Identification of γ-Secretase Inhibitor Potency Determinants on Presenilin

Zhao, Byron; Yu, Mei; Neitzel, Martin L.; Marugg, Jennifer L.; Jagodziński, Jacek; Lee, Mike; Hu, Kang; Schenk, Dale; Yednock, Ted; Basi, Guriqbal S.

doi:10.1074/jbc.m708870200

Cited by 58 publications

(47 citation statements)

References 61 publications

(56 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…MRK-560 also showed a differential interaction to PS1 compared with PS2, providing a molecular explanation to the observed preference for PS1-containing ␥-secretases. It has previously been proposed that GSIs of the sulfonamide type preferentially inhibit PS1-containing ␥-secretase (Zhao et al, 2008;Borgegard et al, 2011), but our data show that the preference for PS1 versus PS2 processing varies considerably among different sulfonamide GSIs: MRK-560 exhibited a considerably stronger preference for PS1 over PS2 processing, whereas avagacestat (BMS-708163) did not. This difference is of interest with regard to the results from recent clinical trials, where avagacestat caused Notch-related side effects in Phase 2 clinical trials (Imbimbo et al, 2011).…”

Section: Discussioncontrasting

confidence: 49%

“…Gene targeting of ␥-secretase subunits in mice has revealed distinct physiological roles for specific ␥-secretase components in vivo (Saura et al, 2004;Serneels et al, 2005). In the context of AD, it is of particular interest that PS1 seems to catalyze the vast majority of CNS A␤ production (De Strooper et al, 1998;Borgegard et al, 2011) and that certain GSIs of the sulfonamide class appear to exhibit a preference for PS1 over PS2 ␥-secretase activities (Zhao et al, 2008;Borgegard et al, 2011), supporting the notion that development of ␥-secretase subcomplex selective GSIs may be feasible. In line with this, the sulfonamide GSI, MRK-560, inhibits A␤ production in an efficacious manner and reduces neural plaque formation without producing the Notchrelated off target effects observed in chronic studies in mice (Best et al, 2007).…”

Section: Introductionmentioning

confidence: 85%

See 1 more Smart Citation

Alzheimer's Disease: Presenilin 2-Sparing γ-Secretase Inhibition Is a Tolerable Aβ Peptide-Lowering Strategy

et al. 2012

View full text Add to dashboard Cite

␥-Secretase inhibition represents a major therapeutic strategy for lowering amyloid ␤ (A␤) peptide production in Alzheimer's disease (AD).Progress toward clinical use of ␥-secretase inhibitors has, however, been hampered due to mechanism-based adverse events, primarily related to impairment of Notch signaling. The ␥-secretase inhibitor MRK-560 represents an exception as it is largely tolerable in vivo despite displaying only a small selectivity between A␤ production and Notch signaling in vitro. In exploring the molecular basis for the observed tolerability, we show that MRK-560 displays a strong preference for the presenilin 1 (PS1) over PS2 subclass of ␥-secretases and is tolerable in wild-type mice but causes dose-dependent Notch-related side effect in PS2-deficient mice at drug exposure levels resulting in a substantial decrease in brain A␤ levels. This demonstrates that PS2 plays an important role in mediating essential Notch signaling in several peripheral organs during pharmacological inhibition of PS1 and provide preclinical in vivo proof of concept for PS2-sparing inhibition as a novel, tolerable and efficacious ␥-secretase targeting strategy for AD.

show abstract

Section: Discussioncontrasting

confidence: 49%

Section: Introductionmentioning

confidence: 85%

Alzheimer's Disease: Presenilin 2-Sparing γ-Secretase Inhibition Is a Tolerable Aβ Peptide-Lowering Strategy

et al. 2012

View full text Add to dashboard Cite

show abstract

“…Further analysis on the role of TMD3 on substrates other than APP and Notch would be required. Intriguingly, some residues on TMD3 have been implicated in the determination of PS1/PS2 specificity of a subset of the ␥-secretase inhibitors (26). Nevertheless, these data support the idea that TMD3 is involved in the acquisition of proper cleavage activity of the ␥-secretase after the assembly of the complex.…”

Section: Transmembrane Domains 8 and 9 Of Presenilin 1 Arecontrasting

confidence: 50%

Functional Analysis of the Transmembrane Domains of Presenilin 1

Watanabe

Takagi

Tominaga

et al. 2010

Journal of Biological Chemistry

View full text Add to dashboard Cite

␥-Secretase is a multimeric membrane protein complex composed of presenilin (PS), nicastrin, Aph-1, and Pen-2, which mediates intramembrane proteolysis of a range of type I transmembrane proteins. We previously analyzed the functional roles of the N-terminal transmembrane domains (TMDs) 1-6 of PS1 in the assembly and proteolytic activity of the ␥-secretase using a series of TMD-swap PS1 mutants. Here we applied the TMD-swap method to all the TMDs of PS1 for the structurefunction analysis of the proteolytic mechanism of ␥-secretase. We found that TMD2-or -6-swapped mutant PS1 failed to bind the helical peptide-based, substrate-mimic ␥-secretase inhibitor. Cross-linking experiments revealed that both TMD2 and TMD6 of PS1 locate in proximity to the TMD9, the latter being implicated in the initial substrate binding. Taken together, our data suggest that TMD2 and the luminal side of TMD6 are involved in the formation of the initial substrate-binding site of the ␥-secretase complex.

show abstract

“…Consequently, we suggest that γ-secretase inhibitors that preferentially inhibit PS1-containing γ-secretase complexes (e.g., sulfonamides [30, 40]) represent a promising avenue for reducing Aβ production while leaving the generation of the physiologically critical AICD and NICD products relatively unaffected. …”

Section: Discussionmentioning

confidence: 99%

Evidence that Enzyme Processivity Mediates Differential Aβ Production by PS1 and PS2

Pintchovski¹,

Basi²

2013

Current Alzheimer Research

View full text Add to dashboard Cite

The γ-secretase complex cleaves the carboxy-terminal 99 residue (C99) fragment of the amyloid precursor protein (APP) to generate the amyloid-β (Aβ) peptide. The catalytic activity of this complex is mediated either by the presenilin-1 (PS1) or the presenilin-2 (PS2) subunit. In vitro and in vivo studies have demonstrated that PS1-containing complexes generate more total Aβ product than PS2-containing complexes, indicating greater cleavage activity by PS1-containing γ-secretase complexes at the APP γ-site. However, it remains untested whether γ-secretase cleavage at the APP ε-site, which precedes γ-site cleavage and produces the physiologically active APP intracellular domain (AICD), follows the same rule. Using a novel Swedish APP-GVP substrate to facilitate the parallel detection of Aβ and AICD products from PS1-/-/PS2-/- cells co-transfected with either PS1 or PS2, we observed that while PS1 generates more total Aβ product than PS2, consistent with published reports, PS1 and PS2 unexpectedly generate equal amounts of AICD product. We also observed that PS1 and PS2 produce equivalent amounts of Notch intracellular domain (NICD), indicating equal cleavage activity at the Notch S3-site (the corollary of the APP ε-site). Our findings suggest that processivity differences between PS1 and PS2 underlie the differential production of Aβ peptide. Taken together these findings offer novel insights into γ-secretase biology and have important implications for therapeutically targeting γ-secretase

show abstract

Identification of γ-Secretase Inhibitor Potency Determinants on Presenilin

Cited by 58 publications

References 61 publications

Alzheimer's Disease: Presenilin 2-Sparing γ-Secretase Inhibition Is a Tolerable Aβ Peptide-Lowering Strategy

Alzheimer's Disease: Presenilin 2-Sparing γ-Secretase Inhibition Is a Tolerable Aβ Peptide-Lowering Strategy

Functional Analysis of the Transmembrane Domains of Presenilin 1

Evidence that Enzyme Processivity Mediates Differential Aβ Production by PS1 and PS2

Contact Info

Product

Resources

About