Cooperation of the tumour suppressors IRF-1 and p53 in response to DNA damage

Tanaka, Nobuyuki; Ishihara, Masahiko; Lamphier, Marc S.; Nozawa, Hiroaki; Matsuyama, Tomohiro; Mak, Tak W.; Aizawa, Shinichi; Tokino, Takashi; Oren, Moshe; Taniguchi, Tadatsugu

doi:10.1038/382816a0

Cited by 320 publications

(298 citation statements)

References 26 publications

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“…Although BAX expression is not modulated during the combined activation of HER1 and IRF-1 (data not shown) the experiments demonstrate a further similarity between IRF-1 and p53. It has been reported earlier that both tumor suppressor proteins cooperate in response to DNA damage (Tamura et al, 1995;Tanaka et al, 1996).…”

Section: Discussionmentioning

confidence: 95%

“…The principle of synergistic action of transcription factors with IRF-1 is quite common; IRF-1 has been shown to cooperatively interact with TFIIB (Wang et al, 1996); NF-kB (Drew et al, 1995), and STAT1 (Chon et al, 1996). It is also described that IRF-1 together with p53 induces the cell cycle inhibitor p21 (Tanaka et al, 1996). However, so far we were not able to detect a direct interaction of IRF-1 with one of the STAT proteins, neither by gel retardation nor by a two hybrid system in mammalian cells (data not shown).…”

Section: Discussionmentioning

confidence: 99%

“…MHC class I (Hobart et al, 1996;Salkowski et al, 1996), iNOS (Kamijo et al, 1994) and GBP (Briken et al, 1995). IRF-1 is also necessary for proper expression of IL-15 (Ogasawara et al, 1998), p21 (Tanaka et al, 1996), and IFN-b (Fujita et al, 1993). Studies with IRF-1 knock-out cells demonstrate that IRF-1 is involved in the differentiation and function of NK cells (Ohteki et al, 1998;Ogasawara et al, 1998), in the generation of the TH 1 type of T helper cell and DNA damage (Tamura et al, 1997;Tanaka et al, 1996).…”

Section: Introductionmentioning

confidence: 99%

“…IRF-1 is also necessary for proper expression of IL-15 (Ogasawara et al, 1998), p21 (Tanaka et al, 1996), and IFN-b (Fujita et al, 1993). Studies with IRF-1 knock-out cells demonstrate that IRF-1 is involved in the differentiation and function of NK cells (Ohteki et al, 1998;Ogasawara et al, 1998), in the generation of the TH 1 type of T helper cell and DNA damage (Tamura et al, 1997;Tanaka et al, 1996). Moreover, IRF-1 shows tumor suppressor activity under certain conditions (Tanaka et al, 1994b(Tanaka et al, , 1996 and IRF-1 overexpression inhibits cell growth (Kirchho et al, 1993).…”

Section: Introductionmentioning

confidence: 99%

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Cooperative activity between HER oncogenes and the tumor suppressor IRF-1 results in apoptosis

Kirchhoff¹,

Hauser²

1999

Oncogene

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Section: Discussionmentioning

confidence: 95%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Cooperative activity between HER oncogenes and the tumor suppressor IRF-1 results in apoptosis

Kirchhoff¹,

Hauser²

1999

Oncogene

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“…It was found that IRF7/7 MEFs are de®cient in their ability to undergo DNA-damageinduced cell-cycle arrest (Tanaka et al, 1996). Transcriptional activation of the cyclin dependent kinase inhibitor (CDKI) p21 gene in these cells by irradiation, was found to be dependent both on p53 and IRF-1.…”

Section: Terminal DI Erentiation Negative Growth Control and Myd Genesmentioning

confidence: 99%

MyD genes in negative growth control

Liebermann

Hoffman

1998

Oncogene

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Induction of expression of MHC-class-II antigen on human thyroid carcinoma by wild-type p53

et al. 1998

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Mutation of the tumor‐suppressor gene p53 is involved in carcinogenetics. We investigated the role of p53 in the induction of anti‐tumor immune responses by establishing a thyroid carcinoma cell line (1F3) prepared by transfection of wild‐type human p53 gene into a p53‐deficient cell line (FRO). Our results showed for the first time the involvement of p53 in the induction of anti‐tumor immune responses, as demonstrated by: (i) expression of the major‐histocompatibility‐complex(MHC)‐class‐II antigen on 1F3, but not FRO; (ii) mRNA of class‐II gene was expressed both in 1F3 and in FRO, but was stable at post‐transcriptional level in FRO, which restrained protein synthesis; (iii) 1F3 induced MHC‐class‐II‐specific CD4+ cytotoxic‐T‐cell activity through allo‐antigen presentation and co‐stimulation. Although our novel results are limited to the wild‐type‐p53‐expressing clone from a p53‐deficient cell line, we suggest that the absence of p53 in carcinoma cells may reduce the induction of CD4+ cytotoxic‐T‐cell activity against carcinoma cells by diminishing the expression of class‐II antigen. Int. J. Cancer 75:391–395, 1998. © 1998 Wiley‐Liss, Inc.

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Cooperation of the tumour suppressors IRF-1 and p53 in response to DNA damage

Cited by 320 publications

References 26 publications

Cooperative activity between HER oncogenes and the tumor suppressor IRF-1 results in apoptosis

Cooperative activity between HER oncogenes and the tumor suppressor IRF-1 results in apoptosis

MyD genes in negative growth control

Induction of expression of MHC-class-II antigen on human thyroid carcinoma by wild-type p53

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