Add to ORKGp53 mutations are the most commonly observed genetic alterations in human cancers to date. A majority of these point mutations cluster in four evolutionarily conserved domains spanning amino acids 100-300. This region of p53 has been called its central conserved, or conformational domain. This domain of p53 is also targeted by the SV40 T antigen. Mutation, as well as interaction with SV40 T antigen results in inactivation of p53. We hypothesized that mutations and SV40 T antigen disrupt p53 function by interfering with the molecular interactions of the central conserved domain. Using a chimeric protein consisting of the central conserved domain of wild-type p53 (amino acids 115-295) and a protein A affinity tail, we isolated several cellula...
The tumor suppressor protein p53 can lose its function upon DNA-contact mutations (R273C and R273H) ...
<div><p>The tumor suppressor protein p53 can lose its function upon DNA-contact mutations (R273C and...
To gain insights into the mechanisms by which certain second-site suppressor mutations rescue the fu...
p53 mutations are the most commonly observed genetic alterations in human cancers to date. A majorit...
The tumor suppressor protein p53 was first isolated as a simian virus 40 large T antigen-associated ...
The p53 tumor suppressor is a sequence-specific DNA binding protein that activates gene transcriptio...
We identified a minimal domain of human p53 required for the transactivation of a p53 response eleme...
The p53 protein is a critical tumor suppressor that is mutated in over half of all human cancers. It...
We showed previously that bacterially expressed full-length human wild-type p53b(1-393) binds select...
The DNA binding activity of p53 is required for its tumor suppressor function; we show here that thi...
p53 is an intrinsically disordered transcription factor that suppresses tumor development by arresti...
AbstractThe tetrameric tumor suppressor p53 plays a pivotal role in the control of the cell cycle an...
p53 is required for the maintenance of the genomic stability of cells. Mutations in the p53 tumor-su...
p53 is required for the maintenance of the genomic stability of cells. Mutations in the p53 tumor-su...
An intramolecular interaction between the p53 transactivation and DNA binding domains inhibits DNA b...
The tumor suppressor protein p53 can lose its function upon DNA-contact mutations (R273C and R273H) ...
<div><p>The tumor suppressor protein p53 can lose its function upon DNA-contact mutations (R273C and...
To gain insights into the mechanisms by which certain second-site suppressor mutations rescue the fu...
p53 mutations are the most commonly observed genetic alterations in human cancers to date. A majorit...
The tumor suppressor protein p53 was first isolated as a simian virus 40 large T antigen-associated ...
The p53 tumor suppressor is a sequence-specific DNA binding protein that activates gene transcriptio...
We identified a minimal domain of human p53 required for the transactivation of a p53 response eleme...
The p53 protein is a critical tumor suppressor that is mutated in over half of all human cancers. It...
We showed previously that bacterially expressed full-length human wild-type p53b(1-393) binds select...
The DNA binding activity of p53 is required for its tumor suppressor function; we show here that thi...
p53 is an intrinsically disordered transcription factor that suppresses tumor development by arresti...
AbstractThe tetrameric tumor suppressor p53 plays a pivotal role in the control of the cell cycle an...
p53 is required for the maintenance of the genomic stability of cells. Mutations in the p53 tumor-su...
p53 is required for the maintenance of the genomic stability of cells. Mutations in the p53 tumor-su...
An intramolecular interaction between the p53 transactivation and DNA binding domains inhibits DNA b...
The tumor suppressor protein p53 can lose its function upon DNA-contact mutations (R273C and R273H) ...
<div><p>The tumor suppressor protein p53 can lose its function upon DNA-contact mutations (R273C and...
To gain insights into the mechanisms by which certain second-site suppressor mutations rescue the fu...