Regulation of Lef-mediated transcription and p53-dependent pathway by associating β-catenin with CBP/p300

Makoto Miyagishi; Ryouji Fujii; Mitsutoki Hatta; Eisaku Yoshida; Natsumi Araya; Akira Nagafuchi; Satoru Ishihara; Toshihiro Nakajima; Akiyoshi Fukamizu

doi:10.1074/jbc.C000258200

Regulation of Lef-mediated transcription and p53-dependent pathway by associating β-catenin with CBP/p300

Makoto Miyagishi
, Ryouji Fujii
, Mitsutoki Hatta
, Eisaku Yoshida
, Natsumi Araya
, Akira Nagafuchi
, Satoru Ishihara
, Toshihiro Nakajima
, Akiyoshi Fukamizu

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

102 被引用数 (Scopus)

抄録

CBP and its homologue p300 play significant roles in cell differentiation, cell cycle, and anti-oncogenesis. We demonstrated that β-catenin, recently known as a potent oncogene, and CBP/p300 are associated through its CH3 region, which is a primary target of adenoviral oncoprotein E1A and various nuclear proteins, such as p53, cyclin E, and AP-1, and both are colocalized in the nuclear bodies. CBP/p300 potentiated Lef-mediated transactivation of β-catenin, and E1A, a potent inhibitor of CBP/p300, repressed its transactivation. Furthermore, overexpression of stable β-catenin mutant competitively suppressed the p53-dependent pathway. These may be a key mechanism of β-catenin involved in oncogenic events underlying disruption of tumor suppressor function through CBP/p300.

本文言語	英語
ページ（範囲）	35170-35175
ページ数	6
ジャーナル	Journal of Biological Chemistry
巻	275
号	45
DOI	https://doi.org/10.1074/jbc.C000258200
出版ステータス	出版済み - 10-11-2000
外部発表	はい

All Science Journal Classification (ASJC) codes

生化学
分子生物学
細胞生物学

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10.1074/jbc.C000258200

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引用スタイル

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title = "Regulation of Lef-mediated transcription and p53-dependent pathway by associating β-catenin with CBP/p300",

abstract = "CBP and its homologue p300 play significant roles in cell differentiation, cell cycle, and anti-oncogenesis. We demonstrated that β-catenin, recently known as a potent oncogene, and CBP/p300 are associated through its CH3 region, which is a primary target of adenoviral oncoprotein E1A and various nuclear proteins, such as p53, cyclin E, and AP-1, and both are colocalized in the nuclear bodies. CBP/p300 potentiated Lef-mediated transactivation of β-catenin, and E1A, a potent inhibitor of CBP/p300, repressed its transactivation. Furthermore, overexpression of stable β-catenin mutant competitively suppressed the p53-dependent pathway. These may be a key mechanism of β-catenin involved in oncogenic events underlying disruption of tumor suppressor function through CBP/p300.",

author = "Makoto Miyagishi and Ryouji Fujii and Mitsutoki Hatta and Eisaku Yoshida and Natsumi Araya and Akira Nagafuchi and Satoru Ishihara and Toshihiro Nakajima and Akiyoshi Fukamizu",

year = "2000",

month = nov,

day = "10",

doi = "10.1074/jbc.C000258200",

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TY - JOUR

T1 - Regulation of Lef-mediated transcription and p53-dependent pathway by associating β-catenin with CBP/p300

AU - Miyagishi, Makoto

AU - Fujii, Ryouji

AU - Hatta, Mitsutoki

AU - Yoshida, Eisaku

AU - Araya, Natsumi

AU - Nagafuchi, Akira

AU - Ishihara, Satoru

AU - Nakajima, Toshihiro

AU - Fukamizu, Akiyoshi

PY - 2000/11/10

Y1 - 2000/11/10

N2 - CBP and its homologue p300 play significant roles in cell differentiation, cell cycle, and anti-oncogenesis. We demonstrated that β-catenin, recently known as a potent oncogene, and CBP/p300 are associated through its CH3 region, which is a primary target of adenoviral oncoprotein E1A and various nuclear proteins, such as p53, cyclin E, and AP-1, and both are colocalized in the nuclear bodies. CBP/p300 potentiated Lef-mediated transactivation of β-catenin, and E1A, a potent inhibitor of CBP/p300, repressed its transactivation. Furthermore, overexpression of stable β-catenin mutant competitively suppressed the p53-dependent pathway. These may be a key mechanism of β-catenin involved in oncogenic events underlying disruption of tumor suppressor function through CBP/p300.

AB - CBP and its homologue p300 play significant roles in cell differentiation, cell cycle, and anti-oncogenesis. We demonstrated that β-catenin, recently known as a potent oncogene, and CBP/p300 are associated through its CH3 region, which is a primary target of adenoviral oncoprotein E1A and various nuclear proteins, such as p53, cyclin E, and AP-1, and both are colocalized in the nuclear bodies. CBP/p300 potentiated Lef-mediated transactivation of β-catenin, and E1A, a potent inhibitor of CBP/p300, repressed its transactivation. Furthermore, overexpression of stable β-catenin mutant competitively suppressed the p53-dependent pathway. These may be a key mechanism of β-catenin involved in oncogenic events underlying disruption of tumor suppressor function through CBP/p300.

UR - https://www.scopus.com/pages/publications/0034634586

UR - https://www.scopus.com/pages/publications/0034634586#tab=citedBy

U2 - 10.1074/jbc.C000258200

DO - 10.1074/jbc.C000258200

M3 - Article

C2 - 10906119

AN - SCOPUS:0034634586

SN - 0021-9258

VL - 275

SP - 35170

EP - 35175

JO - Journal of Biological Chemistry

JF - Journal of Biological Chemistry

IS - 45

ER -

Regulation of Lef-mediated transcription and p53-dependent pathway by associating β-catenin with CBP/p300

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