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Abnormal centrosomal structure and duplication in Cep135-deficient vertebrate cells

Authors :
Burcu Inanç
Peter Dockery
Fanni Gergely
Pierce Lalor
Monika Pütz
Ryoko Kuriyama
Ciaran G. Morrison
Source :
Molecular Biology of the Cell
Publication Year :
2013
Publisher :
The American Society for Cell Biology, 2013.

Abstract

Gene targeting was used to ablate Cep135, a component of the centriolar cartwheel, in chicken DT40 cells. Cep135-deficient cells showed no major defects in centrosome composition or function, although centrosome amplification after HU treatment increased significantly. EM revealed an unusual structure in the lumen of Cep135-null centrioles.<br />Centrosomes are key microtubule-organizing centers that contain a pair of centrioles, conserved cylindrical, microtubule-based structures. Centrosome duplication occurs once per cell cycle and relies on templated centriole assembly. In many animal cells this process starts with the formation of a radially symmetrical cartwheel structure. The centrosomal protein Cep135 localizes to this cartwheel, but its role in vertebrates is not well understood. Here we examine the involvement of Cep135 in centriole function by disrupting the Cep135 gene in the DT40 chicken B-cell line. DT40 cells that lack Cep135 are viable and show no major defects in centrosome composition or function, although we note a small decrease in centriole numbers and a concomitant increase in the frequency of monopolar spindles. Furthermore, electron microscopy reveals an atypical structure in the lumen of Cep135-deficient centrioles. Centrosome amplification after hydroxyurea treatment increases significantly in Cep135-deficient cells, suggesting an inhibitory role for the protein in centrosome reduplication during S-phase delay. We propose that Cep135 is required for the structural integrity of centrioles in proliferating vertebrate cells, a role that also limits centrosome amplification in S-phase–arrested cells.

Details

Language :
English
ISSN :
19394586 and 10591524
Volume :
24
Issue :
17
Database :
OpenAIRE
Journal :
Molecular Biology of the Cell
Accession number :
edsair.doi.dedup.....eba0eedfe0b8a5e092d58c750c58a4ed