Interaction interface in the C-terminal parts of centriole proteins Sas6 and Ana2
Abstract
The centriole is a ninefold symmetrical structure found at the core of centrosomes and, as a basal body, at the base of cilia, whose conserved duplication is regulated by Plk4 kinase. Plk4 phosphorylates a single serine residue at the N-terminus of Ana2 to promote Ana2's loading to the site of procentriole formation. Four conserved serines in Ana2's STAN motif are then phosphorylated by Plk4, enabling Sas6 recruitment. Crystallographic data indicate that the coiled–coil domain of Ana2 forms a tetramer but the structure of full-length Ana2 has not been solved. Here, we have employed hydrogen–deuterium exchange coupled with mass spectrometry (HDX-MS) to uncover the conformational dynamics of Ana2, revealing the high flexibility of this protein with one rigid region. To determine the elusive nature of the interaction surfaces between Ana2 and Sas6, we have confirmed complex formation between the phosphomimetic form of Ana2 (Ana2-4D) and Sas6 in vitro and in vivo. Analysis of this complex by HDX-MS identifies short critical regions required for this interaction, which lie in the C-terminal parts of both proteins. Mutational studies confirmed the relevance of these regions for the Ana2–Sas6 interaction. The Sas6 site required for Ana2 binding is distinct from the site required for Sas6 to bind Gorab and Sas6 is able to bind both these protein partners simultaneously.
Additional Information
© 2020 The Authors. Published by the Royal Society under the terms of the Creative Commons Attribution License http://creativecommons.org/licenses/by/4.0/, which permits unrestricted use, provided the original author and source are credited. Manuscript received 20/07/2020; Manuscript accepted 20/10/2020; Published online 11/11/2020. We would like to thank all members of the Glover and Dadlez labs, especially to Krzysztof Tarnowski, for their insightful comments and discussions. D.M.G. wishes to thank the Wellcome Trust for supporting the work of A.F., and Caltech for personal support. Data accessibility: The raw data are available from the authors. Authors' contributions: A.F. designed and carried out experiments, collected and analysed data. N.S.D. designed and carried out the Co-IP experiment. M.D. and D.M.G. supervised the work and raised grant funding. A.F., N.S.D. and D.M.G. wrote the manuscript. The authors declare that they have no competing interests. A.F. and M.D. were funded in part by National Science Centre MAESTRO project (UMO-2014/14/A/NZ1/00306), while the instruments were funded in part by Centre of Preclinical Research and Technology (POIG.02.02.00-14-024/08-00) and Foundation of Polish Science TEAM-Tech Core Facility (TEAM TECH CORE FACILITY/2016-2/2) grants.Attached Files
Published - rsob.200221.pdf
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Additional details
- PMCID
- PMC7729032
- Eprint ID
- 106608
- Resolver ID
- CaltechAUTHORS:20201111-084020109
- Wellcome Trust
- UMO-2014/14/A/NZ1/00306
- National Science Centre (Poland)
- POIG.02.02.00-14-024/08-00
- Centre of Preclinical Research and Technology
- 2016-2/2
- Foundation of Polish Science
- Created
-
2020-11-11Created from EPrint's datestamp field
- Updated
-
2021-11-16Created from EPrint's last_modified field
- Caltech groups
- Division of Biology and Biological Engineering