Trimerisation is important for the function of clathrin at the mitotic spindle

doi:10.1242/jcs.03192

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First published online 12 September 2006
doi: 10.1242/jcs.03192

Journal of Cell Science 119, 4071-4078 (2006)
Published by The Company of Biologists 2006

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Research Article

Trimerisation is important for the function of clathrin at the mitotic spindle

Stephen J. Royle^*^, and Leon Lagnado

MRC Laboratory of Molecular Biology, Hills Road, Cambridge, CB2 2QH, UK

^* Author for correspondence (e-mail: S.J.Royle{at}liverpool.ac.uk)

Accepted 21 July 2006

Clathrin is a triskelion consisting of three heavy chains eachwith an associated light chain. During mitosis, clathrin contributesto kinetochore fibre stability. As the N-terminal domain atthe foot of each leg can bind to the mitotic spindle, we proposedpreviously a `bridge hypothesis' wherein clathrin acts as abrace between two or three microtubules within a kinetochorefibre to increase fibre stability. Here, we have tested thishypothesis by replacing endogenous clathrin heavy chain in humancells with a panel of clathrin constructs. Mutants designedto abolish trimerisation were unable to rescue the mitotic defectscaused by depletion of endogenous clathrin. By contrast, stuntedtriskelia with contracted legs could partially rescue normalmitosis. These results indicate that the key structural featuresof clathrin that are necessary for its function in mitosis area trimeric molecule with a spindle interaction domain at eachend, supporting the bridge hypothesis for clathrin functionin mitosis.

Key words: Clathrin, Mitosis, Endocytosis, RNAi

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