RhoC is dispensable for embryogenesis and tumor initiation but essential for metastasis
Anne Hakem(Ontario Institute for Cancer Research), Otto Sanchez-Sweatman(Ontario Institute for Cancer Research), Annick You-Ten(Ontario Institute for Cancer Research), Gordon S. Duncan(Ontario Institute for Cancer Research), Andrew Wakeham(Ontario Institute for Cancer Research), Rama Khokha(Ontario Institute for Cancer Research), Tak W. Mak(Ontario Institute for Cancer Research)
Cited by 292Open Access
Abstract
The Rho proteins are Ras-related guanosine triphosphatases (GTPases) that function in cytoskeletal reorganization, cell migration, and stress fiber and focal adhesion formation. Overexpression of RhoC enhances the ability of melanoma cells to exit the blood and colonize the lungs. However, in vivo confirmation of RhoC's role in metastasis has awaited a RhoC-deficient mouse model. Here we report the generation of RhoC-deficient mice and show that RhoC is dispensable for embryonic and post-natal development. We demonstrate that loss of RhoC does not affect tumor development but decreases tumor cell motility and metastatic cell survival leading to a drastic inhibition of metastasis.
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