Cosolvent-induced transformation of a death domain tertiary structure

Authors

Tsan Xiao, The Howard Hughes Medical Institute and Department of Biochemistry, University of Texas Southwestern Medical Center, 5323 Harry Hines Boulevard, Dallas, TX 75390-9050, USA.
Kevin H. Gardner
Stephen R. SprangFollow

Document Type

Article

Publication Title

Proceedings of the National Academy of Sciences of the United States of America

Publication Date

8-20-2002

Volume

99

Issue

17

Disciplines

Biology | Life Sciences

Abstract

The death domain (DD) of the protein kinase Pelle adopts a six-helix bundle fold in the crystal structure of the complex with its dimerization partner, Tube-DD. However, in crystals obtained from a solution of 45% 2-methyl-2,4-pentanediol (MPD), the C-terminal half of Pelle-DD folds into a single helix, and the N-terminal half of the molecule is disordered. The helical segment forms an antiparallel dimer with the corresponding helix of a symmetry-related molecule, and together they form extensive lattice interactions similar in number, composition, and buried surface to those in the six-helix bundle of the native fold. Secondary structure analysis by heteronuclear nuclear magnetic resonance spectroscopy (NMR) demonstrates that Pelle-DD adopts a six-helix bundle fold in aqueous solution. The fold is perturbed by MPD, with the largest chemical shift changes in one helix and two loop regions that encompass the Tube-DD binding site. Pelle-DD is stable to urea denaturation with a folding free energy of 7.9 kcal/mol at 25 degrees C but is destabilized, with loss of urea binding sites, in the presence of MPD. The data are consistent with a cosolvent denaturation model in which MPD denatures the N terminus of Pelle-DD but induces the C terminus to form a more compact structure and aggregate. A similar perturbation in vivo might occur at the plasma membrane and could have consequences for Pelle-mediated regulation. Generally, crystallographers should be aware that high concentrations of MPD or related cosolvents can alter the tertiary structure of susceptible proteins.

DOI

10.1073/pnas.172188399

Rights

© 2002, The National Academy of Sciences.

Recommended Citation

Xiao, Tsan; Gardner, Kevin H.; and Sprang, Stephen R., "Cosolvent-induced transformation of a death domain tertiary structure" (2002). Biological Sciences Faculty Publications. 519.
https://scholarworks.umt.edu/biosci_pubs/519