Modular assembly of the principal microtubule nucleator γ-TuRC

Würtz, Martin; Župa, Erik; Atorino, Enrico; Neuner, Annett; Böhler, Anna; Rahadian, Ariani S; Vermeulen, Bram J. A.; Tonon, Giulia; Eustermann, Sebastian; Schiebel, Elmar; Pfeffer, Stefan

doi:10.1038/s41467-022-28079-0

Cited by 26 publications

(48 citation statements)

References 55 publications

(91 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…1b). This fits with the fact that γ-TuRCs derived from cells where all GCP3 subunits bear a GFP tag would be expected to contain five GCP3-GFP subunits 18–21, 24 .…”

Section: Resultssupporting

confidence: 69%

“…This finding raises the possibility that γ-TuRCnucleated microtubules may not be fully attached to their template, and some protofilaments might have a flared conformation that would permit CAMSAP binding. Furthermore, since the microtubulenucleating activity of purified γ-TuRC turned out to be quite low 18,22 , a potential mechanism of stimulating nucleation would be to alter γ-TuRC conformation to make it more similar to the microtubule structure 6,7,23,24 . To explore these possibilities, we have set up in vitro reconstitution assays and confirmed that purified γ-TuRC has by itself a rather low activity that can be enhanced by nucleation-promoting factors, microtubule polymerase chTOG, and γ-TuRC associated protein CDK5RAP2 [25][26][27] .…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

CAMSAP-driven microtubule release from γ-TuRC and its regulation by nucleation-promoting factors

Rai

Hua

Monster

et al. 2022

Preprint

View full text Add to dashboard Cite

Abstractγ-tubulin ring complex (γ-TuRC) is the major microtubule-nucleating factor. After nucleation, microtubules can be released from γ-TuRC and stabilized by other proteins, such as CAMSAPs, but the biochemical cross-talk between minus-end regulation pathways is poorly understood. Here, we reconstituted this process in vitro using purified components. We found that all CAMSAP proteins could bind to the minus-ends of γ-TuRC-attached microtubules. CAMSAP2 and CAMSAP3, which decorate and stabilize growing minus ends, but not the minus-end tracking protein CAMSAP1 induced microtubule release from γ-TuRC. CDK5RAP2, a γ-TuRC-interactor, and CLASP2, a regulator of microtubule growth, stimulated γ-TuRC-dependent microtubule nucleation, but only CDK5RAP2 inhibited CAMSAP-driven microtubule detachment by suppressing CAMSAP binding to γ-TuRC-anchored minus ends. CDK5RAP2 also improved γ-TuRC selectivity for 13-rather than 14-protofilament microtubules in microtubule-capping assays. Our results support a model whereby CAMSAPs exploit an imperfect attachment between γ-TuRC and the nucleated microtubule to promote minus-end elongation and release, whereas CDK5RAP2 improves the fit between γ-TuRC and 13-protofilament microtubules and enhances nucleation.

show abstract

“…1b). This fits with the fact that γ-TuRCs derived from cells where all GCP3 subunits bear a GFP tag would be expected to contain five GCP3-GFP subunits 18–21, 24 .…”

Section: Resultssupporting

confidence: 69%

Section: Introductionmentioning

confidence: 99%

CAMSAP-driven microtubule release from γ-TuRC and its regulation by nucleation-promoting factors

Rai

Hua

Monster

et al. 2022

Preprint

View full text Add to dashboard Cite

show abstract

“…Cloning of the MultiBac TM (GENEVA Biotech) constructs, all with polH expression cassettes, was done as described previously 50 , 51 , tagging individual proteins inspired by 24 . Genes of the X. laevis augmin TII and TIII complexes (HAUS1 (XM_018267162.1), HAUS2 (NP_001085195.1), HAUS3 (XM_018226568.1), HAUS4 (NM_001096090.1), HAUS5 (XM_018226568.1), HAUS6 (NM_001097095.1), and HAUS7 (NP_001121229.1)) were purchased (Integrated DNA Technologies IDT, USA) optimised for insect cell expression.…”

Section: Methodsmentioning

confidence: 99%

The augmin complex architecture reveals structural insights into microtubule branching

et al. 2022

Self Cite

View full text Add to dashboard Cite

In mitosis, the augmin complex binds to spindle microtubules to recruit the γ-tubulin ring complex (γ-TuRC), the principal microtubule nucleator, for the formation of branched microtubules. Our understanding of augmin-mediated microtubule branching is hampered by the lack of structural information on the augmin complex. Here, we elucidate the molecular architecture and conformational plasticity of the augmin complex using an integrative structural biology approach. The elongated structure of the augmin complex is characterised by extensive coiled-coil segments and comprises two structural elements with distinct but complementary functions in γ-TuRC and microtubule binding, linked by a flexible hinge. The augmin complex is recruited to microtubules via a composite microtubule binding site comprising a positively charged unordered extension and two calponin homology domains. Our study provides the structural basis for augmin function in branched microtubule formation, decisively fostering our understanding of spindle formation in mitosis.

show abstract

“…The assembly of γ-TuRC is modular, starting with the formation of a stable subcomplex of six spokes, consisting of GCP2-3-4-5-4-6, which then expands with the addition of four preformed GCP2-3 units (γ-TuSC), MZT1, and actin (Würtz et al, 2022). DNAseI binds directly to actin with high affinity.…”

Section: Figurementioning

confidence: 99%

“…The in vitro nucleation activity of isolated endogenous γ-TuRC was markedly inhibited after treatment with DNAseI, and saturation of DNAseI with actin abolished this inhibition, suggesting a functional importance of actin in the complex (Liu et al, 2020). Actin has been shown not to be required for assembly of γ-TuRC, but to determine the geometry of the complex and ensure effective nucleation of microtubules (Würtz et al, 2022). On the outer surface of reconstituted γ- (Zupa et al, 2021).…”

Section: Figurementioning

confidence: 99%

γ-Tubulin in microtubule nucleation and beyond

Sulimenko

Dráberová

2022

Front. Cell Dev. Biol.

View full text Add to dashboard Cite

Microtubules composed of αβ-tubulin dimers are dynamic cytoskeletal polymers that play key roles in essential cellular processes such as cell division, organelle positioning, intracellular transport, and cell migration. γ-Tubulin is a highly conserved member of the tubulin family that is required for microtubule nucleation. γ-Tubulin, together with its associated proteins, forms the γ-tubulin ring complex (γ-TuRC), that templates microtubules. Here we review recent advances in the structure of γ-TuRC, its activation, and centrosomal recruitment. This provides new mechanistic insights into the molecular mechanism of microtubule nucleation. Accumulating data suggest that γ-tubulin also has other, less well understood functions. We discuss emerging evidence that γ-tubulin can form oligomers and filaments, has specific nuclear functions, and might be involved in centrosomal cross-talk between microtubules and microfilaments.

show abstract

Modular assembly of the principal microtubule nucleator γ-TuRC

Cited by 26 publications

References 55 publications

CAMSAP-driven microtubule release from γ-TuRC and its regulation by nucleation-promoting factors

CAMSAP-driven microtubule release from γ-TuRC and its regulation by nucleation-promoting factors

The augmin complex architecture reveals structural insights into microtubule branching

γ-Tubulin in microtubule nucleation and beyond

Contact Info

Product

Resources

About