Overexpression of kin17 protein disrupts nuclear morphology and inhibits the growth of mammalian cells
Author:
Affiliation:
1. Laboratoire de Genetique de la Radiosensibilite, Departement de Radiobiologie et de Radiopathologie, Direction des Sciences du Vivant, Centre d'Etudes de Fontenay-aux-Roses, CEA, avenue du General-Leclerc, B.P. no. 6, France.
Abstract
Publisher
The Company of Biologists
Subject
Cell Biology
Link
http://journals.biologists.com/jcs/article-pdf/112/19/3215/1353912/3215.pdf
Reference34 articles.
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2. Enhanced expression of the kin17 protein immediately after low doses of ionizing radiation.;Biard;Rad. Res,1997
3. Ectopic expression of (Mm)Kin17 protein inhibits cell proliferation of human tumor-derived cells.;Biard;Exp. Cell Res,1999
4. Further characterisation of the p53 responsive element—identification of new candidate genes for trans-activation by p53.;Bourdon;Oncogene,1997
5. Mouse p53 inhibits SV40 origin-dependent DNA replication.;Braithwaite;Nature,1987
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1. A genetic screen in C. elegans reveals roles for KIN17 and PRCC in maintaining 5’ splice site identity;PLOS Genetics;2022-02-10
2. 1H, 15N, and 13C resonance assignments of the SH3-like tandem domain of human KIN protein;Biomolecular NMR Assignments;2021-08-20
3. A Tandem of SH3-like Domains Participates in RNA Binding in KIN17, a Human Protein Activated in Response to Genotoxics;Journal of Molecular Biology;2006-12
4. Poly(ethylene oxide) facilitates the characterization of an affinity between strongly basic proteins with DNA by affinity capillary electrophoresis;ELECTROPHORESIS;2005-08
5. The Human Stress-Activated Protein kin17 Belongs to the Multiprotein DNA Replication Complex and Associates In Vivo with Mammalian Replication Origins;Molecular and Cellular Biology;2005-05
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