Apo and Inhibitor Complex Structures of BACE (β-secretase)

Patel, Sahil; Vuillard, Laurent; Cleasby, Anne; Murray, Christopher W.; Yon, Jeannine

doi:10.1016/j.jmb.2004.08.018

Cited by 181 publications

(224 citation statements)

References 52 publications

Supporting

Mentioning

211

Contrasting

Unclassified

Order By: Relevance

“…Protein Crystallography-Protein expression and purification for structural studies was done as previously described by Patel et al (36). Crystallization of compounds bound to BACE1 has been described by Swahn et al (37).…”

Section: Methodsmentioning

confidence: 99%

Discovery of AZD3839, a Potent and Selective BACE1 Inhibitor Clinical Candidate for the Treatment of Alzheimer Disease

Jeppsson

Eketjäll

Janson

et al. 2012

Journal of Biological Chemistry

112

View full text Add to dashboard Cite

Section: Methodsmentioning

confidence: 99%

Discovery of AZD3839, a Potent and Selective BACE1 Inhibitor Clinical Candidate for the Treatment of Alzheimer Disease

Jeppsson

Eketjäll

Janson

et al. 2012

Journal of Biological Chemistry

112

View full text Add to dashboard Cite

“…The protein solution was estimated to be Ͼ95% pure as judged by sodium dodecyl sulfate-polyacrylamide gel electrophoresis. Crystallization for apo BACE1 was performed by the sitting-drop vapor diffusion method described previously (24). Equal volumes of protein solution and mother liquor, containing 15 to 22.5% (wt/vol) polyethylene glycol 5000 monomethyl ether (PEG 5000 MME), 200 mM ammonium iodide, 200 mM sodium citrate, pH 6.0 to 7.0, were mixed in a single droplet and equilibrated against 0.5 ml of mother liquor at 20°C.…”

Section: Methodsmentioning

confidence: 99%

“…These studies indicated that the active site of BACE1 is covered by a flexible antiparallel ␤-hairpin, called a flap, which is believed to control substrate access to the active site and set the substrate into the correct geometry for the catalytic process. It has been reported that the flap of the inhibitor-bound form is tightly packed in a closed conformation; however, the substrate-free (apo) structure of BACE1 showed that the flap was in an open conformation (14,24). These results indicate that a conformational change must take place upon binding of the inhibitor/ substrate to the active site and may participate kinetically in substrate binding in the closed conformation and product release in the open conformation.…”

mentioning

confidence: 86%

“…BACE1 has become a major target in the development of drugs for AD, and X-ray crystallography has determined numerous structures of BACE1 complexes (12,13,24,34). These studies indicated that the active site of BACE1 is covered by a flexible antiparallel ␤-hairpin, called a flap, which is believed to control substrate access to the active site and set the substrate into the correct geometry for the catalytic process.…”

mentioning

confidence: 99%

See 1 more Smart Citation

Crystal Structure of an Active Form of BACE1, an Enzyme Responsible for Amyloid β Protein Production

Shimizu

Tosaki

Kaneko

et al. 2008

Molecular and Cellular Biology

176

175

View full text Add to dashboard Cite

BACE1 (␤-secretase) is a transmembrane aspartic protease that cleaves the ␤-amyloid precursor protein and generates the amyloid ␤ peptide (A␤). BACE1 cycles between the cell surface and the endosomal system many times and becomes activated interconvertibly during its cellular trafficking, leading to the production of A␤. Here we report the crystal structure of the catalytically active form of BACE1. The active form has novel structural features involving the conformation of the flap and subsites that promote substrate binding. The functionally essential residues and water molecules are well defined and play a key role in the iterative activation of BACE1. We further describe the crystal structure of the dehydrated form of BACE1, showing that BACE1 activity is dependent on the dynamics of a catalytically required Asp-bound water molecule, which directly affects its catalytic properties. These findings provide insight into a novel regulation of BACE1 activity and elucidate how BACE1 modulates its activity during cellular trafficking.

show abstract

“…In the x-ray structure of BACE1 (Protein Data Bank code 1W50) (41), the 10s loop is positioned between the third strand and insert F segments. The molecular dynamics simulation shows that the Gln 12 residue of the 10s loop mediates interactions between the third strand and insert F. In WTBACE1, the backbone and the side chain of Gln 12 (10s loop) form hydrogen bonds with the side chains of Ser 113 (third strand) and Glu…”

Section: Bace1-gpi Chimeras With Different Gpi Anchors Elicit Reducedmentioning

confidence: 99%

Loss of Cleavage at β′-Site Contributes to Apparent Increase in β-Amyloid Peptide (Aβ) Secretion by β-Secretase (BACE1)-Glycosylphosphatidylinositol (GPI) Processing of Amyloid Precursor Protein

Vetrivel

Barman

Chen

et al. 2011

Journal of Biological Chemistry

View full text Add to dashboard Cite

Several lines of evidence implicate lipid raft microdomains inAlzheimer disease-associated ␤-amyloid peptide (A␤) production. Notably, targeting ␤-secretase (␤-site amyloid precursor protein (APP)-cleaving enzyme 1 (BACE1)) exclusively to lipid rafts by the addition of a glycosylphosphatidylinositol (GPI) anchor to its ectodomain has been reported to elevate A␤ secretion. Paradoxically, A␤ secretion is not reduced by the expression of non-raft resident S-palmitoylation-deficient BACE1 (BACE1-4C/A (C474A/C478A/C482A/C485A)). We addressed this apparent discrepancy in raft microdomain-associated BACE1 processing of APP in this study. As previously reported, we found that expression of BACE1-GPI elevated A␤ secretion as compared with wild-type BACE1 (WTBACE1) or BACE1-4C/A. However, this increase occurred without any difference in the levels of APP ectodomain released following BACE1 cleavage (soluble APP␤), arguing against an overall increase in BACE1 processing of APP per se. Further analysis revealed that WTBACE1 cleaves APP at ␤-and ␤-sites, generating ؉1 and ؉11 ␤-C-terminal fragments and secreting intact as well as N-terminally truncated A␤. In contrast, three different BACE1-GPI chimeras preferentially cleaved APP at the ␤-site, mainly generating ؉1 ␤-C-terminal fragment and secreting intact A␤. As a consequence, cells expressing BACE1-GPI secreted relatively higher levels of intact A␤ without an increase in BACE1 processing of APP. Markedly reduced cleavage at ␤-site exhibited by BACE1-GPI was cell type-independent and insensitive to subcellular localization of APP or the pathogenic KM/NL mutant. We conclude that the apparent elevation in A␤ secretion by BACE1-GPI is mainly attributed to preferential cleavage at the ␤-site and failure to detect ؉11 A␤ species secreted by cells expressing WTBACE1.

show abstract

Apo and Inhibitor Complex Structures of BACE (β-secretase)

Cited by 181 publications

References 52 publications

Discovery of AZD3839, a Potent and Selective BACE1 Inhibitor Clinical Candidate for the Treatment of Alzheimer Disease

Discovery of AZD3839, a Potent and Selective BACE1 Inhibitor Clinical Candidate for the Treatment of Alzheimer Disease

Crystal Structure of an Active Form of BACE1, an Enzyme Responsible for Amyloid β Protein Production

Loss of Cleavage at β′-Site Contributes to Apparent Increase in β-Amyloid Peptide (Aβ) Secretion by β-Secretase (BACE1)-Glycosylphosphatidylinositol (GPI) Processing of Amyloid Precursor Protein

Contact Info

Product

Resources

About