Abstract

Photodynamic therapy (PDT) may be improved by enhancing the delivery of photosensitizers (PS) to selected lesions using targeted macromolecular conjugates. Recently it has become accepted that tumor-associated macrophages (TAMs) assist the tumor to grow and spread by several distinct mechanisms (paracrine growth factors, increased angiogenesis, and matrix-degrading enzymes) and they have been proposed to be a valid target for cancer therapy. This revised proposal investigates a new approach to killing TAMs by targeted delivery of modified albumin-chlorin (e6) conjugates that are recognized by the scavenger receptors present on TAMs, together with tumor-confined illumination. We have shown that this approach allows very specific photodestruction of mouse macrophages in vitro and leads to substantial inhibition of tumor growth in vivo in both macrophage and non-macrophage tumors. This proposal will test the hypothesis that the combination of macrophage selectivity and directed illumination will kill TAMs without harming other distant macrophage populations, and hence produce beneficial tumor responses including growth delay, decreased angiogenesis and metastasis, increased survival, and development of tumor immunity. The interaction of the conjugates with macrophages is likely to depend on their cellular activation state and this will be investigated with gene expression arrays and quantitation of scavenger-receptor expression by RT-PCR. J774 cells form highly aggressive and metastatic s.c. tumors in BALB/c mice and the biodistribution and PDT response of these conjugates will be compared to free PS. Immunohistochemistry will allow microvessel density, macrophage content, and proliferative index to be determined in frozen sections from treated tumors. The PDT responses of a pair of s.c. mouse tumors differing in macrophage content and immunogenicity (EMT-6 and RIF- 1) will be determined with quantitative comparison of targeted and non-targeted PDT at roughly equal effective doses. The enhancement of PDT by an adjuvant (OK432) designed to increase the degree of tumor infiltration by TAMs and to increase their activation state will be explored. It is proposed that a PDT response which is inflammatory will encourage the induction of a specific anti-tumor immune response, which will be explored by rechallenging cured animals with the same and unrelated cell lines, and measurement of effector cell functions (cytotoxic T lymphocyte, natural killer cell and macrophage) from spleens and draining lymph nodes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA083882-03
Application #
6706259
Study Section
Radiation Study Section (RAD)
Program Officer
Stone, Helen B
Project Start
2002-04-01
Project End
2006-03-31
Budget Start
2004-04-01
Budget End
2006-03-31
Support Year
3
Fiscal Year
2004
Total Cost
$246,525
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
073130411
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Xia, Yumin; Gupta, Gaurav K; Castano, Ana P et al. (2014) CpG oligodeoxynucleotide as immune adjuvant enhances photodynamic therapy response in murine metastatic breast cancer. J Biophotonics 7:897-905
Mroz, Pawel; Vatansever, Fatma; Muchowicz, Angelika et al. (2013) Photodynamic therapy of murine mastocytoma induces specific immune responses against the cancer/testis antigen P1A. Cancer Res 73:6462-70
Naeser, Margaret A; Saltmarche, Anita; Krengel, Maxine H et al. (2011) Improved cognitive function after transcranial, light-emitting diode treatments in chronic, traumatic brain injury: two case reports. Photomed Laser Surg 29:351-8
Mroz, Pawel; Hashmi, Javad T; Huang, Ying-Ying et al. (2011) Stimulation of anti-tumor immunity by photodynamic therapy. Expert Rev Clin Immunol 7:75-91
Mroz, Pawel; Xia, Yumin; Asanuma, Daisuke et al. (2011) Intraperitoneal photodynamic therapy mediated by a fullerene in a mouse model of abdominal dissemination of colon adenocarcinoma. Nanomedicine 7:965-74
Mroz, Pawel; Szokalska, Angelika; Wu, Mei X et al. (2010) Photodynamic therapy of tumors can lead to development of systemic antigen-specific immune response. PLoS One 5:e15194
Mroz, Pawel; Huang, Ying-Ying; Szokalska, Angelika et al. (2010) Stable synthetic bacteriochlorins overcome the resistance of melanoma to photodynamic therapy. FASEB J 24:3160-70
Mroz, Pawel; Bhaumik, Jayeeta; Dogutan, Dilek K et al. (2009) Imidazole metalloporphyrins as photosensitizers for photodynamic therapy: role of molecular charge, central metal and hydroxyl radical production. Cancer Lett 282:63-76
Huang, Ying-Ying; Chen, Aaron C-H; Carroll, James D et al. (2009) Biphasic dose response in low level light therapy. Dose Response 7:358-83
Castano, Ana P; Mroz, Pawel; Wu, Mei X et al. (2008) Photodynamic therapy plus low-dose cyclophosphamide generates antitumor immunity in a mouse model. Proc Natl Acad Sci U S A 105:5495-500

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