Genome-wide expression analysis of therapy-resistant tumors reveals SPARC as a novel target for cancer therapy
Isabella T. Tai, … , David A. Owen, Lan Bo Chen
Isabella T. Tai, … , David A. Owen, Lan Bo Chen
Published June 1, 2005
Citation Information: J Clin Invest. 2005;115(6):1492-1502. https://doi.org/10.1172/JCI23002.
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Categories: Research Article Oncology

Genome-wide expression analysis of therapy-resistant tumors reveals SPARC as a novel target for cancer therapy

Abstract

Overcoming resistance to chemotherapy and radiation therapy has been a difficult but important goal in the effort to cure cancer. We used gene-expression microarrays to identify differentially expressed genes involved in colorectal cancer resistance to chemotherapy and identified secreted protein, acidic and rich in cysteine (osteonectin) (SPARC) as a putative resistance-reversal gene by demonstrating low SPARC expression in refractory human MIP101 colon cancer cells. We were able to achieve restoration of their radiosensitivity and sensitivity to 5-fluorouracil and irinotecan by reexpression of SPARC in tumor xenografts. Moreover, treatment of mice with SPARC conferred increased sensitivity to chemotherapy and led to significant regression of xenografted tumors. The results show that modulation of SPARC expression affects colorectal cancer sensitivity to radiation and chemotherapy. SPARC-based gene or protein therapy may ameliorate the emergence of resistant clones and eradicate existing refractory clones and offers a novel approach to treating cancer.

Authors

Isabella T. Tai, Meiru Dai, David A. Owen, Lan Bo Chen

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Effect of chemotherapy and radiation therapy on tumor xenografts of MIP/...
Effect of chemotherapy and radiation therapy on tumor xenografts of MIP/SP cells. (A) Tumor regression in MIP/SP tumor xenografts exposed to 5-FU or CPT-11 compared with MIP/Zeo cells. To allow better visualization of the results provided in A, data from control animals only (tumors of MIP/Zeo and nontreated MIP/SP xenografts) are shown in B, while data from all MIP/SP xenografts treated with 5-FU or CPT-11 are represented in C. (D) Representative MIP/Zeo or MIP/SP tumor xenografts following treatment with 2 cycles of 5-FU or CPT-11. (E) Effect of radiation therapy on MIP/SP tumor xenografts (n = 10 animals/group; total dose of radiation, 100 Gy, single dose; P = 0.02 after 3 weeks of radiation; standard 2-sample t test). (F) SPARC levels in serum obtained from animals with xenografts of MIP/SP an MIP/Zeo 42 days after implantation.