Mouse mutants reveal that putative protein interaction sites in the p53 proline-rich domain are dispensable for tumor suppression - Wikidata - wikimedia - TriplyDB

Mouse mutants reveal that putative protein interaction sites in the p53 proline-rich domain are dispensable for tumor suppression

Mouse mutants reveal that putative protein interaction sites in the p53 proline-rich domain are dispensable for tumor suppression

http://www.wikidata.org/entity/Q35641901

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Prolyl isomerase Pin1 as a molecular switch to determine the fate of phosphoproteins Prolyl isomerase Pin1 in cancer Deacetylation of p53 induces autophagy by suppressing Bmf expression p53 Amino-terminus region (1-125) stabilizes and restores heat denatured p53 wild phenotype.Posttranslational modification of p53: cooperative integrators of function p53 at a glance.In vivo analysis of p53 tumor suppressor function using genetically engineered mouse models The Naked Mole Rat Genome Resource: facilitating analyses of cancer and longevity-related adaptations.A genetic variant of p53 restricts the mucous secretory phenotype by regulating SPDEF and Bcl-2 expression.The relationship of TP53 R72P polymorphism to disease outcome and TP53 mutation in myelodysplastic syndromes Peptidyl Prolyl Isomerase PIN1 Directly Binds to and Stabilizes Hypoxia-Inducible Factor-1α.MDM2 and MDM4: p53 regulators as targets in anticancer therapy.Structure of tumor suppressor p53 and its intrinsically disordered N-terminal transactivation domain.p53 polymorphisms: cancer implications.The tumor suppressor p53: from structures to drug discovery.Peptidyl-prolyl cis-trans isomerase Pin1 in ageing, cancer and Alzheimer disease.Illuminating p53 function in cancer with genetically engineered mouse models.Insights into wild-type and mutant p53 functions provided by genetically engineered mice.Genetic Modifiers of the p53 Pathway.Does control of mutant p53 by Mdm2 complicate cancer therapy?Activation of p53 following ionizing radiation, but not other stressors, is dependent on the proline-rich domain (PRD).Chromatin remodeling protein MORC2 promotes breast cancer invasion and metastasis through a PRD domain-mediated interaction with CTNND1.The proline rich domain of p53 is dispensable for MGMT-dependent DNA repair and cell survival following alkylation damage.

P2860

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P2860

Mouse mutants reveal that putative protein interaction sites in the p53 proline-rich domain are dispensable for tumor suppression

http://www.wikidata.org/entity/Q35641901

description

2006 nî lūn-bûn

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2006年の論文

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2006年論文

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2006年論文

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2006年論文

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2006年論文

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2006年論文

@zh-tw

2006年论文

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2006年论文

@zh

2006年论文

@zh-cn

name

Mouse mutants reveal that puta ...... pensable for tumor suppression

@ast

Mouse mutants reveal that puta ...... pensable for tumor suppression

@en

type

label

Mouse mutants reveal that puta ...... pensable for tumor suppression

@ast

Mouse mutants reveal that puta ...... pensable for tumor suppression

@en

prefLabel

Mouse mutants reveal that puta ...... pensable for tumor suppression

@ast

Mouse mutants reveal that puta ...... pensable for tumor suppression

@en

P1433

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P2860

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P1433

Molecular and Cellular Biology

P1476

Mouse mutants reveal that puta ...... pensable for tumor suppression

@en

P2093

Chung-Wen Liu

http://www.w3.org/2001/XMLSchema#string

Crystal J Lee

http://www.w3.org/2001/XMLSchema#string

Franck Toledo

http://www.w3.org/2001/XMLSchema#string

Geoffrey M Wahl

http://www.w3.org/2001/XMLSchema#string

Kurt A Krummel

http://www.w3.org/2001/XMLSchema#string

Luo-Wei Rodewald

http://www.w3.org/2001/XMLSchema#string

P2860

Direct activation of Bax by p53 mediates mitochondrial membrane permeabilization and apoptosis

Identification of a novel p53 functional domain that is necessary for efficient growth suppression

PUMA couples the nuclear and cytoplasmic proapoptotic function of p53

The structure and function of proline-rich regions in proteins

The requirement for the p53 proline-rich functional domain for mediation of apoptosis is correlated with specific PIG3 gene transactivation and with transcriptional repression.

Role of Pin1 in the regulation of p53 stability and p21 transactivation, and cell cycle checkpoints in response to DNA damage

The prolyl isomerase Pin1 reveals a mechanism to control p53 functions after genotoxic insults

Phosphorylation-specific prolyl isomerization: is there an underlying theme?

Critical roles for the serine 20, but not the serine 15, phosphorylation site and for the polyproline domain in regulating p53 turnover

Sequence-specific and phosphorylation-dependent proline isomerization: a potential mitotic regulatory mechanism

P304

1425-1432

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scholarly article

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10.1128/MCB.00999-06

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4

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27

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2006-12-11T00:00:00Z

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6640630

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17158931

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1800716

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