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Literature DB >> 21919498

Dissociation between the processivity and total activity of γ-secretase: implications for the mechanism of Alzheimer's disease-causing presenilin mutations.

Omar Quintero-Monzon¹, Morgan M Martin, Marty A Fernandez, Christina A Cappello, Amanda J Krzysiak, Pamela Osenkowski, Michael S Wolfe.

Abstract

The amyloid β-peptide (Aβ), strongly implicated in the pathogenesis of Alzheimer's disease (AD), is produced from the amyloid β-protein precursor (APP) through consecutive proteolysis by β- and γ-secretases. The latter protease contains presenilin as the catalytic component of a membrane-embedded aspartyl protease complex. Missense mutations in presenilin are associated with early-onset familial AD, and these mutations generally both decrease Aβ production and increase the ratio of the aggregation-prone 42-residue form (Aβ42) to the 40-residue form (Aβ40). The connection between these two effects is not understood. Besides Aβ40 and Aβ42, γ-secretase produces a range of Aβ peptides, the result of initial cutting at the ε site to form Aβ48 or Aβ49 and subsequent trimming every three or four residues. Thus, γ-secretase displays both overall proteolytic activity (ε cutting) and processivity (trimming) toward its substrate APP. Here we tested whether a decrease in total activity correlates with decreased processivity using wild-type and AD-mutant presenilin-containing protease complexes. Changes in pH, temperature, and salt concentration that reduced the overall activity of the wild-type enzyme did not consistently result in increased proportions of longer Aβ peptides. Low salt concentrations and acidic pH were notable exceptions that subtly alter the proportion of individual Aβ peptides, suggesting that the charged state of certain residues may influence processivity. Five different AD mutant complexes, representing a broad range of effects on overall activity, Aβ42:Aβ40 ratios, and ages of disease onset, were also tested, revealing again that changes in total activity and processivity can be dissociated. Factors that control initial proteolysis of APP at the ε site apparently differ significantly from factors affecting subsequent trimming and the distribution of Aβ peptides.

Entities: CellLine Chemical Disease Gene Mutation Species

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Year: 2011 PMID： 21919498 PMCID： PMC3205908 DOI： 10.1021/bi2007146

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

75 in total

1. Evidence that Abeta42 plasma levels in presenilin-1 mutation carriers do not allow for prediction of their clinical phenotype.

Authors: C De Jonghe; P Cras; H Vanderstichele; M Cruts; I Vanderhoeven; I Smouts; E Vanmechelen; J J Martin; L Hendriks; C Van Broeckhoven
Journal: Neurobiol Dis Date: 1999-08 Impact factor: 5.996

2. Endoproteolytic processing and stabilization of wild-type and mutant presenilin.

Authors: T Ratovitski; H H Slunt; G Thinakaran; D L Price; S S Sisodia; D R Borchelt
Journal: J Biol Chem Date: 1997-09-26 Impact factor: 5.157

3. Subcellular distribution and turnover of presenilins in transfected cells.

Authors: J Zhang; D E Kang; W Xia; M Okochi; H Mori; D J Selkoe; E H Koo
Journal: J Biol Chem Date: 1998-05-15 Impact factor: 5.157

4. Two transmembrane aspartates in presenilin-1 required for presenilin endoproteolysis and gamma-secretase activity.

Authors: M S Wolfe; W Xia; B L Ostaszewski; T S Diehl; W T Kimberly; D J Selkoe
Journal: Nature Date: 1999-04-08 Impact factor: 49.962

5. Proteolytic release and nuclear translocation of Notch-1 are induced by presenilin-1 and impaired by pathogenic presenilin-1 mutations.

Authors: W Song; P Nadeau; M Yuan; X Yang; J Shen; B A Yankner
Journal: Proc Natl Acad Sci U S A Date: 1999-06-08 Impact factor: 11.205

6. The proteolytic fragments of the Alzheimer's disease-associated presenilin-1 form heterodimers and occur as a 100-150-kDa molecular mass complex.

Authors: A Capell; J Grünberg; B Pesold; A Diehlmann; M Citron; R Nixon; K Beyreuther; D J Selkoe; C Haass
Journal: J Biol Chem Date: 1998-02-06 Impact factor: 5.157

7. Evidence that levels of presenilins (PS1 and PS2) are coordinately regulated by competition for limiting cellular factors.

Authors: G Thinakaran; C L Harris; T Ratovitski; F Davenport; H H Slunt; D L Price; D R Borchelt; S S Sisodia
Journal: J Biol Chem Date: 1997-11-07 Impact factor: 5.157

8. Longer forms of amyloid beta protein: implications for the mechanism of intramembrane cleavage by gamma-secretase.

Authors: Yue Qi-Takahara; Maho Morishima-Kawashima; Yu Tanimura; Georgia Dolios; Naoko Hirotani; Yuko Horikoshi; Fuyuki Kametani; Masahiro Maeda; Takaomi C Saido; Rong Wang; Yasuo Ihara
Journal: J Neurosci Date: 2005-01-12 Impact factor: 6.167

9. Human presenilin-1, but not familial Alzheimer's disease (FAD) mutants, facilitate Caenorhabditis elegans Notch signalling independently of proteolytic processing.

Authors: R Baumeister; U Leimer; I Zweckbronner; C Jakubek; J Grünberg; C Haass
Journal: Genes Funct Date: 1997-04

10. The presenilin C-terminus is required for ER-retention, nicastrin-binding and gamma-secretase activity.

Authors: Christoph Kaether; Anja Capell; Dieter Edbauer; Edith Winkler; Bozidar Novak; Harald Steiner; Christian Haass
Journal: EMBO J Date: 2004-11-18 Impact factor: 11.598

58 in total

1. Shifting a complex debate on γ-secretase cleavage and Alzheimer's disease.

Authors: Todd E Golde; Yong Ran; Kevin M Felsenstein
Journal: EMBO J Date: 2012-04-13 Impact factor: 11.598

2. Nicastrin functions to sterically hinder γ-secretase-substrate interactions driven by substrate transmembrane domain.

Authors: David M Bolduc; Daniel R Montagna; Yongli Gu; Dennis J Selkoe; Michael S Wolfe
Journal: Proc Natl Acad Sci U S A Date: 2015-12-22 Impact factor: 11.205

3. Generation of Alzheimer disease-associated amyloid β42/43 peptide by γ-secretase can be inhibited directly by modulation of membrane thickness.

Authors: Edith Winkler; Frits Kamp; Johannes Scheuring; Amelie Ebke; Akio Fukumori; Harald Steiner
Journal: J Biol Chem Date: 2012-04-24 Impact factor: 5.157

Dissociation between the processivity and total activity of γ-secretase: implications for the mechanism of Alzheimer's disease-causing presenilin mutations.

1. Evidence that Abeta42 plasma levels in presenilin-1 mutation carriers do not allow for prediction of their clinical phenotype.

2. Endoproteolytic processing and stabilization of wild-type and mutant presenilin.

3. Subcellular distribution and turnover of presenilins in transfected cells.

4. Two transmembrane aspartates in presenilin-1 required for presenilin endoproteolysis and gamma-secretase activity.

5. Proteolytic release and nuclear translocation of Notch-1 are induced by presenilin-1 and impaired by pathogenic presenilin-1 mutations.

6. The proteolytic fragments of the Alzheimer's disease-associated presenilin-1 form heterodimers and occur as a 100-150-kDa molecular mass complex.

7. Evidence that levels of presenilins (PS1 and PS2) are coordinately regulated by competition for limiting cellular factors.

8. Longer forms of amyloid beta protein: implications for the mechanism of intramembrane cleavage by gamma-secretase.

9. Human presenilin-1, but not familial Alzheimer's disease (FAD) mutants, facilitate Caenorhabditis elegans Notch signalling independently of proteolytic processing.

10. The presenilin C-terminus is required for ER-retention, nicastrin-binding and gamma-secretase activity.

1. Shifting a complex debate on γ-secretase cleavage and Alzheimer's disease.

2. Nicastrin functions to sterically hinder γ-secretase-substrate interactions driven by substrate transmembrane domain.

3. Generation of Alzheimer disease-associated amyloid β42/43 peptide by γ-secretase can be inhibited directly by modulation of membrane thickness.

4. γ-Secretase processing and effects of γ-secretase inhibitors and modulators on long Aβ peptides in cells.

Review 5. Unraveling the complexity of γ-secretase.

6. Intramembrane proteolysis of β-amyloid precursor protein by γ-secretase is an unusually slow process.

7. Presenilin 1 mutations influence processing and trafficking of the ApoE receptor apoER2.

Review 8. Toward the treatment and prevention of Alzheimer's disease: rational strategies and recent progress.

Review 9. Toward the structure of presenilin/γ-secretase and presenilin homologs.

Review 10. Development and mechanism of γ-secretase modulators for Alzheimer's disease.