Beta-secretase 1

BACE1
Available structures PDB Ortholog search:PDBeRCSB List of PDB id codes 1FKN,1M4H,1PY1,1SGZ,1TQF,1UJJ,1UJK,1W50,1W51,1XN2,1XN3,1XS7,1YM2,1YM4,2B8L,2B8V,2F3E,2F3F,2FDP,2G94,2HIZ,2HM1,2IQG,2IRZ,2IS0,2NTR,2OAH,2OF0,2OHK,2OHL,2OHM,2OHN,2OHP,2OHQ,2OHR,2OHS,2OHT,2OHU,2P4J,2P83,2P8H,2PH6,2PH8,2Q11,2Q15,2QK5,2QMD,2QMF,2QMG,2QP8,2QU2,2QU3,2QZK,2QZL,2VA5,2VA6,2VA7,2VIE,2VIJ,2VIY,2VIZ,2VJ6,2VJ7,2VJ9,2VKM,2VNM,2VNN,2WEZ,2WF0,2WF1,2WF2,2WF3,2WF4,2WJO,2XFI,2XFJ,2XFK,2ZDZ,2ZE1,2ZHR,2ZHS,2ZHT,2ZHU,2ZHV,2ZJH,2ZJI,2ZJJ,2ZJK,2ZJL,2ZJM,2ZJN,3BRA,3BUF,3BUG,3BUH,3CIB,3CIC,3CID,3CKP,3CKR,3DM6,3DUY,3DV1,3DV5,3EXO,3FKT,3H0B,3HVG,3HW1,3I25,3IGB,3IN3,3IN4,3IND,3INE,3INF,3INH,3IVH,3IVI,3IXJ,3IXK,3KYR,3L38,3L3A,3LHG,3LNK,3MSJ,3MSK,3MSL,3N4L,3NSH,3OOZ,3QI1,3R1G,3RSV,3RTM,3RVI,3S2O,3S7L,3S7M,3TPJ,3TPL,3TPP,3TPR,3UDH,3UDJ,3UDK,3UDM,3UDN,3UDP,3UDQ,3UDR,3UDY,3UFL,3UQP,3UQR,3UQU,3UQW,3UQX,3VEU,3VF3,3VG1,3VV6,3VV7,3ZMG,3ZOV,4ACU,4ACX,4AZY,4B00,4B05,4B0Q,4B1C,4B1D,4B1E,4B70,4B72,4B77,4B78,4BEK,4BFD,4D83,4D85,4D88,4D89,4D8C,4DH6,4DI2,4DJU,4DJV,4DJW,4DJX,4DJY,4DPF,4DPI,4DUS,4DV9,4DVF,4EWO,4EXG,4FCO,4FGX,4FM7,4FM8,4FRI,4FRJ,4FRK,4FRS,4FS4,4FSE,4FSL,4GMI,4H1E,4H3F,4H3G,4H3I,4H3J,4HA5,4HZT,4I0E,4I0F,4I0G,4I0H,4I0J,4I0Z,4I10,4I11,4I12,4I1C,4J0T,4J0V,4J0Y,4J0Z,4J17,4J1C,4J1E,4J1F,4J1H,4J1I,4J1K,4JOO,4JP9,4JPC,4JPE,4K8S,4K9H,4KE0,4KE1,3K5C,3K5D,3K5F,3K5G,3KMX,3KMY,3KN0,3L58,3L59,3L5B,3L5C,3L5D,3L5E,3L5F,3LPI,3LPJ,3LPK,3OHF,3OHH,3PI5,3QBH,3R2F,3RSX,3RTH,3RTN,3RU1,3SKF,3SKG,3U6A,4GID,4LXA,4LXK,4LXM,3WB4,3WB5,4I0D,4I0I,4IVS,4IVT,4J0P,4L7G,4L7H,4L7J,4LC7,4N00,4PZW,4PZX,4R5N,4R8Y,4R91,4R92,4R93,4R95,4RCD,4RCE,4RCF,4RRN,4RRO,4RRS,4WY1,4WY6,4X2L,4X7I,4XKX,4XXS,4YBI,4TRW,4TRZ,4ZSM,4ZSP,4ZSQ,4ZSR,4TRY,4ZPF,4ZPG,5CLM,5F01,5EZZ,5DQC,5F00,5EZX,5HE7,5HD0,5HDX,5HDV,5HE5,5HE4,5HDU,5HDZ,5I3X,5I3W,5I3V,5IE1,5I3Y,5ENK
Identifiers
Aliases	BACE1,ASP2, BACE, HSPC104, beta-secretase 1
External IDs	OMIM:604252;MGI:1346542;HomoloGene:8014;GeneCards:BACE1;OMA:BACE1 - orthologs
EC number	3.4.23.46
Gene location (Human) Chr. Chromosome 11 (human)[1] Band 11q23.3 Start 117,285,232bp[1] End 117,316,259bp[1]
Gene location (Mouse) Chr. Chromosome 9 (mouse)[2] Band 9|9 A5.2 Start 45,749,878bp[2] End 45,775,697bp[2]
RNA expressionpattern Bgee Human Mouse(ortholog) Top expressed in inferior ganglion of vagus nerve body of pancreas C1 segment corpus callosum stromal cell of endometrium subthalamic nucleus medulla oblongata ventral tegmental area inferior olivary nucleus superior vestibular nucleus Top expressed in external carotid artery internal carotid artery Rostral migratory stream medullary collecting duct epithelium of lens facial motor nucleus vas deferens ciliary body anterior horn of spinal cord renal corpuscle More reference expression data BioGPS More reference expression data
Gene ontology Molecular function endopeptidase activity amyloid-beta binding beta-aspartyl-peptidase activity protein binding enzyme binding hydrolase activity peptidase activity aspartic-type endopeptidase activity Cellular component multivesicular body late endosome endoplasmic reticulum lumen membrane plasma membrane cell surface axon endoplasmic reticulum Golgi-associated vesicle lumen endosome membrane cytoplasmic vesicle membrane cytoplasmic vesicle integral component of plasma membrane membrane raft Golgi apparatus integral component of membrane endosome trans-Golgi network lysosome early endosome synaptic vesicle dendrite soma recycling endosome hippocampal mossy fiber to CA3 synapse presynapse Biological process protein catabolic process proteolysis amyloid-beta metabolic process membrane protein ectodomain proteolysis modulation of chemical synaptic transmission response to radiation response to lead ion positive regulation of neuron apoptotic process detection of mechanical stimulus involved in sensory perception of pain prepulse inhibition cellular response to copper ion cellular response to manganese ion cellular response to amyloid-beta regulation of synaptic vesicle exocytosis Sources:Amigo/QuickGO
Orthologs Species Human Mouse Entrez 23621 23821 Ensembl ENSG00000186318 ENSMUSG00000032086 UniProt P56817 P56818 RefSeq (mRNA) NM_138973 NM_001207048 NM_001207049 NM_012104 NM_138971 NM_138972 NM_001145947 NM_011792 RefSeq (protein) NP_001193977 NP_001193978 NP_036236 NP_620427 NP_620428 NP_620429 NP_036236.1 NP_001139419 NP_035922 Location (UCSC) Chr 11: 117.29 – 117.32 Mb Chr 9: 45.75 – 45.78 Mb PubMedsearch [3] [4]
Wikidata
View/Edit Human View/Edit Mouse

Beta-secretase 1,also known asbeta-site amyloid precursor protein cleaving enzyme 1,beta-site APP cleaving enzyme 1(BACE1),membrane-associated aspartic protease 2,memapsin-2,aspartyl protease 2,andASP2,is anenzymethat in humans is encoded by theBACE1gene.^[5]Expression of BACE1 is observed mainly inneuronsandoligodendrocytes.^[6]

BACE1 is anaspartic acid proteaseimportant in the formation ofmyelin sheathsin peripheral nerve cells: in mice the expression of BACE1 is high in the postnatal stages, whenmyelinationoccurs.^[7]Thetransmembrane proteincontains two active siteaspartateresidues in itsextracellularprotein domainand may function as adimer,its cytoplasmic tail is required for the correct maturation and an efficient intracellular trafficking, but does not affect the activity. It is produced as apro-enzyme,the endoproteolitc removal occurs after BACE leavesendoplasmic reticulum,in theGolgi apparatus.In addition thepro-peptidereceives additional sugars to increase the molecular mass.^[8]and the tail became apalmitoylated.^{[citation needed]}

The BACE1 expression is influenced by the inflammatory state: duringADthecytokinesreduce thePPAR1an inhibitor of BACE1 mRNA.^{[citation needed]}

BACE1 is the major beta secretase for the generation ofamyloid-βpeptidesin the neurons.^[9]

Generation of the 40 or 42amino acid-longamyloid-βpeptidesthat aggregate in thebrainof Alzheimer's patients requires two sequential cleavages of theamyloid precursor protein(APP). Extracellular cleavage of APP by BACE1 creates a soluble extracellular fragment and a cell membrane-bound fragment referred to as C99. Cleavage of C99 within its transmembrane domain byγ-secretasereleases the intracellular domain of APP and produces amyloid-β. Sincegamma-secretasecleaves APP closer to thecell membranethan BACE1 does, it removes a fragment of the amyloid-β peptide. Initial cleavage of APP by α-secretase rather than BACE1 prevents eventual generation of amyloid-β, formingP3,this demonstrates that BACE1 andAlpha secretasecompete for the APP processing.

Unlike APP and thepresenilinproteins important in γ-secretase, no knownmutationsin thegeneencoding BACE1 cause early-onset,familial Alzheimer's disease,which is a rare form of the disorder. However, levels of this enzyme have been shown to be elevated in the far more common late-onset sporadic Alzheimer's.BACE2is a closehomologof BACE1 with no reported APP cleavagein vivo.

The physiological purpose of BACE's cleavage of APP and other transmembrane proteins is unknown: some studies observed that BACE1 is involved inmyelination(it is co-express withneuregulin 1type III). In a manner analogous to APP processing, theVGSCsubunit beta is a substrate for BACE1.^[10]

However a single residue mutation in APP reduces the ability of BACE1 to cleave it to produce amyloid-beta and reduces the risk of Alzheimer's disease and other cognitive declines.^[11][12]

Drugs to block this enzyme (BACE inhibitors) in theory would prevent the buildup of beta-amyloid and (per theAmyloid hypothesis) may help slow or stop Alzheimer's disease.^[13]

Several companies are in the early stages of development and testing of this potential class of treatment.^[14][15]In March 2008 phase I results were reported for CoMentis Inc's candidate CTS-21166.^[16]

In April 2012Merck & Co.,Inc reported phase I results for its candidateverubecestat(MK-8931).^[17]Merck began a Phase II/III trial of MK-8931 in December, 2012 estimated to be completed in July 2019.^[18]In February 2017, Merck halted its late-stage trial of verubecestat for mild to moderate Alzheimer's disease after it was reported as having "virtually no chance" of working according to an independent panel of experts. This came just three months after Eli Lilly & Co. announced its own setback withsolanezumab.

In September 2014AstraZenecaandEli Lilly and Companyannounced an agreement to codeveloplanabecestat(AZD3293).^[19]A pivotal Phase II/III clinical trial of lanabecestat started in late 2014,^[20]but was halted in 2018 before its planned conclusion due to poor results.^[21]

Another BACE1 inhibitor that has reached phase II trials is the Eli Lilly's inhibitor LY2886721. The data on phase I trial were first presented at the Alzheimer's Association International conference in 2012. Daily dosing during 2 weeks, reduced BACE1 activity by 50–75% and CSF Aβ42 by 72% (Willis et al., 2012; Bowman Rogers and Strobel, 2013). Recently, Lilly reported that the phase II trial of LY2886721 was terminated due to liver abnormalities that were found in 4 out of 45 patients (Rogers, 2013). This toxicity, however, does not have to be related to the working mechanism of the inhibitor, but can represent off-target effects as the livers of BACE1 knockout mice are normal.

Tests in mice have indicated that BACE proteases, specifically BACE1, are necessary for the proper function ofmuscle spindles.^[22]These results raise the possibility that BACE inhibiting drugs currently being investigated for the treatment of Alzheimer's may have significant side effects related to impaired motor coordination,^[23]though BACE1knockoutmice are healthy.^[24]

BACE1 is distantly related to the pathogenic aspartic-acid proteaseplasmepsin,which is a potential target for future anti-malarial drugs.^[25]

• TheMEROPSonline database for peptidases and their inhibitors:A01.004
• beta-Secretase: Molecule of the MonthArchived2012-11-21 at theWayback Machine,by David Goodsell, RCSB Protein Data Bank
• HumanBACE1genome location andBACE1gene details page in theUCSC Genome Browser.
• Overview of all the structural information available in thePDBforUniProt:P56817(Human Beta-secretase 1) at thePDBe-KB.