AI Article Synopsis
- Centrosome biogenesis is crucial for proper cell division and maintaining genetic stability, with a key focus on the assembly of pericentriolar material (PCM) around centrioles.
- Research shows that tubulin interacts with the centrosomal protein Sas-4, where this binding negatively regulates the recruitment of PCM, impacting centrosome size and activity.
- The influence of tubulin on PCM recruitment is determined by its guanine nucleotide state: tubulin-GTP inhibits complex formation, while tubulin-GDP promotes it, demonstrating a dual role for tubulin beyond its general function as a microtubule component.
Article Abstract
Regulated centrosome biogenesis is required for accurate cell division and for maintaining genome integrity. Centrosomes consist of a centriole pair surrounded by a protein network known as pericentriolar material (PCM). PCM assembly is a tightly regulated, critical step that determines the size and capability of centrosomes. Here, we report a role for tubulin in regulating PCM recruitment through the conserved centrosomal protein Sas-4. Tubulin directly binds to Sas-4; together they are components of cytoplasmic complexes of centrosomal proteins. A Sas-4 mutant, which cannot bind tubulin, enhances centrosomal protein complex formation and has abnormally large centrosomes with excessive activity. These results suggest that tubulin negatively regulates PCM recruitment. Whereas tubulin-GTP prevents Sas-4 from forming protein complexes, tubulin-GDP promotes it. Thus, the regulation of PCM recruitment by tubulin depends on its GTP/GDP-bound state. These results identify a role for tubulin in regulating PCM recruitment independent of its well-known role as a building block of microtubules. On the basis of its guanine-bound state, tubulin can act as a molecular switch in PCM recruitment.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3411905 | PMC |
| http://dx.doi.org/10.1038/ncb2527 | DOI Listing |
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