Microcirculation and metastasis in a new mouse mammary tumor model system

Cheung,A; Young,L; Chen,P; Chao,C; Ndoye,A; Barry,P; Muller,W; Cardiff,R

doi:10.3892/ijo.11.1.69

Microcirculation and metastasis in a new mouse mammary tumor model system

Authors:
- A Cheung
- L Young
- P Chen
- C Chao
- A Ndoye
- P Barry
- W Muller
- R Cardiff
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Affiliations: UNIV CALIF DAVIS,SCH MED,DEPT MED PATHOL,DAVIS,CA 95616. UNIV CALIF SAN DIEGO,INST BIOMED ENGN,LA JOLLA,CA 92093. FOURTH MIL MED UNIV,TEACHING HOSP 2,DEPT PATHOL,XIAN 710038,PEOPLES R CHINA. MCMASTER UNIV,INST MOL BIOL & TECHNOL,HAMILTON,ON L8S 4K1,CANADA.
Published online on: July 1, 1997 https://doi.org/10.3892/ijo.11.1.69
Pages: 69-77

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Abstract

Two new metastatic mouse mammary tumor transplant lines have been established in nude mice. The Met-1 line, with the polyoma virus middle T (PyV-MT) transgene, metastasized with 100% efficiency. The Db-7 line, expressing a PyV-MT transgene mutated at positions 315 and 322, metastasized with 8.8% efficiency. Histology and computer-assisted intravital microscopy demonstrated that internal microcirculation in Met-1 was more complex than Db-7; Met-1 exhibited higher microvessel density and tortuosity (P < 0.0001). These indices of microvascular complexity correlated with the higher Met-1 metastatic rate (P < 0.0001). These two transplantable lines will be useful for investigating the complex relationship between angiogenesis and metastasis.