Amino-terminal domains of c-myc and N-myc proteins mediate binding to the retinoblastoma gene product
Publication date
1991
Authors
Rustgi, A.K.
Dyson, N.
Bernards, R.A.
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Document Type
Article
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Abstract
The proteins encoded by the myc gene family are involved is the
control of cell proliferation and differentiation, and aberrant
expression of myc proteins has been implicated in the genesis of
a variety of neoplasms. In the carboxyl terminus, myc proteins
have two domains that encode a basic domain/helix-loop-helix
and a leucine zipper motif, respectively. These motifs are involved
both in DNA binding and in protein dimerization. In addition,
myc protein family members share several regions of highly conserved
amino acids in their amino termini that are essential for
transfornation. We report here that an N-terminal domain
present in both the c-myc and N-myc proteins mediates binding
to the retinoblastoma gene product PRb. We show that the human
papilloma virus E7 protein competes with c-myc for binding to
pRb, indicating that these proteins share overlapping binding sites
on pRb. Furthermore, a mutant Rb protein from a human tumour
cell line that carried a 35-amino-acM deletion in its C terminus
failed to bind to c-myc. Our results suggest that c-myc and pRb
cooperate through direct binding to central cell proliferation.