Interaction of c-Myc with the pRb-related protein p107 results in inhibition of c-Myc-mediated transactivation
Publication date
1994
Authors
Beijersbergen, R.L.
Hijmans, E.M.
Zhu, L.
Bernards, R.A.
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Article
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Abstract
The product of the c-myc proto-oncogene, c-Myc, is a
sequence-specific DNA binding protein with an Nterminal
transactivation domain and a C-terminal
DNA binding domain. Several lines of evidence indicate
that c-Myc activity is essential for normal cell cycle
progression. Since the abundance of c-Myc during the
cell cycle is constant, c-Myc's activity may be regulated
at a post-translational level. We have shown previously
that the N-terminus of c-Myc can form a specific
complex with the product of the retinoblastoma gene,
pRb, in vitro. These data suggested a model in which
pRb, or pRb-related proteins, regulate c-Myc activity
through direct binding. We show here that the pRbrelated
protein p107, but not pRb itself, forms a specific
complex with the N-terminal transactivation domain
of c-Myc in vivo. Binding of p107 to c-Myc causes a
significant inhibition of c-Myc transactivation. Expression
of c-Myc releases cells from a p107-induced growth
arrest, but not from pRb-induced growth arrest. Our
data suggest that p107 can control c-Myc activity
through direct binding to the transactivation domain
and that c-Myc is a target for p107-mediated growth
suppression.
Keywords
c-Myc, transactivation, pRb, pl07