Retinoblastoma in transgenic mice
Publication date
1990
Authors
Windle, J.J.
Albert, D.M.
O'Brien, J.M.
Marcus, D.M.
Disteche, Ch.M.
Bernards, R.A.
Mellon, P.L.
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Document Type
Article
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Abstract
Retinoblastoma, a malignancy of the eye occurring in young
children, has been widely studied as a model for genetic predisposition
to cancer. This disease is caused by mutations in both alleles
of an anti-oncogene (the retinoblastoma gene, Rb) that inactivate
or eliminate the Rb encoded protein, pl05rb. Here
we report that expression of a viral oncogene, the simian virus 40
T antigen, in the retina of transgenic mice produces heritable
ocular tumours with histological, ultrastructural and immunohistochemical
features identical to those of human retinoblastoma.
Furthermore, we demonstrate a specific association between
plO5rb and T antigen in mouse retinoblastoma tumour cells. Thus, the occurrence of these tumours is in vivo evidence for oncogenesis
due to the ocular-specific expression of an Rb-binding oncoprotein
that can functionally inactivate the Rb protein. As an animal model
for heritable retinoblastoma, these mice should allow the study of
the ontogeny, pathogenesis and treatment of this malignant disease.