p53 dynamics vary between tissues and are linked with radiation sensitivity

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作者
Jacob Stewart-Ornstein
Yoshiko Iwamoto
Miles A. Miller
Mark A. Prytyskach
Stephane Ferretti
Philipp Holzer
Joerg Kallen
Pascal Furet
Ashwini Jambhekar
William C. Forrester
Ralph Weissleder
Galit Lahav
机构
[1] Blavatnik Institute at Harvard Medical School,Department of Systems Biology and the Ludwig Center at Harvard
[2] Massachusetts General Hospital,Center for Systems Biology
[3] Novartis Institutes for Biomedical Research,Department of Computational and Systems Biology
[4] Chemical Biology and Therapeutics,undefined
[5] Novartis Institutes for Biomedical Research,undefined
[6] University of Pittsburgh Medical School,undefined
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Radiation sensitivity varies greatly between tissues. The transcription factor p53 mediates the response to radiation; however, the abundance of p53 protein does not correlate well with the extent of radiosensitivity across tissues. Given recent studies showing that the temporal dynamics of p53 influence the fate of cultured cells in response to irradiation, we set out to determine the dynamic behavior of p53 and its impact on radiation sensitivity in vivo. We find that radiosensitive tissues show prolonged p53 signaling after radiation, while more resistant tissues show transient p53 activation. Sustaining p53 using a small molecule (NMI801) that inhibits Mdm2, a negative regulator of p53, reduced viability in cell culture and suppressed tumor growth. Our work proposes a mechanism for the control of radiation sensitivity and suggests tools to alter the dynamics of p53 to enhance tumor clearance. Similar approaches can be used to enhance killing of cancer cells or reduce toxicity in normal tissues following genotoxic therapies.
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