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1 November 2001 Identification of KIN (KIN17), a Human Gene Encoding a Nuclear DNA-Binding Protein, as a Novel Component of the TP53-Independent Response to Ionizing Radiation
Christel Masson, Farid Menaa, Ghislaine Pinon-Lataillade, Yveline Frobert, J. Pablo Radicella, Jaime F. Angulo
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Abstract

Masson, C., Menaa, F., Pinon-Lataillade, G., Frobert, Y., Radicella, J. P. and Angulo, J. F. Identification of KIN (KIN17), a Human Gene Encoding a Nuclear DNA-Binding Protein, as a Novel Component of the TP53-Independent Response to Ionizing Radiation. Radiat. Res. 156, 535–544 (2001).

Ionizing radiation elicits a genetic response in human cells that allows cell survival. The human KIN (also known as KIN17) gene encodes a 45-kDa nuclear DNA-binding protein that participates in the response to UVC radiation and is immunologically related to the bacterial RecA protein. We report for the first time that ionizing radiation and bleomycin, a radiomimetic drug, which produce single- and double-strand breaks, increased expression of KIN in human cells established from tumors, including MeWo melanoma, MCF7 breast adenocarcinoma, and ATM( )GM3657 lymphoblast cells. KIN expression increased rapidly in a dose-dependent manner after irradiation. Under the same conditions, several genes controlled by TP53 were induced with kinetics similar to that of KIN. Using the CDKN1A gene as a marker of TP53 responsiveness, we analyzed the up-regulation of KIN and showed that is independent of the status of TP53 and ATM. In contrast, the presence of a dominant mutant for activating transcription factor 2 (ATF2) completely abolished the up-regulation of KIN. Our results suggest a role for ATF2 in the TP53-independent increase in KIN expression after γ irradiation.

Christel Masson, Farid Menaa, Ghislaine Pinon-Lataillade, Yveline Frobert, J. Pablo Radicella, and Jaime F. Angulo "Identification of KIN (KIN17), a Human Gene Encoding a Nuclear DNA-Binding Protein, as a Novel Component of the TP53-Independent Response to Ionizing Radiation," Radiation Research 156(5), 535-544, (1 November 2001). https://doi.org/10.1667/0033-7587(2001)156[0535:IOKKAH]2.0.CO;2
Received: 27 April 2001; Accepted: 1 June 2001; Published: 1 November 2001
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