GroE Facilitates Refolding of Citrate Synthase by Suppressing Aggregation

Johannes Buchner, Marion Schmidt, Miriam Fuchs, Rainer Jaenicke, Rainer Rudolph, Franz X. Schmid, Thomas Kiefhaber

Research output: Contribution to journalArticlepeer-review

483 Scopus citations

Abstract

The molecular chaperone GroE facilitates correct protein folding in vivo and in vitro. The mode of action of GroE was investigated by using refolding of citrate synthase as a model system. In vitro denaturation of this dimeric protein is almost irreversible, since the refolding polypeptide chains aggregate rapidly, as shown directly by a strong, concentration-dependent increase in light scattering. The yields of reactivated citrate synthase were strongly increased upon addition of GroE and MgATP. GroE inhibits aggregation reactions that compete with correct protein folding, as indicated by specific suppression of light scattering. GroEL rapidly forms a complex with unfolded or partially folded citrate synthase molecules. In this complex the refolding protein is protected from aggregation. Addition of GroES and ATP hydrolysis is required to release the polypeptide chain bound to GroEL and to allow further folding to its final, active state.

Original languageEnglish
Pages (from-to)1586-1591
Number of pages6
JournalBiochemistry
Volume30
Issue number6
DOIs
StatePublished - 1 Feb 1991
Externally publishedYes

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