Literature DB >> 33346730

Kinesin-4 KIF21B limits microtubule growth to allow rapid centrosome polarization in T cells.

Peter Jan Hooikaas1, Hugo Gj Damstra1, Oane J Gros1, Wilhelmina E van Riel1, Maud Martin1, Yesper Th Smits2, Jorg van Loosdregt2, Lukas C Kapitein1, Florian Berger1, Anna Akhmanova1.   

Abstract

When a T cell and an antigen-presenting cell form an immunological synapse, rapid dynein-driven translocation of the centrosome toward the contact site leads to reorganization of microtubules and associated organelles. Currently, little is known about how the regulation of microtubule dynamics contributes to this process. Here, we show that the knockout of KIF21B, a kinesin-4 linked to autoimmune disorders, causes microtubule overgrowth and perturbs centrosome translocation. KIF21B restricts microtubule length by inducing microtubule pausing typically followed by catastrophe. Catastrophe induction with vinblastine prevented microtubule overgrowth and was sufficient to rescue centrosome polarization in KIF21B-knockout cells. Biophysical simulations showed that a relatively small number of KIF21B molecules can restrict mirotubule length and promote an imbalance of dynein-mediated pulling forces that allows the centrosome to translocate past the nucleus. We conclude that proper control of microtubule length is important for allowing rapid remodeling of the cytoskeleton and efficient T cell polarization.
© 2020, Hooikaas et al.

Entities:  

Keywords:  cell biology; centrosome; computational biology; human; immunological synapse; kinesin; microtubule; modeling; polarization; systems biology

Mesh:

Substances:

Year:  2020        PMID: 33346730      PMCID: PMC7817182          DOI: 10.7554/eLife.62876

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.140


  84 in total

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