847SARS-CoV-2 Spike - human ACE2 receptor complexSARS-CoV-2 Spike - human ACE2-SLC6A19 complexSARS-CoV Spike - human ACE2 receptor complex59BromhexineChloroquineHydroxychloroquineN-(2-Aminoethyl)-1-aziridineethanamineSPP1148the neurotransmitter:sodium symporter (nss) familythe angiotensin-converting enzyme 2 (ace2) family115 N-Linked glycans (3 sites), 1 O-Fuc glycan, 14 O-Linked glycans (1 site)8 sites, 161 glycans19 sites, 218 N-linked glycans (8 sites), 35 O-linked glycans (11 sites)2 sequenced antibodies1302 antibodies from 46 providershumanACE2Tissue enhanced (gallbladder, intestine, kidney)geneEukaryota26812681Metabolism of Angiotensinogen to AngiotensinsAttachment and EntryPotential therapeutics for SARSAttachment and EntryInduction of Cell-Cell Fusion35 hits in 793 CRISPR screenshumanTchemproteinExpressed in ileal mucosa and 94 other tissuesbaseline and differentialHSM2_ACECollectrin_domPeptidase_M2ANGIOTENSIN-CONVERTING ENZYMEANGIOTENSIN-CONVERTING ENZYME 2CollectrinPeptidase_M2PEPDIPTASEAMetalloproteases ('zincins'), catalytic domainCOLLECTRIN_LIKEPEPTIDASE_M2ZINC_PROTEASEAngiotensin-converting enzyme 23.4.17.23Angiotensin-converting enzyme homologACEHAngiotensin-converting enzyme-related carboxypeptidaseACE-related carboxypeptidase3.4.17.-Metalloprotease MPROT15Processed angiotensin-converting enzyme 2ACE2UNQ868/PRO1885Essential counter-regulatory carboxypeptidase of the renin-angiotensin hormone system that is a critical regulator of blood volume, systemic vascular resistance, and thus cardiovascular homeostasis (PubMed:27217402). Converts angiotensin I to angiotensin 1-9, a nine-amino acid peptide with anti-hypertrophic effects in cardiomyocytes, and angiotensin II to angiotensin 1-7, which then acts as a beneficial vasodilator and anti-proliferation agent, counterbalancing the actions of the vasoconstrictor angiotensin II (PubMed:10969042, PubMed:10924499, PubMed:11815627, PubMed:19021774, PubMed:14504186). Also removes the C-terminal residue from three other vasoactive peptides, neurotensin, kinetensin, and des-Arg bradykinin, but is not active on bradykinin (PubMed:10969042, PubMed:11815627). Also cleaves other biological peptides, such as apelins (apelin-13, [Pyr1]apelin-13, apelin-17, apelin-36), casomorphins (beta-casomorphin-7, neocasomorphin) and dynorphin A with high efficiency (PubMed:11815627, PubMed:27217402, PubMed:28293165). In addition, ACE2 C-terminus is homologous to collectrin and is responsible for the trafficking of the neutral amino acid transporter SL6A19 to the plasma membrane of gut epithelial cells via direct interaction, regulating its expression on the cell surface and its catalytic activity (PubMed:18424768, PubMed:19185582).(Microbial infection) Acts as a receptor for human coronaviruses SARS-CoV and SARS-CoV-2, as well as human coronavirus NL63/HCoV-NL63.Non-functional as a carboxypeptidase.(Microbial infection) Non-functional as a receptor for human coronavirus SARS-CoV-2.Binds 1 zinc ion per subunit.Binds 1 Cl(-) ion per subunit.Regulated by chloride and fluoride, but not bromide (PubMed:11815627). Chloride increases angiotensin I and decreases angiotensin II cleavage (PubMed:19021774). Inhibited by MLN-4760, cFP_Leu, and EDTA (PubMed:15231706, PubMed:10924499), but not by the ACE inhibitors lisinopril, captopril and enalaprilat (PubMed:10969042, PubMed:10924499). Highly potent and selective in vitro ACE2 inhibitors were identified (PubMed:12358520).kcat is 0.034 sec(-1) with angiotensin I as substrate. kcat is 3.5 sec(-1) with angiotensin II as substrate. kcat is 13 sec(-1) with apelin-13 as substrate. kcat is 62 sec(-1) with [des-Arg(9)]-bradykinin as substrate. kcat is 26 sec(-1) with Lys-[des-Arg(9)]-bradykinin as substrate. kcat is 6.8 sec(-1) with beta-casomorphin as substrate. kcat is 16 sec(-1) with dynorphin A-(1-13) as substrate. kcat is 57 sec(-1) with neurotensin-(1-8) as substrate (PubMed:11815627). kcat is 19.1 sec(-1) with [Pyr1]apelin-13 as substrate. kcat is 7.7 sec(-1) with apelin-17 as substrate (PubMed:27217402).6.9 uM for angiotensin I2 uM for angiotensin II6.8 uM for apelin-13290 uM for [des-Arg(9)]-bradykinin130 uM for Lys-[des-Arg(9)]-bradykinin31 uM for beta-casomorphin5.5 uM for dynorphin A-(1-13)300 uM for neurotensin-(1-8)58.6 uM for angiotensin II12 uM for [Pyr1]apelin-1319 uM for apelin-1728.7 nmol/min/mg enzyme with angiotensin II as substrateOptimum pH is 6.5 in the presence of 1 M NaCl. Active from pH 6 to 9.Homodimer (PubMed:32132184). Interacts with the catalytically active form of TMPRSS2 (PubMed:21068237). Interacts with SLC6A19; this interaction is essential for expression and function of SLC6A19 in intestine (By similarity). Interacts with ITGA5:ITGB1 (PubMed:15276642, PubMed:33102950). Probably interacts (via endocytic sorting signal motif) with AP2M1; the interaction is inhibited by phosphorylation of Tyr-781 (PubMed:33436498). Interacts (via PDZ-binding motif) with NHERF1 (via PDZ domains); the interaction may enhance ACE2 membrane residence (PubMed:34189428).(Microbial infection) Interacts with SARS coronavirus/SARS-CoV spike protein.(Microbial infection) Interacts with SARS coronavirus-2/SARS-CoV-2 spike protein (via RBD domain).(Microbial infection) Interacts with human coronavirus NL63 spike protein.(Microbial infection) Interacts with human coronavirus NL63/HCoV-NL63 spike glycoprotein.(Microbial infection) Interacts with SARS coronavirus-2/SARS-CoV-2 spike protein; the interaction is increased by AVP/Arg-vasopressin with which they may form a complex.Detected in both cell membrane and cytoplasm in neurons.Expressed in endothelial cells from small and large arteries, and in arterial smooth muscle cells (at protein level) (PubMed:15141377). Expressed in enterocytes of the small intestine, Leydig cells and Sertoli cells (at protein level) (PubMed:15141377). Expressed in the renal proximal tubule and the small intestine (at protein level) (PubMed:18424768). Expressed in heart, kidney, testis, and gastrointestinal system (at protein level) (PubMed:10969042, PubMed:10924499, PubMed:15231706, PubMed:12459472, PubMed:15671045, PubMed:32715618, PubMed:32170560). In lung, expressed at low levels in some alveolar type 2 cells, the expression seems to be individual-specific (at protein level) (PubMed:32425701, PubMed:15141377, PubMed:32715618, PubMed:32170560, PubMed:33432184). Expressed in nasal epithelial cells (at protein level) (PubMed:33432184, PubMed:32333915). Coexpressed with TMPRSS2 within some lung alveolar type 2 cells, ileal absorptive enterocytes, intestinal epithelial cells, cornea, gallbladder and nasal goblet secretory cells (PubMed:32413319, PubMed:32327758, PubMed:32358202). Coexpressed with TMPRSS4 within mature enterocytes (PubMed:32404436).Expressed in nasal and bronchial epithelial cells (at protein level).Up-regulated in failing heart (PubMed:14504186, PubMed:15151696, PubMed:15671045). Expression is induced by IFNA and IFNG (PubMed:32413319, PubMed:32425701). Exposure to cigarette smoke increases expression in lungs (PubMed:32425701). Expression is decreased in nasal and bronchial epithelium of individuals with allergy after allergen challenge (PubMed:32333915). IL13 stimulation decreases expression in nasal and bronchial epithelium (PubMed:32333915).Not induced by interferons such as IFNA, IFNB and IFNG.Expression is induced by interferons such as IFNA, IFNB and IFNG. It seems that isoform 2 is an interferon-stimulated gene (ISG) but not isoform 1.(Microbial infection) In airway epithelial cells, expression is increased upon influenza A virus infection (PubMed:32413319).(Microbial infection) In airway epithelial cells, expression is induced by viruses such rhinoviruses and influenza virus.(Microbial infection) Induced by human coronavirus SARS-CoV-2.The extracellular region of the ACE2 enzyme is composed of two domains. The first is a zinc metallopeptidase domain (residues 19-611). The second domain is located at the C-terminus (residues 612-740) and is 48% identical to human collectrin.The cytoplasmic tail contains several linear motifs such as LIR, PDZ-binding, PTB and endocytic sorting signal motifs that would allow interaction with proteins that mediate endocytic trafficking and autophagy.N-glycosylation on Asn-90 may limit SARS infectivity.Proteolytic cleavage by ADAM17 generates a secreted form (PubMed:15983030, PubMed:33713620). Also cleaved by serine proteases: TMPRSS2, TMPRSS11D and HPN/TMPRSS1.Phosphorylated. Phosphorylation at Tyr-781 probably inhibits interaction with AP2M1 and enables interactions with proteins containing SH2 domains.An engeneered stable, dimeric and secreted receptor with combined mutations that increase the affinity for human coronavirus SARS-CoV-2 spike protein shows potent SARS-CoV and SARS-CoV-2 neutralization in vitro.Belongs to the peptidase M2 family.117Angiotensin-converting enzyme 29074518805Processed angiotensin-converting enzyme 280106708Extracellular740Helical741761Cytoplasmic762Peptidase M219607Collectrin-like614Interaction with SARS-CoV spike glycoprotein3041Interaction with SARS-CoV spike glycoprotein8284Interaction with SARS-CoV spike glycoprotein353357Essential for cleavage by ADAM17652659Essential for cleavage by TMPRSS11D and TMPRSS2697716Disordered772LIR778786SH2-binding781785Endocytic sorting signal784PTB792795PDZ-binding803Polar residuesProton acceptor375Proton donor505169273345346374378402477481515PhosphotyrosinePhosphoserine783N-linked (GlcNAc...) asparagine53N-linked (GlcNAc...) asparagine90N-linked (GlcNAc...) asparagine103N-linked (GlcNAc...) asparagine322N-linked (GlcNAc...) asparagine432N-linked (GlcNAc...) asparagine546N-linked (GlcNAc...) asparagine690133141344361530542In isoform 2.MREAGWDKGG356R26V468S638D720Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.PSlightly inhibits interaction with SARS-CoV spike glycoprotein.KAE24Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.TIncreases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.V25Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein. In sACE2.v2.2; increases interaction with RBD domain of SARS-CoV-2 spike protein; when associated with Y-330 and L-386.Y27Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.F29Abolishes interaction with SARS-CoV spike glycoprotein.D31Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.YIncreases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.D33Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.A34No effect on interaction with SARS-CoV spike glycoprotein.A37No effect on interaction with SARS-CoV spike glycoprotein.A38Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.R39Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.D40Strongly inhibits interaction with SARS-CoV spike glycoprotein.AIncreases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.RIncreases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.L42Slightly inhibits interaction with SARS-CoV spike glycoprotein.D68Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.V69Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.Y72Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.K75Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.T76Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.T79Inhibits interaction with SARS-CoV spike glycoprotein.NFSIncreases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.P89Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.QIncreases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.P91Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.Q92No effect on interaction with SARS-CoV spike glycoprotein.P110No effect on interaction with SARS-CoV spike glycoprotein.SM135136No effect on interaction with SARS-CoV spike glycoprotein.R160About 95% loss of angiotensin I cleavage.QNo effect on interaction with SARS-CoV spike glycoprotein.D192No effect on interaction with SARS-CoV spike glycoprotein.D219No effect on interaction with SARS-CoV spike glycoprotein.Q239About 95% loss of angiotensin I cleavage.Q271Complete loss of enzyme activity. Does not affect amino acid transport activity of SLC6A19.QNo effect on interaction with SARS-CoV spike glycoprotein.D309No effect on interaction with SARS-CoV spike glycoprotein.A312No effect on interaction with SARS-CoV spike glycoprotein.A324Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.PIncreases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.P325Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein. In sACE2.v2.2; increases interaction with RBD domain of SARS-CoV-2 spike protein; when associated with Y-27 and L-386.Y330No effect on interaction with SARS-CoV spike glycoprotein.DDR338340Complete loss of enzyme activity.ANo effect on interaction with SARS-CoV spike glycoprotein.A350Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein.F351Abolishes interaction with SARS-CoV spike glycoprotein.HADStrongly inhibits interaction with SARS-CoV spike glycoprotein.A355Strongly inhibits interaction with SARS-CoV spike glycoprotein.ANo effect on interaction with SARS-CoV spike glycoprotein.KA359Slightly inhibits interaction with SARS-CoV spike glycoprotein.A383Increases slightly the interaction with RBD domain of SARS-CoV-2 spike protein. In sACE2.v2.2; increases interaction with RBD domain of SARS-CoV-2 spike protein; when associated with Y-27 and Y-330.L386Slightly inhibits interaction with SARS-CoV spike glycoprotein.A389Increases very slightly the interaction with RBD domain of SARS-CoV-2 spike protein.DSlightly inhibits interaction with SARS-CoV spike glycoprotein.A393Increases very slightly the interaction with RBD domain of SARS-CoV-2 spike protein.KSlightly inhibits interaction with SARS-CoV spike glycoprotein.PSN425427No effect on interaction with SARS-CoV spike glycoprotein.QDK465467About 80% loss of angiotensin I cleavage.QComplete loss of enzyme activity.AAbout 50% loss of angiotensin I cleavage but two-fold greater activity with angiotensin II.Q514Increases very slightly the interaction with RBD domain of SARS-CoV-2 spike protein.G518Slightly inhibits interaction with SARS-CoV spike glycoprotein.S559No effect on interaction with SARS-CoV spike glycoprotein.T603Loss of interaction with NHERF1.AAAA802HD508R63123525677788587100104107129131134137143144146148154158171173193196198199204205207213215220251253255258260264266267276278279282284287294297298300304316317319327337339347352366384385387390392396399400413415420422426446449466470472473483486488494496499502504507531532534539541548558562566574575578582598600602609612615618622624627629637657667669670673677686694706715719724765substratecatalyticfalse8false2false5false2false3false3false4false2false6false4false19false5false2false3false2false2false4false7false2false3false4true4true2true4true4true254true2true57true3true2true9ACE2AGTAGTAP2M1APPCLEC4MDEFA5GRM2HSPA5ITGB1KDM1AKNG1NTSPDZK1SFTPDSHANK1SLC6A19SLC9A3R1SNX27TMPRSS2VIMKpna2SSSSSSSSS2005-08-022true92463906dc56d5c9c5513eef859ee82e802671longMSSSSWLLLSLVAVTAAQSTIEEQAKTFLDKFNHEAEDLFYQSSLASWNYNTNITEENVQNMNNAGDKWSAFLKEQSTLAQMYPLQEIQNLTVKLQLQALQQNGSSVLSEDKSKRLNTILNTMSTIYSTGKVCNPDNPQECLLLEPGLNEIMANSLDYNERLWAWESWRSEVGKQLRPLYEEYVVLKNEMARANHYEDYGDYWRGDYEVNGVDGYDYSRGQLIEDVEHTFEEIKPLYEHLHAYVRAKLMNAYPSYISPIGCLPAHLLGDMWGRFWTNLYSLTVPFGQKPNIDVTDAMVDQAWDAQRIFKEAEKFFVSVGLPNMTQGFWENSMLTDPGNVQKAVCHPTAWDLGKGDFRILMCTKVTMDDFLTAHHEMGHIQYDMAYAAQPFLLRNGANEGFHEAVGEIMSLSAATPKHLKSIGLLSPDFQEDNETEINFLLKQALTIVGTLPFTYMLEKWRWMVFKGEIPKDQWMKKWWEMKREIVGVVEPVPHDETYCDPASLFHVSNDYSFIRYYTRTLYQFQFQEALCQAAKHEGPLHKCDISNSTEAGQKLFNMLRLGKSEPWTLALENVVGAKNMNVRPLLNYFEPLFTWLKDQNKNSFVGWSTDWSPYADQSIKVRISLKSALGDKAYEWNDNEMYLFRSSVAYAMRQYFLKVKNQMILFGEEDVRVANLKPRISFNFFVTAPKNVSDIIPRTEVEKAIRMSRSRINDAFRLNDNSLEFLGIQPTLGPPNQPPVSIWLIVFGVVMGVIVVGIVILIFTGIRDRKKKNKARSGENPYASIDISKGENNPGFQNTDDVQTSF2deltadACE2shortMREAGWDKGGRILMCTKVTMDDFLTAHHEMGHIQYDMAYAAQPFLLRNGANEGFHEAVGEIMSLSAATPKHLKSIGLLSPDFQEDNETEINFLLKQALTIVGTLPFTYMLEKWRWMVFKGEIPKDQWMKKWWEMKREIVGVVEPVPHDETYCDPASLFHVSNDYSFIRYYTRTLYQFQFQEALCQAAKHEGPLHKCDISNSTEAGQKLFNMLRLGKSEPWTLALENVVGAKNMNVRPLLNYFEPLFTWLKDQNKNSFVGWSTDWSPYADQSIKVRISLKSALGDKAYEWNDNEMYLFRSSVAYAMRQYFLKVKNQMILFGEEDVRVANLKPRISFNFFVTAPKNVSDIIPRTEVEKAIRMSRSRINDAFRLNDNSLEFLGIQPTLGPPNQPPVSIWLIVFGVVMGVIVVGIVILIFTGIRDRKKKNKARSGENPYASIDISKGENNPGFQNTDDVQTSFtruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetruetrue2007-05-292023-06-28148B3GN5_HUMANMolecular cloning and characterization of UDP-GlcNAc:lactosylceramide beta 1,3-N-acetylglucosaminyltransferase (beta 3Gn-T5), an essential enzyme for the expression of HNK-1 and Lewis X epitopes on glycolipids.Togayachi A.Akashima T.Ookubo R.Kudo T.Nishihara S.Iwasaki H.Natsume A.Mio H.Inokuchi J.Irimura T.Sasaki K.Narimatsu H.doi:10.1074/jbc.m0113692002001J. Biol. Chem.27622032-22040NUCLEOTIDE SEQUENCE [MRNA]CATALYTIC ACTIVITYTISSUE SPECIFICITYINDUCTIONFUNCTIONCloning of a mouse beta 1,3 N-acetylglucosaminyltransferase GlcNAc(beta 1,3)Gal(beta 1,4)Glc-ceramide synthase gene encoding the key regulator of lacto-series glycolipid biosynthesis.Henion T.R.Zhou D.Wolfer D.P.Jungalwala F.B.Hennet T.doi:10.1074/jbc.m1029792002001J. Biol. Chem.27630261-30269NUCLEOTIDE SEQUENCE [MRNA]CATALYTIC ACTIVITYFUNCTIONBennett E.P.2000-12EMBL/GenBank/DDBJNUCLEOTIDE SEQUENCE [MRNA]Totoki Y.Toyoda A.Takeda T.Sakaki Y.Tanaka A.Yokoyama S.Ohara O.Nagase T.Kikuno R.F.2005-03EMBL/GenBank/DDBJNUCLEOTIDE SEQUENCE [LARGE SCALE MRNA]BrainMural R.J.Istrail S.Sutton G.G.Florea L.Halpern A.L.Mobarry C.M.Lippert R.Walenz B.Shatkay H.Dew I.Miller J.R.Flanigan M.J.Edwards N.J.Bolanos R.Fasulo D.Halldorsson B.V.Hannenhalli S.Turner R.Yooseph S.Lu F.Nusskern D.R.Shue B.C.Zheng X.H.Zhong F.Delcher A.L.Huson D.H.Kravitz S.A.Mouchard L.Reinert K.Remington K.A.Clark A.G.Waterman M.S.Eichler E.E.Adams M.D.Hunkapiller M.W.Myers E.W.Venter J.C.2005-09EMBL/GenBank/DDBJNUCLEOTIDE SEQUENCE [LARGE SCALE GENOMIC DNA]The status, quality, and expansion of the NIH full-length cDNA project: the Mammalian Gene Collection (MGC).The MGC Project Teamdoi:10.1101/gr.25965042004Genome Res.142121-2127NUCLEOTIDE SEQUENCE [LARGE SCALE MRNA]Functional Glycomics Gateway - GTase; Beta1,3-N-acetylglucosaminyltransferase 5Frameshift.52Glycosyltransferase Family 311 site, No reported glycans1 site