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Volumn 277, Issue 29, 2002, Pages 26699-26707

A novel p53 transcriptional repressor element (p53TRE) and the asymmetrical contribution of two p53 binding sites modulate the response of the placental transforming growth factor-β promoter to p53

(3) Wong, Jeffrey a Li, Pei Xiang b Klamut, Henry J a

a PRINCESS MARGARET HOSPITAL (Canada)

b UNIVERSITY OF TORONTO (Canada)

Author keywords

[No Author keywords available]

Indexed keywords

BIOASSAY; DNA; ELECTROPHORESIS; GROWTH KINETICS; RNA; SIGNALING;

TRANSCIPTIONAL REPRESSOR ELEMENT;

BIOCHEMISTRY;

MESSENGER RNA; P53 TRANSCRIPTIONAL REPRESSOR ELEMENT; PLACENTAL TRANSFORMING GROWTH FACTOR BETA; PROTEIN P21; PROTEIN P53; REPRESSOR PROTEIN; TRANSFORMING GROWTH FACTOR BETA; UNCLASSIFIED DRUG;

ARTICLE; BINDING SITE; CONTROLLED STUDY; DOWN REGULATION; ELECTROPHORETIC MOBILITY; HUMAN; HUMAN CELL; KINETICS; MUTATIONAL ANALYSIS; PRIORITY JOURNAL; PROMOTER REGION; PROTEIN BINDING; PROTEIN EXPRESSION; PROTEIN FUNCTION; TRANSACTIVATION; TRANSCRIPTION REGULATION; TUMOR CELL LINE;

BASE SEQUENCE; BINDING SITES; CYCLIN-DEPENDENT KINASE INHIBITOR P21; CYCLINS; DNA MUTATIONAL ANALYSIS; DOWN-REGULATION; FEMALE; GROWTH SUBSTANCES; HELA CELLS; HUMANS; MOLECULAR SEQUENCE DATA; PREGNANCY PROTEINS; PROMOTER REGIONS (GENETICS); REPRESSOR PROTEINS; RNA, MESSENGER; STRUCTURE-ACTIVITY RELATIONSHIP; TRANS-ACTIVATION (GENETICS); TUMOR CELLS, CULTURED; TUMOR SUPPRESSOR PROTEIN P53;

EID: 0037135581 PISSN: 00219258 EISSN: None Source Type: Journal
DOI: 10.1074/jbc.M203020200 Document Type: Article

Times cited : (22)

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