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Effect of Thrombin Treatment of Tumor Cells on Adhesion of Tumor Cells to Platelets in Vitro and Tumor Metastasis in Vivo

Mary Lynn R. Nierodzik, Francis Kajumo and Simon Karpatkin
Mary Lynn R. Nierodzik
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Francis Kajumo
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Simon Karpatkin
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DOI:  Published June 1992
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Abstract

Seven different tumor cell lines (human melanoma SK MEL 28; hamster melanoma HM29; murine melanomas B16F10 and amelanotic melanoma B16a; human colon carcinoma HCT8; murine colon carcinoma CT26; and murine Lewis lung carcinoma) were treated with thrombin at 0.5–1 unit/ml and examined for their ability to bind to adherent platelets; HM29 was studied for its ability to bind to fibronectin and von Willebrand factor; CT26, B16F1, B16F10, and B16a were studied for their ability to form pulmonary metastasis after i.v. injection of thrombin-treated tumor cells; CT26 was studied for its ability to grow s.c. Five of 7 thrombin-treated tumor cell lines increased their adhesion to adherent platelets 2- to 3-fold. HM29 increased its adherence to fibronectin and von Willebrand factor 2- to 3-fold. CT26, B16F1, B16F10, and B16a increased experimental pulmonary metastasis 10- to 156-fold. Thrombin-treated CT26 cells demonstrated 2-fold greater growth in vivo after s.c. injection. The mechanism of enhanced adhesion of thrombin-treated tumor cells to platelets required the platelet integrin GPIIb-GPIIIa since it could be inhibited by agents known to block adhesion of ligands to GPIIb-GPIIIa (monoclonal antibody 10E5, tetrapeptide RGDS, disintegrin Albolabrin); as well as a “GPIIb-GPIIIa-like” structure on tumor cells since it could be inhibited by treatment of thrombin-treated tumor cells with 10E5 and RGDS. The thrombin effect on tumor cells was optimum at 1 h of incubation with thrombin, did not require active thrombin on the tumor cell surface, and did not require protein synthesis (not inhibited by cycloheximide). Thus, thrombin-treated tumor cells markedly enhance pulmonary metastasis. It is suggested that this may be secondary to thrombin-induced enhanced adhesion as well as growth of tumor cells.

Footnotes

  • ↵1 Supported by Grant HL-13336-21 of the National Lung and Blood Institute, Grant CH-59789 of the American Cancer Society, and a Department of Veterans Affairs Research Advisory Group Grant. Presented at the Thirty-second Annual Meeting of the American Society of Hematology, Boston, MA, December 1, 1990.

  • ↵2 To whom requests for reprints should be addressed.

  • Received July 11, 1991.
  • Accepted April 6, 1992.
  • ©1992 American Association for Cancer Research.
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June 1992
Volume 52, Issue 12
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Effect of Thrombin Treatment of Tumor Cells on Adhesion of Tumor Cells to Platelets in Vitro and Tumor Metastasis in Vivo
Mary Lynn R. Nierodzik, Francis Kajumo and Simon Karpatkin
Cancer Res June 15 1992 (52) (12) 3267-3272;

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Effect of Thrombin Treatment of Tumor Cells on Adhesion of Tumor Cells to Platelets in Vitro and Tumor Metastasis in Vivo
Mary Lynn R. Nierodzik, Francis Kajumo and Simon Karpatkin
Cancer Res June 15 1992 (52) (12) 3267-3272;
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