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  Proliferating versus differentiating stem and cancer cells exhibit distinct midbody-release behaviour.

Ettinger, A., Wilsch-Bräuninger, M., Marzesco, A.-M., Bickle, M., Lohmann, A., Maliga, Z., et al. (2011). Proliferating versus differentiating stem and cancer cells exhibit distinct midbody-release behaviour. Nature Communications, 2: 503.

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 Creators:
Ettinger, Andreas1, Author           
Wilsch-Bräuninger, Michaela1, Author           
Marzesco, Anne-Marie1, Author           
Bickle, Marc1, Author           
Lohmann, Annett1, Author           
Maliga, Zoltan1, Author           
Karbanová, Jana, Author
Corbeil, Denis1, Author           
Hyman, Anthony A.1, Author           
Huttner, Wieland B.1, Author           
Affiliations:
1Max Planck Institute of Molecular Cell Biology and Genetics, Max Planck Society, ou_2340692              

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 Abstract: The central portion of the midbody, a cytoplasmic bridge between nascent daughter cells at the end of cell division, has generally been thought to be retained by one of the daughter cells, but has, recently, also been shown to be released into the extracellular space. The significance of midbody-retention versus -release is unknown. Here we show, by quantitatively analysing midbody-fate in various cell lines under different growth conditions, that the extent of midbody-release is significantly greater in stem cells than cancer-derived cells. Induction of cell differentiation is accompanied by an increase in midbody-release. Knockdown of the endosomal sorting complex required for transport family members, Alix and tumour-suppressor gene 101, or of their interaction partner, centrosomal protein 55, impairs midbody-release, suggesting mechanistic similarities to abscission. Cells with such impaired midbody-release exhibit enhanced responsiveness to a differentiation stimulus. Taken together, midbody-release emerges as a characteristic feature of cells capable of differentiation.

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 Dates: 2011
 Publication Status: Issued
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 Identifiers: eDoc: 585264
Other: 4616
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Title: Nature Communications
Source Genre: Journal
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Pages: - Volume / Issue: 2 Sequence Number: 503 Start / End Page: - Identifier: -