| Literature DB >> 35787744 |
Fangrui Chen1, Jingchao Wu1, Malina K Iwanski1, Daphne Jurriens1, Arianna Sandron1, Milena Pasolli1, Gianmarco Puma1, Jannes Z Kromhout1, Chao Yang1, Wilco Nijenhuis1,2, Lukas C Kapitein1,2, Florian Berger1, Anna Akhmanova1.
Abstract
The major microtubule-organizing center (MTOC) in animal cells, the centrosome, comprises a pair of centrioles surrounded by pericentriolar material (PCM), which nucleates and anchors microtubules. Centrosome assembly depends on PCM binding to centrioles, PCM self-association and dynein-mediated PCM transport, but the self-assembly properties of PCM components in interphase cells are poorly understood. Here, we used experiments and modeling to study centriole-independent features of interphase PCM assembly. We showed that when centrioles are lost due to PLK4 depletion or inhibition, dynein-based transport and self-clustering of PCM proteins are sufficient to form a single compact MTOC, which generates a dense radial microtubule array. Interphase self-assembly of PCM components depends on γ-tubulin, pericentrin, CDK5RAP2 and ninein, but not NEDD1, CEP152, or CEP192. Formation of a compact acentriolar MTOC is inhibited by AKAP450-dependent PCM recruitment to the Golgi or by randomly organized CAMSAP2-stabilized microtubules, which keep PCM mobile and prevent its coalescence. Linking of CAMSAP2 to a minus-end-directed motor leads to the formation of an MTOC, but MTOC compaction requires cooperation with pericentrin-containing self-clustering PCM. Our data reveal that interphase PCM contains a set of components that can self-assemble into a compact structure and organize microtubules, but PCM self-organization is sensitive to motor- and microtubule-based rearrangement.Entities:
Keywords: CAMSAP; PLK4; cell biology; centrosome; dynein; human; microtubule; microtubule-organizing center; pericentrin; pericentriolar material
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Year: 2022 PMID: 35787744 PMCID: PMC9307276 DOI: 10.7554/eLife.77892
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.713