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  Securin Is Not Required for Chromosomal Stability in Human Cells

Pfleghaar, K., Heubes, S., Cox, J., Stemmann, O., & Speicher, M. R. (2005). Securin Is Not Required for Chromosomal Stability in Human Cells. PLoS Biology, 3(12): e416. doi:10.1371/journal.pbio.0030416.

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PLoS_Biol_3(12)_e416.pdf (beliebiger Volltext), 3MB
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© 2005 Pfleghaar et al. This is an open-access article distributed under the terms of the Creative Commons Attr
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 Urheber:
Pfleghaar, Katrin, Autor
Heubes, Simone1, Autor           
Cox, Jürgen2, Autor           
Stemmann, Olaf3, Autor           
Speicher, Michael R., Autor
Affiliations:
1Jentsch, Stefan / Molecular Cell Biology, Max Planck Institute of Biochemistry, Max Planck Society, ou_1565156              
2External Organizations, ou_persistent22              
3Former Research Groups, Max Planck Institute of Biochemistry, Max Planck Society, ou_1565145              

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 Zusammenfassung: Abnormalities of chromosome number are frequently observed in cancers. The mechanisms regulating chromosome segregation in human cells are therefore of great interest. Recently it has been reported that human cells without an hSecurin gene lose chromosomes at a high frequency. Here we show that, after hSecurin knockout through homologous recombination, chromosome losses are only a short, transient effect. After a few passages hSecurin−/− cells became chromosomally stable and executed mitoses normally. This was unexpected, as the securin loss resulted in a persisting reduction of the sister-separating protease separase and inefficient cleavage of the cohesin subunit Scc1. Our data demonstrate that securin is dispensable for chromosomal stability in human cells. We propose that human cells possess efficient mechanisms to compensate for the loss of genes involved in chromosome segregation.

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Sprache(n): eng - English
 Datum: 2005
 Publikationsstatus: Online veröffentlicht
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 Art der Begutachtung: Expertenbegutachtung
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Titel: PLoS Biology
Genre der Quelle: Zeitschrift
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Seiten: - Band / Heft: 3 (12) Artikelnummer: e416 Start- / Endseite: - Identifikator: -