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Journal ArticleDOI

In vitro effect of cryptophycin 52 on microtubule assembly and tubulin: molecular modeling of the mechanism of action of a new antimitotic drug.

TLDR
This report details the mechanism by which C52 substoichiometrically inhibits tubulin self-assembly into microtubules and shows that C52 induces tubulin to form ring-shaped oligomers (single rings) and inhibits the formation of double rings from either GTP- or GDP-tubulin.
Abstract
Cryptophycin 52 (C52) is a new synthetic compound of the cryptophycin family of antitumor agents that is currently undergoing clinical evaluation for cancer chemotherapy. The cryptophycin class of compounds acts on microtubules. This report details the mechanism by which C52 substoichiometrically inhibits tubulin self-assembly into microtubules. The inhibition data were analyzed through a model described by Perez-Ramirez [Perez-Ramirez, B., Andreu, J. M., Gorbunoff, M. J., and Timasheff, S. N. (1996) Biochemistry 35, 3277-3285]. We thereby determined the values of the apparent binding constant of the tubulin-C52 complex to the end of a growing microtubule (K(i)) and the apparent binding constant of C52 to tubulin (K(b)). The binding of C52 depended on tubulin concentration, and binding induced changes in the sedimentation pattern of tubulin, which indicates that C52 induces the self-association of tubulin and tubulin aggregates other than microtubules. Using analytical ultracentrifugation and electron microscopy, we show that C52 induces tubulin to form ring-shaped oligomers (single rings). We also show that C52 inhibits the formation of double rings from either GTP- or GDP-tubulin. In addition, the advances made by electron crystallography in understanding the structure of the tubulin and the microtubule allowed us to visualize the putative binding site of C52 and to reconstruct C52-induced ring oligomers by molecular modeling.

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Citations
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Journal ArticleDOI

On the analysis of protein self-association by sedimentation velocity analytical ultracentrifugation.

TL;DR: New tools for the analysis of protein self-association by sedimentation velocity are developed, their statistical properties are examined, and considerations for optimal experimental design are discussed.
Journal ArticleDOI

Tubulin Is an Inherent Component of Mitochondrial Membranes That Interacts with the Voltage-dependent Anion Channel

TL;DR: It is shown by immunoprecipitation experiments that the mitochondrial tubulin is specifically associated with the voltage-dependent anion channel, the main component of the permeability transition pore, and it could play a role in apoptosis via interaction with the permeable Transition pore.
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Antiangiogenic concentrations of paclitaxel induce an increase in microtubule dynamics in endothelial cells but not in cancer cells.

TL;DR: Results show that paclitaxel mediates antiangiogenesis by an increase in microtubule dynamics in living endothelial cells and suggest that the impairment of interphase microtubules functions is responsible for the inhibition of angiogenesis.
Journal ArticleDOI

Stathmin and interfacial microtubule inhibitors recognize a naturally curved conformation of tubulin dimers.

TL;DR: Analytical ultracentrifugation and binding measurements show that tubulin-stathmin associations and binding of ligands are thermodynamically independent from one another, irrespective of tubulin being bound to GTP or GDP.
References
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Journal ArticleDOI

High-resolution model of the microtubule.

TL;DR: A high-resolution model of the microtubule has been obtained by docking the crystal structure of tubulin into a 20 A map of themicrotubule, and the excellent fit indicates the similarity of the tubulin conformation in both polymers and defines the orientation of the Tubulin structure within the micro Tubule.
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Pharmaceuticals from cultured algae

TL;DR: Screening of these groups for biologically active components has lead to the isolation of pachydictyol and caulerpenyne from cultured macroalgae, while a series of hapalindoles and an antifungal depsipeptide have been isolated from cyanobacteria.
Journal ArticleDOI

HYDRO: a computer program for the prediction of hydrodynamic properties of macromolecules

TL;DR: HYDRO is a program for the calculation of sedimentation and diffusion coefficients, rotational relaxation times, and intrinsic viscosities of rigid macromolecules of arbitrary shape that are represented by bead models.
Journal ArticleDOI

Total Synthesis of Cryptophycins. Revision of the Structures of Cryptophycins A and C

TL;DR: The convergent total synthesis of cryptophycins C and D is described, showing that in both natural products the absolute configuration of the a-amino acid corresponds to the D-series and correcting the structural assignment for cryptophycin C has been corrected.
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