International Journal of Molecular Sciences (Mar 2019)

Crystal Structure of the Cyclostreptin-Tubulin Adduct: Implications for Tubulin Activation by Taxane-Site Ligands

  • Francisco de Asís Balaguer,
  • Tobias Mühlethaler,
  • Juan Estévez-Gallego,
  • Enrique Calvo,
  • Juan Francisco Giménez-Abián,
  • April L. Risinger,
  • Erik J. Sorensen,
  • Christopher D. Vanderwal,
  • Karl-Heinz Altmann,
  • Susan L. Mooberry,
  • Michel O. Steinmetz,
  • María Ángela Oliva,
  • Andrea E. Prota,
  • J. Fernando Díaz

DOI
https://doi.org/10.3390/ijms20061392
Journal volume & issue
Vol. 20, no. 6
p. 1392

Abstract

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It has been proposed that one of the mechanisms of taxane-site ligand-mediated tubulin activation is modulation of the structure of a switch element (the M-loop) from a disordered form in dimeric tubulin to a folded helical structure in microtubules. Here, we used covalent taxane-site ligands, including cyclostreptin, to gain further insight into this mechanism. The crystal structure of cyclostreptin-bound tubulin reveals covalent binding to βHis229, but no stabilization of the M-loop. The capacity of cyclostreptin to induce microtubule assembly compared to other covalent taxane-site agents demonstrates that the induction of tubulin assembly is not strictly dependent on M-loop stabilization. We further demonstrate that most covalent taxane-site ligands are able to partially overcome drug resistance mediated by βIII-tubulin (βIII) overexpression in HeLa cells, and compare their activities to pironetin, an interfacial covalent inhibitor of tubulin assembly that displays invariant growth inhibition in these cells. Our findings suggest a relationship between a diminished interaction of taxane-site ligands with βIII-tubulin and βIII tubulin-mediated drug resistance. This supports the idea that overexpression of βIII increases microtubule dynamicity by counteracting the enhanced microtubule stability promoted by covalent taxane-site binding ligands.

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