Self-assembly of pericentriolar material in interphase cells lacking centrioles
Chen, Fangrui; Wu, Jingchao; Iwanski, Malina K; Jurriens, Daphne; Sandron, Arianna; Pasolli, Milena; Puma, Gianmarco; Kromhout, Jannes Z; Yang, Chao; Nijenhuis, Wilco; Kapitein, Lukas C; Berger, Florian; Akhmanova, Anna
(2022) eLife, volume 11, pp. 1 - 47
(Article)
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
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poorly understood. Here, we used experiments and modeling to study centriole18 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 minus25 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.
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Keywords: Animals, Centrioles/metabolism, Centrosome/metabolism, Dyneins/metabolism, Interphase, Microtubules/metabolism, Human, PLK4, pericentrin, microtubule-organizing center, pericentriolar material, centrosome, dynein, microtubule, CAMSAP, General Biochemistry,Genetics and Molecular Biology, General Immunology and Microbiology, General Neuroscience
ISSN: 2050-084X
Publisher: eLife Sciences Publications
Note: Funding Information: We thank Lynne Cassimeris (Lehigh University, USA), Pierre Gönczy and Didier Trono (EPFL, Switzerland), Dr. Duane Compton (Geisel School of Medicine at Dartmouth, USA) and Dr. Laurence Pelletier (Lunenfeld-Tanenbaum Research Institute, Canada) for the gift of materials and Ilya Grigoriev and Eugene Katrukha (Biology Imaging Center, Utrecht University) for the help with imaging and image analysis. This work was supported by China Scholarship Council scholarships to Fangrui Chen, Jingchao Wu and Chao Yang, the Netherlands Organization for Scientific Research Spinoza prize to A.A, as well as the European Research Council Consolidator Grant 819219 to L.C.K. and the Eindhoven-Wageningen-Utrecht Alliance (www.ewuu.nl) that supports the Center for Living Technologies. Funding Information: We?thank?Lynne?Cassimeris?(Lehigh?University,?USA),?Pierre?Gönczy?and?Didier?Trono?(EPFL,? Switzerland),?Dr.?Duane?Compton?(Geisel?School?of?Medicine?at?Dartmouth,?USA)?and?Dr.?Laurence? Pelletier?(Lunenfeld‐Tanenbaum?Research?Institute,?Canada)?for?the?gift?of?materials?and?Ilya? Grigoriev?and?Eugene?Katrukha?(Biology?Imaging?Center,?Utrecht?University)?for?the?help?with? imaging?and?image?analysis.?This?work?was?supported?by?China?Scholarship?Council?scholarships?to? Fangrui?Chen,?Jingchao?Wu?and?Chao?Yang,?the?Netherlands?Organization?for?Scientific?Research? Spinoza?prize?to?A.A,?as?well?as?the?European?Research?Council?Consolidator?Grant?819219?to?L.C.K.? and?the?Eindhoven‐Wageningen‐Utrecht?Alliance?(www.ewuu.nl)?that?supports?the?Center?for?Living? Technologies.? Publisher Copyright: © 2022, eLife Sciences Publications Ltd. All rights reserved.
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