TUMOR DORMANCY IN VIVO BY PREVENTION OF NEOVASCULARIZATION

doi:10.1084/jem.136.2.261

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ARTICLE

TUMOR DORMANCY IN VIVO BY PREVENTION OF NEOVASCULARIZATION

Michael A. Gimbrone Jr. ¹, Stephen B. Leapman ¹, Ramzi S. Cotran ¹, and Judah Folkman ¹

¹ From the Department of Surgery, Children's Hospital Medical Center; the Harvard Pathology Unit, Mallory Institute of Pathology; and the Departments of Surgery and Pathology, Harvard Medical School, Boston, Massachusetts 02115

Dormant solid tumors were produced in vivo by prevention ofneovascularization.

When small fragments of anaplastic Brown-Pearcecarcinoma were implanted directly on the iris in susceptiblerabbits, they always vascularized. A characteristic growth pattern,consisting of prevascular, vascular, and late phases, was observed,which terminated with destruction of the eye within 2 wk. Thebeginning of exponential volume increase was shown to coincidewith vascularization of the implant, as demonstrated by perfusionwith intravenous fluorescein and by histologic sections.

Incontrast, implants placed in the anterior chamber, at a distancefrom the iris, did not become vascularized. After initial growthinto spheroids, they remained arrested at a small size comparableto prevascular iris implants, for periods as long as 6 wk. Althoughdormant in terms of expansion, these avascular tumors containeda population of viable and mitotically active tumor cells. Whenreimplanted on the iris, vascularization was followed by rapid,invasive growth.

These observations suggest that neovascularizationis a necessary condition for malignant growth of a solid tumor.When a small mass of tumor cells is prevented from elicitingnew vessel ingrowth from surrounding host tissues, populationdormancy results. These data suggest that the specific blockadeof tumor-induced angiogenesis may be an effective means of controllingneoplastic growth.

Submitted on April 3, 1972

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