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Literature DB >> 19374450

Effects of pH and iminosugar pharmacological chaperones on lysosomal glycosidase structure and stability.

Raquel L Lieberman¹, J Alejandro D'aquino, Dagmar Ringe, Gregory A Petsko.

Abstract

Human lysosomal enzymes acid-beta-glucosidase (GCase) and acid-alpha-galactosidase (alpha-Gal A) hydrolyze the sphingolipids glucosyl- and globotriaosylceramide, respectively, and mutations in these enzymes lead to the lipid metabolism disorders Gaucher and Fabry disease, respectively. We have investigated the structure and stability of GCase and alpha-Gal A in a neutral-pH environment reflective of the endoplasmic reticulum and an acidic-pH environment reflective of the lysosome. These details are important for the development of pharmacological chaperone therapy for Gaucher and Fabry disease, in which small molecules bind mutant enzymes in the ER to enable the mutant enzyme to meet quality control requirements for lysosomal trafficking. We report crystal structures of apo GCase at pH 4.5, at pH 5.5, and in complex with the pharmacological chaperone isofagomine (IFG) at pH 7.5. We also present thermostability analysis of GCase at pH 7.4 and 5.2 using differential scanning calorimetry. We compare our results with analogous experiments using alpha-Gal A and the chaperone 1-deoxygalactonijirimycin (DGJ), including the first structure of alpha-Gal A with DGJ. Both GCase and alpha-Gal A are more stable at lysosomal pH with and without their respective iminosugars bound, and notably, the stability of the GCase-IFG complex is pH sensitive. We show that the conformations of the active site loops in GCase are sensitive to ligand binding but not pH, whereas analogous galactose- or DGJ-dependent conformational changes in alpha-Gal A are not seen. Thermodynamic parameters obtained from alpha-Gal A unfolding indicate two-state, van't Hoff unfolding in the absence of the iminosugar at neutral and lysosomal pH, and non-two-state unfolding in the presence of DGJ. Taken together, these results provide insight into how GCase and alpha-Gal A are thermodynamically stabilized by iminosugars and suggest strategies for the development of new pharmacological chaperones for lysosomal storage disorders.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：

Year: 2009 PMID： 19374450 PMCID： PMC2699628 DOI： 10.1021/bi9002265

Source DB: PubMed Journal: Biochemistry ISSN： 0006-2960 Impact factor: 3.162

77 in total

1. PRODRG: a tool for high-throughput crystallography of protein-ligand complexes.

Authors: Alexander W Schüttelkopf; Daan M F van Aalten
Journal: Acta Crystallogr D Biol Crystallogr Date: 2004-07-21

2. Structure of acid beta-glucosidase with pharmacological chaperone provides insight into Gaucher disease.

Authors: Raquel L Lieberman; Brandon A Wustman; Pedro Huertas; Allan C Powe; Corey W Pine; Richie Khanna; Michael G Schlossmacher; Dagmar Ringe; Gregory A Petsko
Journal: Nat Chem Biol Date: 2006-12-24 Impact factor: 15.040

3. The iminosugar isofagomine increases the activity of N370S mutant acid beta-glucosidase in Gaucher fibroblasts by several mechanisms.

Authors: Richard A Steet; Stephen Chung; Brandon Wustman; Allan Powe; Hung Do; Stuart A Kornfeld
Journal: Proc Natl Acad Sci U S A Date: 2006-08-31 Impact factor: 11.205

4. An adaptable standard for protein export from the endoplasmic reticulum.

Authors: R Luke Wiseman; Evan T Powers; Joel N Buxbaum; Jeffery W Kelly; William E Balch
Journal: Cell Date: 2007-11-16 Impact factor: 41.582

5. Sustained therapeutic effects of oral miglustat (Zavesca, N-butyldeoxynojirimycin, OGT 918) in type I Gaucher disease.

Authors: D Elstein; C Hollak; J M F G Aerts; S van Weely; M Maas; T M Cox; R H Lachmann; M Hrebicek; F M Platt; T D Butters; R A Dwek; A Zimran
Journal: J Inherit Metab Dis Date: 2004 Impact factor: 4.982

6. In vitro inhibition and intracellular enhancement of lysosomal alpha-galactosidase A activity in Fabry lymphoblasts by 1-deoxygalactonojirimycin and its derivatives.

Authors: N Asano; S Ishii; H Kizu; K Ikeda; K Yasuda; A Kato; O R Martin; J Q Fan
Journal: Eur J Biochem Date: 2000-07

7. Chemical chaperones improve transport and enhance stability of mutant alpha-glucosidases in glycogen storage disease type II.

Authors: Toshika Okumiya; Marian A Kroos; Laura Van Vliet; Hiroaki Takeuchi; Ans T Van der Ploeg; Arnold J J Reuser
Journal: Mol Genet Metab Date: 2006-11-13 Impact factor: 4.797

8. N-octyl-beta-valienamine up-regulates activity of F213I mutant beta-glucosidase in cultured cells: a potential chemical chaperone therapy for Gaucher disease.

Authors: Hou Lin; Yuko Sugimoto; Yuki Ohsaki; Haruaki Ninomiya; Akira Oka; Miyako Taniguchi; Hiroyuki Ida; Yoshikatsu Eto; Seiichiro Ogawa; Yuji Matsuzaki; Miwa Sawa; Takehiko Inoue; Katsumi Higaki; Eiji Nanba; Kousaku Ohno; Yoshiyuki Suzuki
Journal: Biochim Biophys Acta Date: 2004-08-04

9. Thermal denaturation of the core protein of lac repressor.

Authors: S P Manly; K S Matthews; J M Sturtevant
Journal: Biochemistry Date: 1985-07-16 Impact factor: 3.162

10. In situ radiation-inactivation size of fibroblast membrane-bound acid beta-glucosidase in Gaucher type 1, type 2 and type 3 disease.

Authors: F Y Choy; M Woo; M Potier
Journal: Biochim Biophys Acta Date: 1986-03-07

60 in total

1. Ex vivo and in vivo effects of isofagomine on acid β-glucosidase variants and substrate levels in Gaucher disease.

Authors: Ying Sun; Benjamin Liou; You-Hai Xu; Brian Quinn; Wujuan Zhang; Rick Hamler; Kenneth D R Setchell; Gregory A Grabowski
Journal: J Biol Chem Date: 2011-12-13 Impact factor: 5.157

2. Binding of 3,4,5,6-tetrahydroxyazepanes to the acid-β-glucosidase active site: implications for pharmacological chaperone design for Gaucher disease.

Authors: Susan D Orwig; Yun Lei Tan; Neil P Grimster; Zhanqian Yu; Evan T Powers; Jeffery W Kelly; Raquel L Lieberman
Journal: Biochemistry Date: 2011-11-14 Impact factor: 3.162

Effects of pH and iminosugar pharmacological chaperones on lysosomal glycosidase structure and stability.

1. PRODRG: a tool for high-throughput crystallography of protein-ligand complexes.

2. Structure of acid beta-glucosidase with pharmacological chaperone provides insight into Gaucher disease.

3. The iminosugar isofagomine increases the activity of N370S mutant acid beta-glucosidase in Gaucher fibroblasts by several mechanisms.

4. An adaptable standard for protein export from the endoplasmic reticulum.

5. Sustained therapeutic effects of oral miglustat (Zavesca, N-butyldeoxynojirimycin, OGT 918) in type I Gaucher disease.

6. In vitro inhibition and intracellular enhancement of lysosomal alpha-galactosidase A activity in Fabry lymphoblasts by 1-deoxygalactonojirimycin and its derivatives.

7. Chemical chaperones improve transport and enhance stability of mutant alpha-glucosidases in glycogen storage disease type II.

8. N-octyl-beta-valienamine up-regulates activity of F213I mutant beta-glucosidase in cultured cells: a potential chemical chaperone therapy for Gaucher disease.

9. Thermal denaturation of the core protein of lac repressor.

10. In situ radiation-inactivation size of fibroblast membrane-bound acid beta-glucosidase in Gaucher type 1, type 2 and type 3 disease.

1. Ex vivo and in vivo effects of isofagomine on acid β-glucosidase variants and substrate levels in Gaucher disease.

2. Binding of 3,4,5,6-tetrahydroxyazepanes to the acid-β-glucosidase active site: implications for pharmacological chaperone design for Gaucher disease.

3. Molecular basis of reduced glucosylceramidase activity in the most common Gaucher disease mutant, N370S.

4. α-Galactosidase aggregation is a determinant of pharmacological chaperone efficacy on Fabry disease mutants.

5. Characterizing Thermal Transitions of IgG with Mass Spectrometry.

6. Impact of cysteine variants on the structure, activity, and stability of recombinant human α-galactosidase A.

7. Enzyme enhancers for the treatment of Fabry and Pompe disease.

Review 8. An integrative approach to improving the biocatalytic reactions of whole cells expressing recombinant enzymes.

Review 9. Clarifying lysosomal storage diseases.

10. Catalytic mechanism of human alpha-galactosidase.