Literature DB >> 15858260

Crystal engineering yields crystals of cyclophilin D diffracting to 1.7 A resolution.

Daniel Schlatter1, Ralf Thoma, Erich Küng, Martine Stihle, Francis Müller, Edilio Borroni, Andrea Cesura, Michael Hennig.   

Abstract

In the pharmaceutical industry, knowledge of the three-dimensional structure of a specific target facilitates the drug-discovery process. Despite possessing favoured analytical properties such as high purity and monodispersion in light scattering, some proteins are not capable of forming crystals suitable for X-ray analysis. Cyclophilin D, an isoform of cyclophilin that is expressed in the mitochondria, was selected as a drug target for the treatment of cardiac disorders. As the wild-type enzyme defied all attempts at crystallization, protein engineering on the enzyme surface was performed. The K133I mutant gave crystals that diffracted to 1.7 A resolution using in-house X-ray facilities and were suitable for soaking experiments. The crystals were very robust and diffraction was maintained after soaking in 25% DMSO solution: excellent conditions for the rapid analysis of complex structures including crystallographic fragment screening.

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Year:  2005        PMID: 15858260     DOI: 10.1107/S0907444905003070

Source DB:  PubMed          Journal:  Acta Crystallogr D Biol Crystallogr        ISSN: 0907-4449


  13 in total

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