Abstract

Measurement of tumor blood flow and metabolism by non-invasive methods, such as PET , is key to following the effect of antiangiogenic treatment in tumors. Preliminary results obtained by PET in our phase I study of antiangiogenic treatment with Endostatin, have yielded two critical pieces of information. The first is that at low doses of Endostatin (<60 mg/meter squared), both blood flow and glucose metabolism are increased as a function of time. At higher doses (>120 mg/meter squared), there is a clear reduction of blood flow to le tumors but an increase in glucose metabolism. These results suggest that blood flow decrease may precede metabolism decrease in antiangiogenic treatment of tumors and that tumor blood flow and glucose metabolism become uncoupled under moderately ischemic conditions. The second is that tumors can change in size, shape, and distribution, very rapidly. The imaged lesions are heterogeneous in blood flow and metabolism and therefore an accurate measure of these crucial parameters will require the development of new and automated methods of data analysis that are more sensitive and reproducible. Based on these issues, our Specific Aims in this Developmental Project are: (1) To define the parameters that will provide insight into the sequential changes occurring in blood flow and metabolism in tumors following therapy with antiangiogenic agents. (2) To develop methods and software tools to automatically extract this information from serial PET images of human tumors with emphasis on reproducibility and accuracy. (3) To validate these methods using data from a phase I trial of Endostatin; with subsequent application to other early clinical trials of putative antiangiogenic therapies such as PKI166 (Core D) and SU6668 (Developmental Project 4) The short-term significance of this Developmental Project is that these new and automated methods will shorten the time required for early clinical testing of new antiangiogenic agents. The long-term significance of this project is that these tools may eventually be used in patients to accurately predict antiangiogenic effects on tumors thereby optimizing anticancer effects.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
5U54CA090810-02
Application #
6563969
Study Section
Special Emphasis Panel (ZCA1)
Project Start
2002-01-01
Project End
2002-12-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
2
Fiscal Year
2002
Total Cost
$296,752
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Type
DUNS #
001910777
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Wang, Ruoning; Jung, Sung Yun; Wu, Chuan Fen et al. (2010) Direct roles of the signaling kinase RSK2 in Cdc25C activation during Xenopus oocyte maturation. Proc Natl Acad Sci U S A 107:19885-90
Kopetz, Scott; Hoff, Paulo M; Morris, Jeffrey S et al. (2010) Phase II trial of infusional fluorouracil, irinotecan, and bevacizumab for metastatic colorectal cancer: efficacy and circulating angiogenic biomarkers associated with therapeutic resistance. J Clin Oncol 28:453-9
Connelly, Sarah F; Isley, Beth A; Baker, Cheryl H et al. (2010) Loss of tyrosine phosphatase-dependent inhibition promotes activation of tyrosine kinase c-Src in detached pancreatic cells. Mol Carcinog 49:1007-21
Trepel, Martin; Stoneham, Charlotte A; Eleftherohorinou, Hariklia et al. (2009) A heterotypic bystander effect for tumor cell killing after adeno-associated virus/phage-mediated, vascular-targeted suicide gene transfer. Mol Cancer Ther 8:2383-91
Ng, Chaan S; Kodama, Yoshihisa; Mullani, Nizar A et al. (2009) Tumor blood flow measured by perfusion computed tomography and 15O-labeled water positron emission tomography: a comparison study. J Comput Assist Tomogr 33:460-5
Wang, Wei; Shao, Ruping; Wu, Qingping et al. (2009) Targeting gelatinases with a near-infrared fluorescent cyclic His-Try-Gly-Phe peptide. Mol Imaging Biol 11:424-33
Kim, M P; Park, S I; Kopetz, S et al. (2009) Src family kinases as mediators of endothelial permeability: effects on inflammation and metastasis. Cell Tissue Res 335:249-59
Kopetz, Scott; Lesslie, Donald P; Dallas, Nikolas A et al. (2009) Synergistic activity of the SRC family kinase inhibitor dasatinib and oxaliplatin in colon carcinoma cells is mediated by oxidative stress. Cancer Res 69:3842-9
Nie, Jing; Chang, Benny; Traktuev, Dmitry O et al. (2008) IFATS collection: Combinatorial peptides identify alpha5beta1 integrin as a receptor for the matricellular protein SPARC on adipose stromal cells. Stem Cells 26:2735-45
Urbanczyk-Pearson, Lauren M; Femia, Frank J; Smith, Jeffrey et al. (2008) Mechanistic investigation of beta-galactosidase-activated MR contrast agents. Inorg Chem 47:56-68

Showing the most recent 10 out of 84 publications