10329603

pubmed:Citation

5

Prostate cancer is the second leading cause of malignancy-related mortality in males in the United States. As a solid tumor, clinically significant tumor growth and metastasis are dependent on nutrients and oxygen supplied by tumor-associated neovasculature. As such, there is a selective tumorigenic advantage for those neoplasms that can produce angiogenic mediators. We show here that human prostate cancer cell lines can constitutively produce angiogenic CXC chemokines. Tumorigenesis of PC-3 prostate cancer cells was shown to be attributable, in part, to the production of the angiogenic CXC chemokine, interleukin (IL)-8. Neutralizing antisera to IL-8 inhibits PC-3 tumor growth in a human prostate cancer/SCID mouse model. Furthermore, angiogenic activity in PC-3 tumor homogenates was attributable to IL-8. In contrast, the Du145 prostate cancer cell line uses a different angiogenic CXC chemokine, GRO-alpha, to mediate tumorigenicity. Neutralizing antisera to GRO-alpha but not IL-8 reduced tumor growth in vivo and reduced the angiogenic activity in tumor homogenates. Thus, prostate cancer cell lines can use distinct CXC chemokines to mediate their tumorigenicity.

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http://linkedlifedata.com/resource/pubmed/journal/0370502

http://linkedlifedata.com/resource/pubmed/chemical/Chemokines, CXC

May

pubmed-author:AddisonC LCL, pubmed-author:ArenbergD ADA, pubmed-author:BurdickM DMD, pubmed-author:GlassMM, pubmed-author:KunkelS LSL, pubmed-author:MooreB BBB, pubmed-author:MorganTT, pubmed-author:MorrisS BSB, pubmed-author:SitterdingSS, pubmed-author:StosEE, pubmed-author:StrieterR MRM, pubmed-author:WilkeCC, pubmed-author:WuDD

154

Y

2009-11-18

1999

Departments of Internal Medicine and Pathology and the Undergraduate Research Opportunities Program, University of Michigan Medical Center, Ann Arbor, Michigan, USA.