Mechanism of Phosphatidylinositol-Specific Phospholipase C: A Unified View of the Mechanism of Catalysis,
- 1 March 1998
- journal article
- research article
- Published by American Chemical Society (ACS) in Biochemistry
- Vol. 37 (13), 4568-4580
- https://doi.org/10.1021/bi972646i
Abstract
The mechanism of phosphatidylinositol-specific phospholipase C (PI-PLC) has been suggested to resemble that of ribonuclease A. The goal of this work is to rigorously evaluate the mechanism of PI-PLC from Bacillus thuringiensis by examining the functional and structural roles of His-32 and His-82, along with the two nearby residues Asp-274 and Asp-33 (which form a hydrogen bond with His-32 and His-82, respectively), using site-directed mutagenesis. In all, twelve mutants were constructed, which, except D274E, showed little structural perturbation on the basis of 1D NMR and 2D NOESY analyses. The H32A, H32N, H32Q, H82A, H82N, H82Q, H82D, and D274A mutants showed a 104−105-fold decrease in specific activity toward phosphatidylinositol; the D274N, D33A, and D33N mutants retained 0.1−1% activity, whereas the D274E mutant retained 13% activity. Steady-state kinetic analysis of mutants using (2R)-1,2-dipalmitoyloxypropane-3-(thiophospho-1d-myo-inositol) (DPsPI) as a substrate generally agreed well with the specific activity toward phosphatidylinositol. The results suggest a mechanism in which His-32 functions as a general base to abstract the proton from 2-OH and facilitates the attack of the deprotonated 2-oxygen on the phosphorus atom. This general base function is augmented by the carboxylate group of Asp-274 which forms a diad with His-32. The H82A and D33A mutants showed an unusually high activity with substrates featuring low pKa leaving groups, such as DPsPI and p-nitrophenyl inositol phosphate (NPIPs). These results suggest that His-82 functions as the general acid with assistance from Asp-33, facilitating the departure of the leaving group by protonation of the glycerol O3 oxygen. The Brønsted coefficients obtained for the WT and the D33N mutant indicate a high degree of proton transfer to the leaving group and further underscore the “helper” function of Asp-33. The complete mechanism also includes activation of the phosphate group toward nucleophilic attack by a hydrogen bond between Arg-69 and a nonbridging oxygen atom. The overall mechanism can be described as “complex” general acid−general base since three elements are required for efficient catalysis.Keywords
This publication has 19 references indexed in Scilit:
- Phosphatidylinositol-Specific Phospholipase C: Kinetic and Stereochemical Evidence for an Interaction between Arginine-69 and the Phosphate Group of Phosphatidylinositol,Biochemistry, 1997
- SYNTHESIS OF ENANTIOMERICALLY PURE PHOSPHOROTHIOLATE ASSAY SUBSTRATE FOR PHOSPHATIDYLINOSITOL-SPECIFIC PHOSPHOLIPASE CBioorganic & Medicinal Chemistry Letters, 1997
- Synthesis of Inositol Phosphodiesters by Phospholipase C-Catalyzed TransesterificationJournal of the American Chemical Society, 1996
- Ribonuclease A: Revealing Structure-Function Relationships with SemisynthesisJournal of the American Chemical Society, 1995
- Are D- and L-chiro-Phosphoinositides Substrates of Phosphatidylinositol-Specific Phospholipase C?Biochemistry, 1994
- Toward the mechanism of phosphoinositide-specific phospholipases CBioorganic & Medicinal Chemistry, 1994
- Metal ion catalysis in the Tetrahymena ribozyme reactionNature, 1993
- Phospholipids chiral at phosphorus. Stereochemical mechanism of reactions catalyzed by phosphatidylinositide-specific phospholipase C from Bacillus cereus and guinea pig uterusBiochemistry, 1990
- Charge description of base-catalyzed alcoholysis of aryl phosphodiesters: a ribonuclease modelJournal of the American Chemical Society, 1988
- Acidic dissociation constants of thiolsJournal of Chemical & Engineering Data, 1968