Journal ArticleDOI
The codon 72 polymorphic variants of p53 have markedly different apoptotic potential.
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TLDR
It is found that in cell lines containing inducible versions of alleles encoding the Pro72 and Arg72 variants, and in cells with endogenous p53, the Arg72 variant induces apoptosis markedly better than does the Pro 72 variant.Abstract:
The gene TP53, encoding p53, has a common sequence polymorphism that results in either proline or arginine at amino-acid position 72. This polymorphism occurs in the proline-rich domain of p53, which is necessary for the protein to fully induce apoptosis. We found that in cell lines containing inducible versions of alleles encoding the Pro72 and Arg72 variants, and in cells with endogenous p53, the Arg72 variant induces apoptosis markedly better than does the Pro72 variant. Our data indicate that at least one source of this enhanced apoptotic potential is the greater ability of the Arg72 variant to localize to the mitochondria; this localization is accompanied by release of cytochrome c into the cytosol. These data indicate that the two polymorphic variants of p53 are functionally distinct, and these differences may influence cancer risk or treatment.read more
Citations
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Association of rheumatoid arthritis with Mdm2 SNP309 and genetic evidence for an allele-specific interaction between MDM2 and p53 P72R variants: a case control study.
Gunter Assmann,J. Voswinkel,M. Mueller,Jörg Thomas Bittenbring,J. Koenig,A. Menzel,Michael Pfreundschuh,K. Roemer,Inga Melchers +8 more
TL;DR: The function of MDM2 depends on the p53 P72R genotype, resulting in either an increased or reduced risk for RA, and it is suggested that in most casesMDM2 stabilizes the conformation of p53, whereas in p53 PP-positive subjects MDM 2 supports the degradation of p 53.
Journal ArticleDOI
TP53 and MDM2 single nucleotide polymorphisms influence survival in non-del(5q) myelodysplastic syndromes.
Kathy L. McGraw,Thomas Cluzeau,David A. Sallman,Ashley A. Basiorka,Brittany A. Irvine,Ling Zhang,Pearlie K. Epling-Burnette,Dana E. Rollison,Mar Mallo,Lubomir Sokol,Francesc Solé,Jaroslaw P. Maciejewski,Alan F. List +12 more
TL;DR: A novel functional SNP scoring system based on predicted p53 activity to provide a novel scoring system independent of IPSS that is predictive for disease outcome and underscore the importance of TP53 R72P and MDM2 SNP309 SNPs in MDS.
Journal ArticleDOI
MDM2 promoter polymorphism and p53 codon 72 polymorphism in chronic myeloid leukemia: The association between MDM2 promoter genotype and disease susceptibility, age of onset, and blast‐free survival in chronic phase patients receiving imatinib
Yi-Chang Liu,Hui-Hua Hsiao,Wen-Chi Yang,Ta-Chih Liu,Chao-Sung Chang,Ming-Yu Yang,Pai-Mei Lin,Jui-Feng Hsu,Ching-Ping Lee,Sheng-Fung Lin +9 more
TL;DR: Closely monitoring CML patients harboring the p53 R72P and MDM2 SNP309 G/G genotype is warranted, as it is associated with an increased risk of CML susceptibility and BP transformation under imatinib treatment.
Journal ArticleDOI
Investigation of genetic polymorphisms related to the outcome of radiotherapy for prostate cancer patients.
Hellen S Cintra,Juliana Castro Dourado Pinezi,Graziella Dias Pinheiro Machado,Gustavo Moura de Carvalho,Ana Terra Silva Carvalho,Thalles Eduardo Dias dos Santos,Ricardo D. Marciano,Renata de Bastos Ascenço Soares +7 more
TL;DR: The results show that clinical characteristics were not determinant on the developing of radiation sensitivity in prostate cancer patients, and intronic TP53 polymorphisms would be associated with increased acute and chronic radiation toxicities, corroborate the importance of investigating the genetic profile to predict adverse side effects in patients undergoing radiotherapy.
Journal ArticleDOI
Genetic variations in TP53 binding sites are predictors of clinical outcomes in prostate cancer patients
Victor C. Lin,Chao-Yuan Huang,Yung-Chin Lee,Chia-Cheng Yu,Chia-Cheng Yu,Ta-Yuan Chang,Te-Ling Lu,Shu-Pin Huang,Bo-Ying Bao +8 more
TL;DR: The results suggested that SNPs within TP53 binding sites might be valuable biomarkers for prostate cancer outcome prediction.
References
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Journal ArticleDOI
WAF1, a potential mediator of p53 tumor suppression
Wafik S. El-Deiry,Takashi Tokino,Victor E. Velculescu,Daniel B. Levy,Ramon Parsons,Jeffrey M. Trent,D Lin,W. Edward Mercer,Kenneth W. Kinzler,Bert Vogelstein +9 more
TL;DR: A gene is identified, named WAF1, whose induction was associated with wild-type but not mutant p53 gene expression in a human brain tumor cell line and that could be an important mediator of p53-dependent tumor growth suppression.
Journal ArticleDOI
Mice Lacking p21CIP1/WAF1 undergo normal development, but are defective in G1 checkpoint control
Chu-Xia Deng,Chu-Xia Deng,Pumin Zhang,J. Wade Harper,Stephen J. Elledge,Stephen J. Elledge,Philip Leder,Philip Leder +7 more
TL;DR: The results establish the role of p21CIP1/WAF1 in the G1 checkpoint, but suggest that the anti-apoptotic and theAnti-oncogenic effects of p53 are more complex.
Journal ArticleDOI
Protein regulation by monoubiquitin
TL;DR: Multi-ubiquitin chains at least four subunits long are required for efficient recognition and degradation of ubiquitylated proteins by the proteasome, but other functions of ubiquitin have been discovered that do not involve the protease.
Journal ArticleDOI
Role of a p53 polymorphism in the development of human papillomavirus-associated cancer.
Alan Storey,Miranda Thomas,Ann Kalita,Catherine A. Harwood,Daniela Gardiol,Fiamma Mantovani,Judith Breuer,Irene M. Leigh,Greg Matlashewski,Lawrence Banks +9 more
TL;DR: Allelic analysis of patients with HPV-associated tumours revealed a striking overrepresentation of homozygous arginine-72 p53 compared with the normal population, which indicated that individuals homozygously for arginin 72 are about seven times more susceptible to HPV- associated tumorigenesis than heterozygotes.
Journal ArticleDOI
Death signal-induced localization of p53 protein to mitochondria. A potential role in apoptotic signaling
TL;DR: This work proposes a model where p53 can contribute to apoptosis by direct signaling at the mitochondria, thereby amplifying the transcription-dependent apoptosis of p53.