuguang; Roberts, Cindi et al. (2010) Single doublecortin gene therapy significantly reduces glioma tumor volume. J Neurosci Res 88:304-14
Singh, Gurmit; Alqawi, Omar; Espiritu, Myrna (2010) Metronomic PDT and cell death pathways. Methods Mol Biol 635:65-78
Zheng, Xuguang; Jiang, Feng; Katakowski, Mark et al. (2009) ADAM17 promotes breast cancer cell malignant phenotype through EGFR-PI3K-AKT activation. Cancer Biol Ther 8:1045-54
Hong, Xin; Jiang, Feng; Kalkanis, Steven N et al. (2009) Intracellular free calcium mediates glioma cell detachment and cytotoxicity after photodynamic therapy. Lasers Med Sci 24:777-86
Santra, Manoranjan; Santra, Sutapa; Roberts, Cindi et al. (2009) Doublecortin induces mitotic microtubule catastrophe and inhibits glioma cell invasion. J Neurochem 108:231-45
Gullo, Francesca; Maffezzoli, Andrea; Dossi, Elena et al. (2009) Short-latency cross- and autocorrelation identify clusters of interacting cortical neurons recorded from multi-electrode array. J Neurosci Methods 181:186-98
Szalad, Alexandra; Katakowski, Mark; Zheng, Xuguang et al. (2009) Transcription factor Sp1 induces ADAM17 and contributes to tumor cell invasiveness under hypoxia. J Exp Clin Cancer Res 28:129

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