Protein Engineering Design and Selection

This Article Full Text FREE Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Email this article to a friend Similar articles in this journal Similar articles in ISI Web of Science Similar articles in PubMed Alert me to new issues of the journal Add to My Personal Archive Download to citation manager Search for citing articles in: ISI Web of Science (23) Request Permissions Google Scholar Articles by Aachmann, F.L. Articles by Wimmer, R. Search for Related Content PubMed PubMed Citation Articles by Aachmann, F.L. Articles by Wimmer, R. Social Bookmarking          What's this?

Protein Engineering vol. 16 no. 12 pp. 905-912, 2003
© 2003 Oxford University Press

Structural background of cyclodextrin–protein interactions

F.L. Aachmann, D.E. Otzen, K.L. Larsen and R. Wimmer¹

Department of Life Sciences, Aalborg University, Sohngaardsholmsvej 49, DK-9000 Aalborg, Denmark

¹ To whom correspondence should be addressed. e-mail: rw{at}bio.auc.dk

Cyclodextrins are cyclic oligosaccharides with the shape of a hollow truncated cone. Their exterior is hydrophilic and their cavity is hydrophobic, which gives cyclodextrins the ability to accommodate hydrophobic molecules/moieties in the cavity. This special molecular arrangement accounts for the variety of beneficial effects cyclodextrins have on proteins, which is widely used in pharmacological applications. We have studied the interaction between ß-cyclodextrin and four non-carbohydrate-binding model proteins: ubiquitin, chymotrypsin inhibitor 2 (CI2), S6 and insulin SerB9Asp by NMR spectroscopy at varying structural detail. We demonstrate that the interaction of ß-cyclodextrin and our model proteins takes place at specific sites on the protein surface, and that solvent accessibility of those sites is a necessary but not compelling condition for the occurrence of an interaction. If this behaviour can be generalized, it might explain the wide range of different effects of cyclodextrins on different proteins: aggregation suppression (if residues responsible for aggregation are highly solvent accessible), protection against degradation (if point of attack of a protease is sterically ‘masked’ by cyclodextrin), alteration of function (if residues involved in function are ‘masked’ by cyclodextrin). The exact effect of cyclodextrins on a given protein will always be related to the particular structure of this protein.

Received May 30, 2003; revised October 27, 2003; accepted October 30, 2003

CiteULike    Connotea    Del.icio.us    What's this?

This article has been cited by other articles:

				M. A. Churchward, T. Rogasevskaia, J. Hofgen, J. Bau, and J. R. Coorssen Cholesterol facilitates the native mechanism of Ca2+-triggered membrane fusion J. Cell Sci., October 15, 2005; 118(20): 4833 - 4848. [Abstract] [Full Text] [PDF]

Online ISSN 1741-0134 - Print ISSN 1741-0126

Copyright © 2009 Oxford University Press

Oxford Journals Oxford University Press

• Site Map
• Privacy Policy
• Frequently Asked Questions

Other Oxford University Press sites: Oxford University Press Oxford Journals China Oxford Journals Japan American National Biography Booksellers' Information Service Children's Fiction and Poetry Children's Reference Corporate & Special Sales Dictionaries Dictionary of National Biography Digital Reference English Language Teaching Higher Education Textbooks Humanities International Education Unit Law Medicine Music Online Products Oxford English Dictionary Reference Rights and Permissions Science School Books Social Sciences Very Short Introductions World's Classics