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  The Caenorhabditis elegans pericentriolar material components SPD-2 and SPD-5 are monomeric in the cytoplasm before incorporation into the PCM matrix.

Wueseke, O., Bunkenborg, J., Hein, M. Y., Zinke, A., Viscardi, V., Woodruff, J., et al. (2014). The Caenorhabditis elegans pericentriolar material components SPD-2 and SPD-5 are monomeric in the cytoplasm before incorporation into the PCM matrix. Molecular Biology of the Cell, 25(19), 2984-2992.

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 Creators:
Wueseke, Oliver1, Author           
Bunkenborg, Jakob, Author
Hein, Marco Y, Author
Zinke, Andrea1, Author           
Viscardi, Valeria, Author
Woodruff, Jeffrey1, Author           
Oegema, Karen1, Author           
Mann, Matthias, Author
Andersen, Jens S, Author
Hyman, Anthony1, Author           
Affiliations:
1Max Planck Institute of Molecular Cell Biology and Genetics, Max Planck Society, ou_2340692              

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 Abstract: Centrosomes are the main microtubule-organizing centers in animal cells. Centrosomes consist of a pair of centrioles surrounded by a matrix of pericentriolar material (PCM) that assembles from cytoplasmic components. In Caenorhabditis elegans embryos, interactions between the coiled-coil proteins SPD-5 and SPD-2 and the kinase PLK-1 are critical for PCM assembly. However, it is not known whether these interactions promote the formation of cytoplasmic complexes that are added to the PCM or whether the components interact only during incorporation into the PCM matrix. Here we address this problem by using a combination of live-cell fluorescence correlation spectroscopy, mass spectrometry, and hydrodynamic techniques to investigate the native state of PCM components in the cytoplasm. We show that SPD-2 is monomeric, and neither SPD-2 nor SPD-5 exists in complex with PLK-1. SPD-5 exists mostly as a monomer but also forms complexes with the PP2A-regulatory proteins RSA-1 and RSA-2, which are required for microtubule organization at centrosomes. These results suggest that the interactions between SPD-2, SPD-5, and PLK-1 do not result in formation of cytoplasmic complexes, but instead occur in the context of PCM assembly.

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 Dates: 2014
 Publication Status: Issued
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 Identifiers: eDoc: 705702
Other: 5869
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Title: Molecular Biology of the Cell
Source Genre: Journal
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Pages: - Volume / Issue: 25 (19) Sequence Number: - Start / End Page: 2984 - 2992 Identifier: -