The role of fibronectin in tumor implantation at surgical sites

Failure of surgical treatment for gastrointestinal cancers is often caused by recurrence of the tumor in traumatized peritoneal surfaces. This study examined the effect of intraperitoneal administration of doxorubicin and recombinant tissue plasminogen activator (rt‐PA), a fibrinolytic agent, on incidence and volume of postoperative tumor implants in peritoneal wounds. Prior to randomization, a surgical wound was created on the right parietal peritoneum of 110 BDIX rats and 6 × 105 DHD/K12 colon cancer cells were inoculated intraperitoneally (ip). The control group was given an intraperitoneal injection of saline. Five groups received 1 mg/kg of ip doxorubicin at different times postoperatively: at the end of surgery (DO), 3 hr after surgery (D + 3), postoperative day 1 (Dl), postoperative day 3 (D3), and postoperative day 7(D7). In a second set of experiments, five groups of rats received, in addition to postoperative doxorubicin, 5 mg/kg of intraoperative ip rt‐PA. Incidence and volume of tumor implants in peritoneal wounds were assessed for each group 20 days after the tumor inoculation. All rats of the control group (incidence = 100%) developed tumor implants in peritoneal wounds. Mean (SD) volume was 16.2 (4.7) mm3. When administered at DO, D + 3, and Dl intraperitoneal doxorubicin reduced significantly the incidence and volume of tumor implants in wounds. Postoperative administration of doxorubicin at D3 and D7 did not affect significantly the incidence and the volume of tumor implants in peritoneal wounds. When rt‐PA was administered intraoperatively, ip injection of doxorubicin at any postoperative timing decreased significantly the incidence and volume of tumor implants. In conclusion, ip doxorubicin administered before postoperative D3 may act on tumor cell implanted in peritoneal wounds. Delayed (D3, D7) ip administration of doxorubicin does not prevent the development of tumor implants in peritoneal wounds. Intraoperative administration of rt‐PA may significantly increase the efficacy of delayed ip chemotherapy. © 1996 Wiley‐Liss, Inc.

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Effect of intraperitoneal chemotherapy and fibrinolytic therapy on tumor implantation in wound sites

Jacquet

Stuart

Dalton

et al. 1996

J. Surg. Oncol.

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The potential role of integrin receptor subunits in the formation of local recurrence and distant metastasis by mouse breast cancer cells

et al. 1996

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Molecular and cellular basis of cancer invasion and metastasis: Implications for treatment

Jiang

Puntis

Hallett

1994

Journal of British Surgery

120

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In the past decade significant advances in establishing the underlying biological mechanisms of tumour invasion and metastasis have been made. Some of the triggering factors and genes relevant to metastatic spread have been identified. Advances have also been made in understanding the signal transduction pathways involved in invasion and metastasis. This increased comprehension of the malignant metastatic process has enabled new antimetastatic strategies to be devised. This review summarizes progress in these areas and discusses the implications for the treatment of metastasis.

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The role of fibronectin in tumor implantation at surgical sites

Cited by 13 publications

References 47 publications

Effect of intraperitoneal chemotherapy and fibrinolytic therapy on tumor implantation in wound sites

Effect of intraperitoneal chemotherapy and fibrinolytic therapy on tumor implantation in wound sites

The potential role of integrin receptor subunits in the formation of local recurrence and distant metastasis by mouse breast cancer cells

Molecular and cellular basis of cancer invasion and metastasis: Implications for treatment

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