a cancer derived mutation in the retinoblastoma gene with a distinct defect for lxcxe dependent interactions癌症中视网膜母细胞瘤基因的突变与不同的缺陷lxcxe依赖交互.pdfVIP
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a cancer derived mutation in the retinoblastoma gene with a distinct defect for lxcxe dependent interactions癌症中视网膜母细胞瘤基因的突变与不同的缺陷lxcxe依赖交互
Henley et al. Cancer Cell International 2010, 10:8
/content/10/1/8
P R I M A R Y R E S E A R C H Open Access
Primary research
A cancer derived mutation in the Retinoblastoma
gene with a distinct defect for LXCXE dependent
interactions
1,3 1,3 1,3 4 1,2,3
Shauna A Henley , Sarah M Francis , Jordan Demone , Peter Ainsworth and Frederick A Dick*
Abstract
Background: The interaction between viral oncoproteins such as Simian virus 40 TAg, adenovirus E1A, and human
papilloma virus E7, and the retinoblastoma protein (pRB) occurs through a well characterized peptide sequence,
LXCXE, on the viral protein and a well conserved groove in the pocket domain of pRB. Cellular proteins, such as histone
deacetylases, also use this mechanism to interact with the retinoblastoma protein to repress transcription at cell cycle
regulated genes. For these reasons this region of the pRB pocket domain is thought to play a critical role in growth
suppression.
Results: In this study, we identify and characterize a tumor derived allele of the retinoblastoma gene (RB1) that
possesses a discrete defect in its ability to interact with LXCXE motif containing proteins that compromises proliferative
control. To assess the frequency of similar mutations in the RB1 gene in human cancer, we screened blood and tumor
samples for similar alleles. We screened almost 700 samples and did not detect additional mutations, indicating that
this class of mutation is rare.
Conclusions: Our work provides proof of principal that alleles encoding distinct, partial loss of function mutations in
the retinoblastoma gene that specifically lose LXCXE dependent interactions, are found in human cancer.
Background
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