CAZyme Information: MGYG000002373_01791

Basic Information

• Species: Clostridium septicum
• Lineage: Bacteria; Firmicutes_A; Clostridia; Clostridiales; Clostridiaceae; Clostridium; Clostridium septicum
• CAZyme ID: MGYG000002373_01791
• CAZy Family: CBM32
• CAZyme Description: hypothetical protein

CAZyme Property

Protein Length	CGC	Molecular Weight	Isoelectric Point
1747	MGYG000002373_20|CGC1	194171.97	4.4685

Genome Property

Genome Assembly ID	Genome Size	Genome Type	Country	Continent
MGYG000002373	3298966	Isolate	France	Europe

• Gene Location: Start: 12608; End: 17851 Strand: +

Full Sequence      

MQSLRKRKGIKRILPLFLVFAMMIGNVYTFANVNISAERENLALNKDAFASSEETTTLTA
SKVTDGQIDREGAKTSRWACERHEQNPWVAIDFGAKTKFNEVVIEWERKNINSYKIETSD
NRESWTTIYTGEKASAYRDIINVGEQDSRYVRVLVSGYSPSEEGSDISWETVSIYEIEVY
RNQNVSKPEAGVNVALNKTTTASSVETNNFTANKATDGLVDRTGAKSSRWASAVSSDDQW
LKVDLGENTQFENVVIEWERRNSPSYRIQVSEDDSTWIDIYTATSAPSNFRDVINLGEKV
SGRYVRLYIDEHISNSEGVDWNTVSVYELEIYNGSAPEPPKTADEVARNLTINELTPEDT
QLTMPTVPDGYGISFIGADYEEVIDYDMNIHKPLVNTKVVVNFEVTKGNEKATSPAIEVT
VPGANEVTGNNKPIVVPELREWAGKTGNFEVTESSRIVVNPSSEANLRKAVEVFAKDYKD
ILGREIEVVTSNEPNSGDFYFELTSNYPELRKEGYYMDVNDVLRVQANEEQGIFLSTRTI
LQILKQNTTYIPKGLVRDYPQYDVRGFMLDVGRKFVSLEYLYEIMKTMSWYKLNDFQVHL
NDNYIWLADDYGNEALENAYAAFRLESNDVGENGVKLTAQDGHYTKEEFGKFIDDSKLHG
VNIVPEFDTPGHALAFTKVHPNYAYEDGNGENAAMLDVTNPKVVEYIKGIFNEYMDGENP
VFRDSTIHIGTDEFYGNSEQYRKYADEMLKFIRDEKGSTPRLWGSLTRKNGSTPVTVEGV
EMNIWNTGWANPKVMYDAGYKLINTDDAYLYIVPGANYYKNYLDIQWLYNNWEVNKFSNG
TILPEGSPNMIGGMFALWNDLIDKRANGIVQYDIFDRIFPAIQVLSEKMWGEADDKNFNE
FKEAANKVALAPNTNPKYKVESATEKVVEYDFENATGNIANDKSGNNYNTVSANNAEITN
GSVNLNGENSYVKTPLKSIGPNYSISFSINRSAESNEEEQVIFESSEGSFKAVQKETGKL
GFSREAYDYSFNYTLPKGEWVDITIVGKMNKTELYVNGEYVDEISKSSTANKFGTFVFPL
EKIGSEEKSFKGSIDNLLVTNRASLEDPTKIPQEQMLATATSEHPNVGTEGLASFAIDGD
ETTIWHTNYNTSSPLPQSITLNLGGTYQVDRVSYLPRQSGGLNGNITGYELHVSTNGSDF
TKVKEGTFENNASLKTIKLDTSAEATHVKLVATEGVGGFASAAELNVYKTKEVVDPSPDP
SEVGFKVTANEEVKVGENFEIKVGTENLTSDNMYAMEFNVEYDRDKFEFTEGTSVDDSKY
IVRAAEKDGKLKVIVATKGVSLENNEDVVKLVFKAKATGENVAFNIVDGKLADGEGNEHA
LGNALVTTNVKEEAINPNPEVNKRALEIAIEYADEVVANGGLVGVVPAVVNEFNTALIEA
RIVYENENATAEEVDKAFNRLMKAIHMLEFKQGDKTELQNLVNIIEALDKTLYTPETWAN
LETALAKANSVLADENAMTEEVNTTFDELMDAFNKLEKAVDKTELQKMVNTVEALDKTLY
IPSTLEELEVALQKAKEVLANENATQKEVDKAFEDLVKAYGKIRLKPNKDMLNDLIKEVN
NIDLSKYTQGSVAKLNKELSKAMEVLNNEEATQKDVDKAVKNLRKAKDNLVAKGDNSQGN
QNNGNNNSGGNSNSGGSNSNGGNSNSTSGNKLNTIPQTGGMASAATVLVLGALASVAGVT
MIKKRKN

Enzyme Prediction     

No EC number prediction in MGYG000002373_01791.

CAZyme Signature Domains

Family	Start	End	Evalue	family coverage
GH20	556	891	1.3e-62	0.973293768545994
CBM32	198	329	7.4e-22	0.9435483870967742
CBM32	1122	1245	2.1e-21	0.9193548387096774
CBM32	49	177	2.3e-18	0.9193548387096774

CDD Domains     

Cdd ID	Domain	E-Value	qStart	qEnd	sStart	sEnd	Domain Description
cd06564	GH20_DspB_LnbB-like	2.17e-130	564	891	2	325	Glycosyl hydrolase family 20 (GH20) catalytic domain of dispersin B (DspB), lacto-N-biosidase (LnbB) and related proteins. Dispersin B is a soluble beta-N-acetylglucosamidase found in bacteria that hydrolyzes the beta-1,6-linkages of PGA (poly-beta-(1,6)-N-acetylglucosamine), a major component of the extracellular polysaccharide matrix. Lacto-N-biosidase hydrolyzes lacto-N-biose (LNB) type I oligosaccharides at the nonreducing terminus to produce lacto-N-biose as part of the GNB/LNB (galacto-N-biose/lacto-N-biose I) degradation pathway. The lacto-N-biosidase from Bifidobacterium bifidum has this GH20 domain, a carbohydrate binding module 32, and a bacterial immunoglobulin-like domain 2, as well as a YSIRK signal peptide and a G5 membrane anchor at the N and C termini, respectively. The GH20 hexosaminidases are thought to act via a catalytic mechanism in which the catalytic nucleophile is not provided by solvent or the enzyme, but by the substrate itself.
cd02742	GH20_hexosaminidase	5.24e-40	565	891	2	303	Beta-N-acetylhexosaminidases of glycosyl hydrolase family 20 (GH20) catalyze the removal of beta-1,4-linked N-acetyl-D-hexosamine residues from the non-reducing ends of N-acetyl-beta-D-hexosaminides including N-acetylglucosides and N-acetylgalactosides. These enzymes are broadly distributed in microorganisms, plants and animals, and play roles in various key physiological and pathological processes. These processes include cell structural integrity, energy storage, cellular signaling, fertilization, pathogen defense, viral penetration, the development of carcinomas, inflammatory events and lysosomal storage disorders. The GH20 enzymes include the eukaryotic beta-N-acetylhexosaminidases A and B, the bacterial chitobiases, dispersin B, and lacto-N-biosidase. The GH20 hexosaminidases are thought to act via a catalytic mechanism in which the catalytic nucleophile is not provided by the solvent or the enzyme, but by the substrate itself.
pfam00728	Glyco_hydro_20	1.79e-34	565	890	4	343	Glycosyl hydrolase family 20, catalytic domain. This domain has a TIM barrel fold.
cd06563	GH20_chitobiase-like	1.78e-33	565	903	4	355	The chitobiase of Serratia marcescens is a beta-N-1,4-acetylhexosaminidase with a glycosyl hydrolase family 20 (GH20) domain that hydrolyzes the beta-1,4-glycosidic linkages in oligomers derived from chitin. Chitin is degraded by a two step process: i) a chitinase hydrolyzes the chitin to oligosaccharides and disaccharides such as di-N-acetyl-D-glucosamine and chitobiose, ii) chitobiase then further degrades these oligomers into monomers. This GH20 domain family includes an N-acetylglucosamidase (GlcNAcase A) from Pseudoalteromonas piscicida and an N-acetylhexosaminidase (SpHex) from Streptomyces plicatus. SpHex lacks the C-terminal PKD (polycystic kidney disease I)-like domain found in the chitobiases. The GH20 hexosaminidases are thought to act via a catalytic mechanism in which the catalytic nucleophile is not provided by solvent or the enzyme, but by the substrate itself.
cd06562	GH20_HexA_HexB-like	1.11e-28	565	901	4	333	Beta-N-acetylhexosaminidases catalyze the removal of beta-1,4-linked N-acetyl-D-hexosamine residues from the non-reducing ends of N-acetyl-beta-D-hexosaminides including N-acetylglucosides and N-acetylgalactosides. The hexA and hexB genes encode the alpha- and beta-subunits of the two major beta-N-acetylhexosaminidase isoenzymes, N-acetyl-beta-D-hexosaminidase A (HexA) and beta-N-acetylhexosaminidase B (HexB). Both the alpha and the beta catalytic subunits have a TIM-barrel fold and belong to the glycosyl hydrolase family 20 (GH20). The HexA enzyme is a heterodimer containing one alpha and one beta subunit while the HexB enzyme is a homodimer containing two beta-subunits. Hexosaminidase mutations cause an inability to properly hydrolyze certain sphingolipids which accumulate in lysosomes within the brain, resulting in the lipid storage disorders Tay-Sachs and Sandhoff. Mutations in the alpha subunit cause in a deficiency in the HexA enzyme and result in Tay-Sachs, mutations in the beta-subunit cause in a deficiency in both HexA and HexB enzymes and result in Sandhoff disease. In both disorders GM(2) gangliosides accumulate in lysosomes. The GH20 hexosaminidases are thought to act via a catalytic mechanism in which the catalytic nucleophile is not provided by solvent or the enzyme, but by the substrate itself.

CAZyme Hits     

Hit ID	E-Value	Query Start	Query End	Hit Start	Hit End
AYE33718.1	0.0	1	1747	1	1747
QAS61873.1	0.0	1	1747	1	1747
ATD55826.1	0.0	1	1676	1	1675
SLK21750.1	0.0	1	1676	1	1675
QBJ76126.1	0.0	1	1676	1	1675

PDB Hits     

Hit ID	E-Value	Query Start	Query End	Hit Start	Hit End	Description
6JQF_A	1.46e-135	345	1094	2	726	Crystallizationanalysis of a beta-N-acetylhexosaminidase (Am2136) from Akkermansia muciniphila [Akkermansia muciniphila ATCC BAA-835]
4A41_A	6.44e-52	1111	1248	25	160	CpGH89CBM32-5,from Clostridium perfringens, in complex with galactose [Clostridium perfringens],4A44_A CpGH89CBM32-5, from Clostridium perfringens, in complex with the Tn Antigen [Clostridium perfringens],4A45_A CpGH89CBM32-5, from Clostridium perfringens, in complex with GalNAc- beta-1,3-galactose [Clostridium perfringens],4AAX_A CpGH89CBM32-5, from Clostridium perfringens, in complex with N- acetylgalactosamine [Clostridium perfringens]
4H04_A	5.27e-34	432	893	33	477	Lacto-N-biosidasefrom Bifidobacterium bifidum [Bifidobacterium bifidum JCM 1254],4H04_B Lacto-N-biosidase from Bifidobacterium bifidum [Bifidobacterium bifidum JCM 1254],4JAW_A Crystal Structure of Lacto-N-Biosidase from Bifidobacterium bifidum complexed with LNB-thiazoline [Bifidobacterium bifidum JCM 1254],4JAW_B Crystal Structure of Lacto-N-Biosidase from Bifidobacterium bifidum complexed with LNB-thiazoline [Bifidobacterium bifidum JCM 1254],5BXP_A LNBase in complex with LNB-LOGNAc [Bifidobacterium bifidum JCM 1254],5BXP_B LNBase in complex with LNB-LOGNAc [Bifidobacterium bifidum JCM 1254],5BXR_A LNBase in complex with LNB-NHAcDNJ [Bifidobacterium bifidum JCM 1254],5BXR_B LNBase in complex with LNB-NHAcDNJ [Bifidobacterium bifidum JCM 1254],5BXS_A LNBase in complex with LNB-NHAcCAS [Bifidobacterium bifidum JCM 1254],5BXS_B LNBase in complex with LNB-NHAcCAS [Bifidobacterium bifidum JCM 1254],5BXT_A LNBase in complex with LNB-NHAcAUS [Bifidobacterium bifidum JCM 1254],5BXT_B LNBase in complex with LNB-NHAcAUS [Bifidobacterium bifidum JCM 1254]
2V72_A	7.69e-32	1109	1249	9	143	Thestructure of the family 32 CBM from C. perfringens NanJ in complex with galactose [Clostridium perfringens]
3GH4_A	2.23e-28	431	903	37	503	Crystalstructure of beta-hexosaminidase from Paenibacillus sp. TS12 [Paenibacillus sp.],3GH5_A Crystal structure of beta-hexosaminidase from Paenibacillus sp. TS12 in complex with GlcNAc [Paenibacillus sp.],3GH7_A Crystal structure of beta-hexosaminidase from Paenibacillus sp. TS12 in complex with GalNAc [Paenibacillus sp.],3SUR_A Crystal structure of beta-hexosaminidase from Paenibacillus sp. TS12 in complex with NAG-thiazoline. [Paenibacillus sp. TS12],3SUS_A Crystal structure of beta-hexosaminidase from Paenibacillus sp. TS12 in complex with Gal-NAG-thiazoline [Paenibacillus sp. TS12],3SUT_A Crystal structure of beta-hexosaminidase from Paenibacillus sp. TS12 in complex with PUGNAc [Paenibacillus sp. TS12],3SUU_A Crystal structure of beta-hexosaminidase from Paenibacillus sp. TS12 in complex with Gal-PUGNAc [Paenibacillus sp. TS12],3SUV_A Crystal structure of beta-hexosaminidase from Paenibacillus sp. TS12 in complex with NHAc-DNJ [Paenibacillus sp. TS12],3SUW_A Crystal structure of beta-hexosaminidase from Paenibacillus sp. TS12 in complex with NHAc-CAS [Paenibacillus sp. TS12]

Swiss-Prot Hits     

Hit ID	E-Value	Query Start	Query End	Hit Start	Hit End	Description
B2UPR7	2.04e-141	335	1099	14	753	Beta-hexosaminidase Amuc_2136 OS=Akkermansia muciniphila (strain ATCC BAA-835 / DSM 22959 / JCM 33894 / BCRC 81048 / CCUG 64013 / CIP 107961 / Muc) OX=349741 GN=Amuc_2136 PE=1 SV=1
Q8XL08	3.37e-41	1034	1408	560	925	O-GlcNAcase NagJ OS=Clostridium perfringens (strain 13 / Type A) OX=195102 GN=nagJ PE=1 SV=1
Q0TR53	4.44e-41	1034	1408	560	925	O-GlcNAcase NagJ OS=Clostridium perfringens (strain ATCC 13124 / DSM 756 / JCM 1290 / NCIMB 6125 / NCTC 8237 / Type A) OX=195103 GN=nagJ PE=1 SV=1
P0DTR4	1.60e-20	1059	1258	458	653	A type blood N-acetyl-alpha-D-galactosamine deacetylase OS=Flavonifractor plautii OX=292800 PE=1 SV=1
E9DFH0	2.08e-19	518	918	130	577	Beta-hexosaminidase 1 OS=Coccidioides posadasii (strain RMSCC 757 / Silveira) OX=443226 GN=HEX1 PE=1 SV=1

SignalP and Lipop Annotations

This protein is predicted as SP

Other	SP_Sec_SPI	LIPO_Sec_SPII	TAT_Tat_SPI	TATLIP_Sec_SPII	PILIN_Sec_SPIII
0.019973	0.977208	0.002020	0.000261	0.000236	0.000259

TMHMM  Annotations     

start	end
13	35
1720	1742