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Differential substrate specificity of group I and group II chaperonins in the archaeon Methanosarcina mazei
Authors:Angela M Hirtreiter  Giulia Calloni  Francesca Forner  Burghardt Scheibe  Magda Puype  Joel Vandekerckhove  Matthias Mann  F Ulrich Hartl  Manajit Hayer‐Hartl
Institution:1. Departments of Cellular Biochemistry and;2. Present address: Research Department of Structural and Molecular Biology, UCL, Gower Street, WC1e 6BT London, UK.;3. These authors contributed equally.;4. Proteomics and Signal Transduction, Max Planck Institute of Biochemistry, Am Klopferspitz 18, D‐82152 Martinsried, Germany.;5. GE Healthcare Europe GmbH, Europlaza – Geb?ude E, Wienerbergstr. 41, A‐1120 Vienna, Austria.;6. Department of Medical Protein Research, VIB Flanders Institute for Biotechnology, Flanders, Belgium.;7. Department of Biochemistry, Ghent University, A. Baertsoenkaai 3, 9000 Ghent, Belgium.
Abstract:Chaperonins are macromolecular machines that assist in protein folding. The archaeon Methanosarcina mazei has acquired numerous bacterial genes by horizontal gene transfer. As a result, both the bacterial group I chaperonin, GroEL, and the archaeal group II chaperonin, thermosome, coexist. A proteome‐wide analysis of chaperonin interactors was performed to determine the differential substrate specificity of GroEL and thermosome. At least 13% of soluble M. mazei proteins interact with chaperonins, with the two systems having partially overlapping substrate sets. Remarkably, chaperonin selectivity is independent of phylogenetic origin and is determined by distinct structural and biochemical features of proteins. GroEL prefers well‐conserved proteins with complex α/β domains. In contrast, thermosome substrates comprise a group of faster‐evolving proteins and contain a much wider range of different domain folds, including small all‐α and all‐β modules, and a greater number of large multidomain proteins. Thus, the group II chaperonins may have facilitated the evolution of the highly complex proteomes characteristic of eukaryotic cells.
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