Abstract

Little is known about how and why hypoxia arises in tumors, ie. whether hypoxia is a chronic process resulting from diffusion limitations, or occurs more acutely due to transient changes in blood perfusion. A new technique for isolating viable tumor cells as a function of their oxygenation status, recently reported by us, shows a clear role of acute hypoxia in at least one experimental tumor system. We now propose to systematically study several additional transplantable murine tumors using this technique. Intravenous administration of the flurochrome Hoechst 33342 into tumor bearing mice results in a heterogeneous staining pattern within the tumors determined by stain delivery (blood flow), and cell location (cells nearer functional vessels are more intensely stained). These differences in staining persist after tumor disaggregation, thus permitting isolation of differentially stained cell populations by fluorescence activated cell sorting. Cells sorted using these techniques will be analyzed for viability using a soft agar clonogenic assay. By analyzing the radiation response of cell populations exposed to Hoechst 33342 either during or at various times before irradiation, we expect to identify acutely and chronically hypoxic cells. The effects of tumor type, size and site of implantation on the existence and amount of acute hypoxia will be investigated. Independent histological procedures will be used to determine the opening and closing rates of individual blood vessels. Reoxygenation and repair of radiation damage in acutely or chronically hypoxic tumor cells will also be evaluated, as will the effectiveness of treatment modalities such as perfluorocarbons, carbogen breathing, and hyperbaric oxygen designed to elminate hypoxia. These studies will lead to a better understanding of tumor hypoxia and its influence on radiation response, a question of particular importance since treatment modalities designed specifically to overcome chronic hypoxia may not be as effective against acutely hypoxic cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA040459-02
Application #
3180455
Study Section
Radiation Study Section (RAD)
Project Start
1986-05-01
Project End
1989-04-30
Budget Start
1987-05-01
Budget End
1988-04-30
Support Year
2
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
British Columbia Cancer Agency
Department
Type
DUNS #
209137736
City
Vancouver
State
BC
Country
Canada
Zip Code
V5 1L3

  Publications

Trotter, M J; Chaplin, D J; Olive, P L (1991) Effect of angiotensin II on intermittent tumour blood flow and acute hypoxia in the murine SCCVII carcinoma. Eur J Cancer 27:887-93
Minchinton, A I; Chaplin, D J (1991) Spatial characterization of glutathione depletion in the KHT sarcoma using flow cytometry. Int J Radiat Biol 59:1425-33
Chaplin, D J; Horsman, M R; Trotter, M J (1990) Effect of nicotinamide on the microregional heterogeneity of oxygen delivery within a murine tumor. J Natl Cancer Inst 82:672-6
Trotter, M J; Chaplin, D J; Durand, R E et al. (1989) The use of fluorescent probes to identify regions of transient perfusion in murine tumors. Int J Radiat Oncol Biol Phys 16:931-4
Chaplin, D J; Trotter, M J; Durand, R E et al. (1989) Evidence for intermittent radiobiological hypoxia in experimental tumour systems. Biomed Biochim Acta 48:S255-9
Trotter, M J; Chaplin, D J; Olive, P L (1989) Use of a carbocyanine dye as a marker of functional vasculature in murine tumours. Br J Cancer 59:706-9
Trotter, M J; Acker, B D; Chaplin, D J (1989) Histological evidence for nonperfused vasculature in a murine tumor following hydralazine administration. Int J Radiat Oncol Biol Phys 17:785-9
Chaplin, D J (1989) Hydralazine-induced tumor hypoxia: a potential target for cancer chemotherapy. J Natl Cancer Inst 81:618-22
Chaplin, D J (1988) Postirradiation modification of tumor blood flow: a method to increase the effectiveness of chemical radiosensitizers. Radiat Res 115:292-302
Chaplin, D J; Horsman, M R (1988) The effect of artificially induced hyperglycemia on the radiation response of the Lewis lung and EMT6 tumor models. Int J Radiat Biol 54:803-11

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