Abstract

) One emphasis of this program project is to understand the structural determinants which make phthalocyanine (Pc) Pc 4 and a few other PCs as effective photosensitizers (PS) for PDT. To achieve this goal, this program continues to have an emphasis on developing new Pc compounds. It is hoped that some of these may have better antitumor properties for PDT. The purpose of the Photosensitizer Evaluation Core is to establish basic in vitro and in vivo data on the PCs synthesized in Project 1. For this purpose, the core provides information generated in standardized analyses. Each newly synthesized Pc is assessed in parallel with Pc 4, and the photodynamic efficacy of the compound is rated in the standardized test system as 'inferior,' 'equal,' or 'superior' Pc 4. The results are then communicated to the program investigators. The choice for ranking of newly synthesized compounds in relation to Pc 4 is made because a) this was the lead compound among the first 6 synthesized, b) other projects have considerable experience and data with this compound, and c) preclinical pharmacokinetics, efficacy and toxicology of Pc 4 have been completed by the Drug Decision Network of the National Cancer Institute and it has been recommended for clinical testing. This core also generates more detailed infomation on selected promising PS. For this, the decision is made by this core and the investigators of Projects 1-5. To ensure uniformity of the treatment and in consideration of cost effectiveness, this core, in collaboration with Project 2, and 5, will also conduct in vivo evaluation of the Pc 4 (and other PCs) PDT response. The six functions of the core outlined in the ongoing work are retained and they have been fine tuned. In addition, two additional functions are added. The functions of the core are: 1. To determine the partioning of newly synthesized PS between n-octonal vs. saline. 2. To conduct initial in vitro evaluation of PS 3. To define initial PDT responses of PS. 4. To determine distribution of PS in plasma, tumor and other tissues in vivo. 5. To determine systemic toxicity and cutaneous photosensitivity responses of PS. 6. To study detailed PDT effects of selected PS. 7. To determine the efficacy of selected PS in human tumor xenografts in nude mice. 8. To participate in studies assessing in vivo effects of Pc 4 (and other Pcs) in Projects 2, and 5.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
2P01CA048735-09
Application #
6102519
Study Section
Project Start
1999-07-15
Project End
2000-04-30
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
9
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Type
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Yang, Yang; Kennedy, Vance O; Updegraph 3rd, James B et al. (2012) Long directional interactions (LDIs) in oligomeric cofacial silicon phthalocyanines and other oligomeric and polymeric cofacial phthalocyanines. J Phys Chem A 116:8718-30
Yang, Yang; Samas, Brian; Kennedy, Vance O et al. (2011) Long, directional interactions in cofacial silicon phthalocyanine oligomers. J Phys Chem A 115:12474-85
Lee, Richard G; Vecchiotti, Mark A; Heaphy, John et al. (2010) Photodynamic therapy of cottontail rabbit papillomavirus-induced papillomas in a severe combined immunodeficient mouse xenograft system. Laryngoscope 120:618-24
Chiu, Song-Mao; Xue, Liang-Yan; Lam, Minh et al. (2010) A requirement for bid for induction of apoptosis by photodynamic therapy with a lysosome- but not a mitochondrion-targeted photosensitizer. Photochem Photobiol 86:1161-73
Baron, Elma D; Malbasa, Christi L; Santo-Domingo, Diana et al. (2010) Silicon phthalocyanine (Pc 4) photodynamic therapy is a safe modality for cutaneous neoplasms: results of a phase 1 clinical trial. Lasers Surg Med 42:728-35
Rodriguez, Myriam E; Zhang, Ping; Azizuddin, Kashif et al. (2009) Structural factors and mechanisms underlying the improved photodynamic cell killing with silicon phthalocyanine photosensitizers directed to lysosomes versus mitochondria. Photochem Photobiol 85:1189-200
Ke, Malcolm S; Xue, Liang-yan; Feyes, Denise K et al. (2008) Apoptosis mechanisms related to the increased sensitivity of Jurkat T-cells vs A431 epidermoid cells to photodynamic therapy with the phthalocyanine Pc 4. Photochem Photobiol 84:407-14
Soldatova, Alexandra V; Kim, Junhwan; Rosa, Angela et al. (2008) Photophysical behavior of open-shell first-row transition-metal octabutoxynaphthalocyanines: CoNc(OBu)8 and CuNc(OBu)8 as case studies. Inorg Chem 47:4275-89
Kim, Junhwan; Rodriguez, Myriam E; Guo, Ming et al. (2008) Oxidative modification of cytochrome c by singlet oxygen. Free Radic Biol Med 44:1700-11
Wang, Ken Kang-Hsin; Wilson, Jeremy D; Kenney, Malcolm E et al. (2007) Irradiation-induced enhancement of Pc 4 fluorescence and changes in light scattering are potential dosimeters for Pc 4-PDT. Photochem Photobiol 83:1056-62

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