Integration of interferon-α/β signalling to p53 responses in tumour suppression and antiviral defence

Akinori Takaoka; Sumio Hayakawa; Hideyuki Yanai; Dagmar Stoiber; Hideo Negishi; Hideaki Kikuchi; Shigeru Sasaki; Kohzoh Imai; Tsukasa Shibue; Kenya Honda; Tadatsugu Taniguchi

doi:10.1038/nature01850

Integration of interferon-α/β signalling to p53 responses in tumour suppression and antiviral defence

Akinori Takaoka
, Sumio Hayakawa
, Hideyuki Yanai
, Dagmar Stoiber
, Hideo Negishi
, Hideaki Kikuchi
, Shigeru Sasaki
, Kohzoh Imai
, Tsukasa Shibue
, Kenya Honda
, Tadatsugu Taniguchi

Publikation: Beitrag in Fachzeitschrift (peer-reviewed) › Artikel in Fachzeitschrift

804 Zitate (Scopus)

Abstract

Swift elimination of undesirable cells is an important feature in tumour suppression and immunity. The tumour suppressor p53 and interferon-α and -β (IFN-α/β) are essential for the induction of apoptosis in cancerous cells and in antiviral immune responses, respectively, but little is known about their interrelationship. Here we show that transcription of the p53 gene is induced by IFN-α/β, accompanied by an increase in p53 protein level. IFN-α/β signalling itself does not activate p53; rather, it contributes to boosting p53 responses to stress signals. We show examples in which p53 gene induction by IFN-α/β contributes to tumour suppression. Furthermore, we show that p53 is activated in virally infected cells to evoke an apoptotic response and that p53 is critical for antiviral defence of the host. Our study reveals a hitherto unrecognized link between p53 and IFN-α/β in tumour suppression and antiviral immunity, which may have therapeutic implications.

Originalsprache	Englisch
Seiten (von - bis)	516-523
Seitenumfang	8
Fachzeitschrift	Nature
Jahrgang	424
Ausgabenummer	6948
DOIs	https://doi.org/10.1038/nature01850
Publikationsstatus	Veröffentlicht - 31 Juli 2003
Extern publiziert	Ja

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abstract = "Swift elimination of undesirable cells is an important feature in tumour suppression and immunity. The tumour suppressor p53 and interferon-α and -β (IFN-α/β) are essential for the induction of apoptosis in cancerous cells and in antiviral immune responses, respectively, but little is known about their interrelationship. Here we show that transcription of the p53 gene is induced by IFN-α/β, accompanied by an increase in p53 protein level. IFN-α/β signalling itself does not activate p53; rather, it contributes to boosting p53 responses to stress signals. We show examples in which p53 gene induction by IFN-α/β contributes to tumour suppression. Furthermore, we show that p53 is activated in virally infected cells to evoke an apoptotic response and that p53 is critical for antiviral defence of the host. Our study reveals a hitherto unrecognized link between p53 and IFN-α/β in tumour suppression and antiviral immunity, which may have therapeutic implications.",

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AU - Takaoka, Akinori

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AU - Yanai, Hideyuki

AU - Stoiber, Dagmar

AU - Negishi, Hideo

AU - Kikuchi, Hideaki

AU - Sasaki, Shigeru

AU - Imai, Kohzoh

AU - Shibue, Tsukasa

AU - Honda, Kenya

AU - Taniguchi, Tadatsugu

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AB - Swift elimination of undesirable cells is an important feature in tumour suppression and immunity. The tumour suppressor p53 and interferon-α and -β (IFN-α/β) are essential for the induction of apoptosis in cancerous cells and in antiviral immune responses, respectively, but little is known about their interrelationship. Here we show that transcription of the p53 gene is induced by IFN-α/β, accompanied by an increase in p53 protein level. IFN-α/β signalling itself does not activate p53; rather, it contributes to boosting p53 responses to stress signals. We show examples in which p53 gene induction by IFN-α/β contributes to tumour suppression. Furthermore, we show that p53 is activated in virally infected cells to evoke an apoptotic response and that p53 is critical for antiviral defence of the host. Our study reveals a hitherto unrecognized link between p53 and IFN-α/β in tumour suppression and antiviral immunity, which may have therapeutic implications.

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Integration of interferon-α/β signalling to p53 responses in tumour suppression and antiviral defence

Abstract

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