Drosophila Mgr, a Prefoldin subunit cooperating with von Hippel Lindau to regulate tubulin stability
Abstract
Mutations in Drosophila merry-go-round (mgr) have been known for over two decades to lead to circular mitotic figures and loss of meiotic spindle integrity. However, the identity of its gene product has remained undiscovered. We now show that mgr encodes the Prefoldin subunit counterpart of human von Hippel Lindau binding-protein 1. Depletion of Mgr from cultured cells also leads to formation of monopolar and abnormal spindles and centrosome loss. These phenotypes are associated with reductions of tubulin levels in both mgr flies and mgr RNAi-treated cultured cells. Moreover, mgr spindle defects can be phenocopied by depleting β-tubulin, suggesting Mgr function is required for tubulin stability. Instability of β-tubulin in the mgr larval brain is less pronounced than in either mgr testes or in cultured cells. However, expression of transgenic β-tubulin in the larval brain leads to increased tubulin instability, indicating that Prefoldin might only be required when tubulins are synthesized at high levels. Mgr interacts with Drosophila von Hippel Lindau protein (Vhl). Both proteins interact with unpolymerized tubulins, suggesting they cooperate in regulating tubulin functions. Accordingly, codepletion of Vhl with Mgr gives partial rescue of tubulin instability, monopolar spindle formation, and loss of centrosomes, leading us to propose a requirement for Vhl to promote degradation of incorrectly folded tubulin in the absence of functional Prefoldin. Thus, Vhl may play a pivotal role: promoting microtubule stabilization when tubulins are correctly folded by Prefoldin and tubulin destruction when they are not.
Additional Information
© 2012 National Academy of Sciences. Edited by Yixian Zheng, Carnegie Institution of Washington, Baltimore, MD, and accepted by the Editorial Board February 23, 2012 (received for review May 31, 2011) We thank Renate Renkawitz-Pohl for anti-β1- and -β2-tubulin antibodies and Matthew Savoian for the β1-tubulin construct; the E7-β-tubulin antibody was developed by Michael Klymkowsky and obtained from the Developmental Studies Hybridoma Bank developed under the auspices of the National Institute of Child Health and Human Development and maintained by the University of Iowa. We thank the Cancer Research Campaign and more recently Cancer Research United Kingdom for supporting this work. N. Delgehyr and U.W. contributed equally to this work. Author contributions: N. Delgehyr, U.W., D.M., C.G., and D.M.G. designed research; N. Delgehyr, U.W., H.R., X.P., G.M., N. Dzhindzhev, D.M., M.R., S.L., and G.C. performed research; N. Delgehyr, U.W., G.M., and N. Dzhindzhev contributed new reagents/analytic tools; N. Delgehyr, U.W., H.R., X.P., D.M., M.R., S.L., G.C., C.G., and D.M.G. analyzed data; and N. Delgehyr, C.G., and D.M.G. wrote the paper. The authors declare no conflict of interest. This article is a PNAS Direct Submission. Y.Z. is a guest editor invited by the Editorial Board. This article contains supporting information online at www.pnas.org/lookup/suppl/doi:10.1073/pnas.1108537109/-/DCSupplemental.Errata
Correction for Delgehyr et al., Drosophila Mgr, a Prefoldin subunit cooperating with von Hippel Lindau to regulate tubulin stability Proceedings of the National Academy of Sciences Nov 2016, 113 (48) E7867-E7868; DOI: 10.1073/pnas.1617441113Attached Files
Published - pnas.201108537.pdf
Supplemental Material - pnas.201108537SI.pdf
Erratum - E7867.full.pdf
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Additional details
- PMCID
- PMC3326472
- Eprint ID
- 104873
- Resolver ID
- CaltechAUTHORS:20200807-170354525
- Cancer Research Campaign
- Cancer Research UK
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2020-08-11Created from EPrint's datestamp field
- Updated
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2023-06-01Created from EPrint's last_modified field