| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1177718 | Biochimica et Biophysica Acta (BBA) - Proteins and Proteomics | 2016 | 9 Pages |
•X-ray structure of the precursor mimic of BlGT was solved.•X-ray Structure highlights a number of residues that are crucial for autoprocessing.•Mutation of H401, T415, T417, E419 and R571 decelerate BlGT autoprocessing.•A possible mechanism of gamma-GT autoprocessing is proposed.
γ-Glutamyl transpeptidases (γ-GTs) are members of N-terminal nucleophile hydrolase superfamily. They are synthetized as single-chain precursors, which are then cleaved to form mature enzymes. Basic aspects of autocatalytic processing of these pro-enzymes are still unknown. Here we describe the X-ray structure of the precursor mimic of Bacillus licheniformis γ-GT (BlGT), obtained by mutating catalytically important threonine to alanine (T399A-BlGT), and report results of autoprocessing of mutants of His401, Thr415, Thr417, Glu419 and Arg571. Data suggest that Thr417 is in a competent position to activate the catalytic threonine (Thr399) for nucleophilic attack of the scissile peptide bond and that Thr415 plays a major role in assisting the process. On the basis of these new structural results, a possible mechanism of autoprocessing is proposed. This mechanism, which guesses the existence of a six-membered transition state involving one carbonyl and two hydroxyl groups, is in agreement with all the available experimental data collected on γ-GTs from different species and with our new Ala-scanning mutagenesis data.
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