2012 ASCB Annual Meeting abstracts
نویسندگان
چکیده
γ-Tubulin nucleates microtubules (MTs) in all eukaryotes and acts in complex with an array of related accessory proteins. It exists in at least two types of complexes inside cells: a ~300kDa γ-Tubulin Small Complex (γTuSC), which can assemble to form a ~2.2MDa γ-Tubulin Ring Complex (γTuRC). In vitro MT nucleation assays have shown that the γTuRC is a more potent nucleator than γTuSC. Interestingly, pure human γ-tubulin can form filaments in vitro that are also much more active than γTuSC. We have examined the structure-function relationship between the configuration of γ-tubulins in these complexes and their ability to nucleate MTs using high-resolution electron microscopic reconstructions of the complexes and in vitro MT nucleation assays. We find that complexes in which the γ-tubulins make lateral contacts like those made by αβ-tubulins in the MT wall are the best nucleators. Our finding that the γTuSC (Tub4 complex) of S. cerevisiae can assemble spontaneously into γTuRC-like rings with 13-fold symmetry, but without a precise MT-lattice-like arrangement of γ-tubulins, suggested a mode of regulation for γTuRC activity. The flexibility observed in one of the "arms" of the V-shaped γTuSC suggests that a conformational change is required to bring the γ-tubulins into an optimal position for achieving MT nucleation. We are exploring this possibility. We have also found that the S. cerevisiae γ-tubulin ring complexes show much greater activity with S. cerevisiae αβtubulin than with pig brain tubulin.
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2011 ASCB Annual Meeting abstracts
The abstracts of the 2011 American Society for Cell Biology (ASCB) Annual Meeting are attached to this article as searchable PDF files. To view the files, click on the Abstracts link in the content box in the middle column of the HTML version of this article. The ASCB and the Editor-in-Chief of Molecular Biology of the Cell (MBoC) decided to present the Annual Meeting abstracts in this manner s...
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