Characterization of Two Related Drosophila γ-tubulin Complexes that Differ in Their Ability to Nucleate Microtubules

Author:

Oegema Karen1,Wiese Christiane1,Martin Ona C.1,Milligan Ronald A.1,Iwamatsu Akihiro1,Mitchison Timothy J.1,Zheng Yixian1

Affiliation:

1. Department of Cell Biology, Harvard Medical School, Boston, Massachusetts 02115; Department of Embryology, Carnegie Institute of Washington, Baltimore, Maryland 21210; Department of Cell Biology, The Scripps Research Institute, La Jolla, California 92037; and Central Laboratories for Key Technology, Kirin Brewery Company, Ltd., Yokohama 236, Japan

Abstract

γ-tubulin exists in two related complexes in Drosophila embryo extracts (Moritz, M., Y. Zheng, B.M. Alberts, and K. Oegema. 1998. J. Cell Biol. 142:1– 12). Here, we report the purification and characterization of both complexes that we name γ-tubulin small complex (γTuSC; ∼280,000 D) and Drosophila γTuRC (∼2,200,000 D). In addition to γ-tubulin, the γTuSC contains Dgrip84 and Dgrip91, two proteins homologous to the Spc97/98p protein family. The γTuSC is a structural subunit of the γTuRC, a larger complex containing about six additional polypeptides. Like the γTuRC isolated from Xenopus egg extracts (Zheng, Y., M.L. Wong, B. Alberts, and T. Mitchison. 1995. Nature. 378:578–583), the Drosophila γTuRC can nucleate microtubules in vitro and has an open ring structure with a diameter of 25 nm. Cryo-electron microscopy reveals a modular structure with ∼13 radially arranged structural repeats. The γTuSC also nucleates microtubules, but much less efficiently than the γTuRC, suggesting that assembly into a larger complex enhances nucleating activity. Analysis of the nucleotide content of the γTuSC reveals that γ-tubulin binds preferentially to GDP over GTP, rendering γ-tubulin an unusual member of the tubulin superfamily.

Publisher

Rockefeller University Press

Subject

Cell Biology

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