Author/Authors :
Kim، نويسنده , , Soo-A and Kim، نويسنده , , Hyun-Woo and Kim، نويسنده , , Do-Kyung and Kim، نويسنده , , Su-Gwan and Park، نويسنده , , Joo-Cheol and Kang، نويسنده , , Dong Wan and Kim، نويسنده , , Si-Wouk and Ahn، نويسنده , , Sang-Gun and Yoon، نويسنده , , Jung-Hoon، نويسنده ,
Abstract :
Several tumor animal models have been provided as a tool for developing cancer therapy. Here, we developed rapid, easy-to use, and cost-effective new rat animal model for invasion and metastasis of cancer using genetically k-ras-induced rat kidney cells (RK3E-ras). We observed tumor as early as 3 days after injection of RK3E-ras cells in subcutaneous of Sprague–Dawley rats. Tumor size and volume were increased exponentially for 2 weeks. The tail vein injected rats obtained the lethal infiltration in the lung within 2 weeks. This tumor animal model has great potential for studying cancer processes and short-term screening of variable cancer therapy strategy.
Keywords :
RK3E , K-ras , Tumor Model , Sprague–Dawley rat
