In Vivo β-Secretase 1 Inhibition Leads to Brain Aβ Lowering and Increased α-Secretase Processing of Amyloid Precursor Protein without Effect on Neuregulin-1

Sankaranarayanan, Sethu; Price, Eric A.; Wu, Guoxin; Crouthamel, Ming-Chih; Shi, Xiao‐Ping; Tugusheva, Katherine; Tyler, Keala X.; Kahana, Jason A.; Ellis, Joan D.; Jin, Lixia; Steele, T. G.; Stachel, Shawn J.; Coburn, Craig A.; Simon, Adam J.

doi:10.1124/jpet.107.130039

Cited by 97 publications

(89 citation statements)

References 78 publications

(124 reference statements)

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“…These profiles should be a merit of this compound, considering the long period of AD medication. The sustained efficacy of TAK-070 markedly differs from those documented in other BACE1 inhibitors (Sankaranarayanan et al, 2008) or on the higher efficacy of a compound in the presence of inhibitors of P-glycoprotein (Hussain et al, 2007), that determines exposure levels of compounds in brains.…”

Section: Discussionmentioning

confidence: 83%

“…However, there were pivotal differences: TAK-070 treatment affected neither the total number of arm entry in Y-maze test (Ohno et al, 2004) nor the swimming speed in Morris water maze test (Ohno et al, 2006), which were documented to be abnormal in BACE1-homozygous KO regardless of APP-transgenic background. Furthermore, BACE1-homozygous KO in nontransgenic background have been reported to show cognitively deteriorative (Ohno et al, 2004(Ohno et al, , 2006(Ohno et al, , 2007, schizophrenia-like (Savonenko et al, 2008), or hypomyelination (Hu et al, 2006;Sankaranarayanan et al, 2008) phenotypes, underscoring the necessity of BACE1 activity for physiological functions, probably due to multiplicity of substrates for BACE1 (for review, see Marks and Berg, 2008). Also in nontransgenic aged rats, TAK-070 ameliorated behavioral deficits in the water maze test (our unpublished observation).…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, cognitive deficits associated with synaptic degeneration have been documented in PS1/PS2 conditional KO mice with or without APP transgenic background (Saura et al, 2004(Saura et al, , 2005Chen et al, 2008). In contrast, BACE1 KO mice do not show such fatal phenotypes despite its complete ablation, except for partial hypomyelination at the developmental stage (Hu et al, 2006;Sankaranarayanan et al, 2008) or schizophrenialike behavior in homozygous BACE1 KO mice (Savonenko et al, 2008), whereas cognitive deficits are ameliorated on APP transgenic background (Ohno et al, 2004(Ohno et al, , 2006(Ohno et al, , 2007. Furthermore, it has been well documented that the protein levels or activities of BACE1 are upregulated in the brains of patients with sporadic AD (Stockley and O'Neill, 2007).…”

Section: Introductionmentioning

confidence: 99%

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A Noncompetitive BACE1 Inhibitor TAK-070 Ameliorates Aβ Pathology and Behavioral Deficits in a Mouse Model of Alzheimer's Disease

Fukumoto

Takahashi²,

Tarui³

et al. 2010

J. Neurosci.

121

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We discovered a nonpeptidic compound, TAK-070, that inhibited BACE1, a rate-limiting protease for the generation of A␤ peptides that are considered causative for Alzheimer's disease (AD), in a noncompetitive manner. TAK-070 bound to full-length BACE1, but not to truncated BACE1 lacking the transmembrane domain. Short-term oral administration of TAK-070 decreased the brain levels of soluble A␤, increased that of neurotrophic sAPP␣ by ϳ20%, and normalized the behavioral impairments in cognitive tests in Tg2576 mice, an APP transgenic mouse model of AD. Six-month chronic treatment decreased cerebral A␤ deposition by ϳ60%, preserving the pharmacological efficacy on soluble A␤ and sAPP␣ levels. These results support the feasibility of BACE1 inhibition with a noncompetitive inhibitor as disease-modifying as well as symptomatic therapy for AD.

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Section: Discussionmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

A Noncompetitive BACE1 Inhibitor TAK-070 Ameliorates Aβ Pathology and Behavioral Deficits in a Mouse Model of Alzheimer's Disease

Fukumoto

Takahashi²,

Tarui³

et al. 2010

J. Neurosci.

121

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“…As noted above, the hypomyelination phenotype was not noted in BACE1 hemizygous mice expressing 50% of BACE1 in brain. In addition, pharmacologic inhibition achieved by direct central administration of a BACE1 inhibitor did not appear to alter Neuregulin-1 cleavage patterns in adult mouse brain (Sankaranarayanan et al, 2008), but functional deficits were not evaluated. Similarly, the deficits in behavioral cognitive tests, e.g., Morris water maze, Y maze, etc., observed in BACE knock-outs were not present in BACE1 hemizygous mice (Laird et al, 2005), suggesting that partial reduction in BACE1 activity may be better tolerated even when it already occurs during development.…”

Section: Discussionmentioning

confidence: 99%

Robust Central Reduction of Amyloid-β in Humans with an Orally Available, Non-Peptidic β-Secretase Inhibitor

May¹,

Dean²,

Lowe³

et al. 2011

J. Neurosci.

340

381

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“…Briefly, baculovirus expressed and purified truncated BACE1 (aa 1-460) (Shi et al, 2001) at 0.3 nmol/L was incubated at a range of concentrations with a previously characterized BACE1 inhibitor MRK-3 (Stachel et al, 2004;Sankaranarayanan et al, 2008;Wu et al, 2011) for 30 min at RT. After this preincubation, the BACE1 substrate (15 amino acid peptide with C-terminal biotin) was added at a final concentration of 300 nmol/L to the reaction buffer (50 mmol/L NaOAc, 0.01% BSA, 15 mmol/L EDTA, 0.2% CHAPS, 1 mmol/L Deferoxamine Mesylate and 10 μmol/L pepstatin A at pH 4.5) and incubated for 2 h at 37°C in a shaker at 40 rpm .…”

Section: Validation Of the In Vitro Bace1 Inhibitor Assaymentioning

confidence: 99%

Pharmacological applications of a novel neoepitope antibody to a modified amyloid precursor protein-derived beta-secretase product

Wu¹,

Sankaranarayanan²,

Montgomery³

et al. 2011

Protein Cell

Self Cite

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We have previously described a novel artificial NFEV β-secretase (BACE1) cleavage site, which when introduced into the amyloid-β precursor protein (APP), significantly enhances APP cleavage by BACE1 in in vitro and cellular assays. In this study, we describe the identification and characterization of a single chain fragment of variable region (scFv), specific to the EV neo-epitope derived from BACE1 cleavage of the NFEV-containing peptide, and its conversion to IgG1. Both the scFv displayed on phage and EV-IgG1 show exquisite specificity for binding to the EV neoepitope without cross-reactivity to other NFEV containing peptides or WT-APP KMDA cleavage products. EV-IgG1 can detect as little as 0.3 nmol/L of the EV peptide. EV-IgG1 antibody was purified, conjugated with alkaline phosphatase and utilized in various biological assays. In the BACE1 enzymatic assay using NFEV substrate, a BACE1 inhibitor MRK-3 inhibited cleavage with an IC 50 of 2.4 nmol/L with excellent reproducibility. In an APP_NFEV stable SH-SY5Y cellular assay, the EC 50 for inhibition of EV-Aβ peptide secretion with MRK-3 was 236 nmol/L, consistent with values derived using an EV polyclonal antibody. In an APP_NFEV knock-in mouse model, both Aβ_EV40 and Aβ_EV42 peptides in brain homogenate showed excellent gene dosage dependence. In conclusion, the EV neoepitope specific monoclonal antibody is a novel reagent for BACE1 inhibitor discovery for both in vitro, cellular screening assays and in vivo biochemical studies. The methods described herein are generally applicable to novel synthetic substrates and enzyme targets to enable robust screening platforms for enzyme inhibitors.

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In Vivo β-Secretase 1 Inhibition Leads to Brain Aβ Lowering and Increased α-Secretase Processing of Amyloid Precursor Protein without Effect on Neuregulin-1

Cited by 97 publications

References 78 publications

A Noncompetitive BACE1 Inhibitor TAK-070 Ameliorates Aβ Pathology and Behavioral Deficits in a Mouse Model of Alzheimer's Disease

A Noncompetitive BACE1 Inhibitor TAK-070 Ameliorates Aβ Pathology and Behavioral Deficits in a Mouse Model of Alzheimer's Disease

Robust Central Reduction of Amyloid-β in Humans with an Orally Available, Non-Peptidic β-Secretase Inhibitor

Pharmacological applications of a novel neoepitope antibody to a modified amyloid precursor protein-derived beta-secretase product

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