dbCAN-PUL

PUL ID	PUL0093
PubMed	31275257, Front Microbiol. 2019 Jun 7;10:1286. doi: 10.3389/fmicb.2019.01286. eCollection 2019.
Characterization method	fosmid library screen,lectin binding assay
Genomic accession number	LR131278.1
Nucelotide position range	76-36757
Substrate	O-glycan,N-glycan
Loci	VDS02490.1-VDS02513.1
Species	uncultured bacterium/77133
Degradation or Biosynthesis	degradation

Gene Name	Locus Tag	Protein ID	Gene Position	GenBank Contig Range	EC Number
-	-	VDS02490.1	76 - 1312 (+)	LR131278.1:152-1388	-
-	-	VDS02491.1	1357 - 2149 (+)	LR131278.1:1433-2225	3.5.99.6
-	-	VDS02492.1	2152 - 4141 (+)	LR131278.1:2228-4217	3.5.99.6
-	-	VDS02493.1	4316 - 5051 (-)	LR131278.1:4392-5127	-
-	-	VDS02494.1	5146 - 6025 (-)	LR131278.1:5222-6101	-
-	-	VDS02495.1	6201 - 7269 (+)	LR131278.1:6277-7345	-
-	-	VDS02496.1	7268 - 10394 (+)	LR131278.1:7344-10470	-
-	-	VDS02497.1	10438 - 11806 (+)	LR131278.1:10514-11882	-
-	-	VDS02498.1	12020 - 12647 (-)	LR131278.1:12096-12723	-
-	-	VDS02499.1	12967 - 13801 (+)	LR131278.1:13043-13877	-
-	-	VDS02500.1	13938 - 14868 (+)	LR131278.1:14014-14944	-
-	-	VDS02501.1	14864 - 15542 (+)	LR131278.1:14940-15618	-
-	-	VDS02502.1	15598 - 18259 (-)	LR131278.1:15674-18335	-
-	-	VDS02503.1	18263 - 19130 (-)	LR131278.1:18339-19206	-
-	-	VDS02504.1	19414 - 20734 (+)	LR131278.1:19490-20810	2.7.13.3
-	-	VDS02505.1	20756 - 21458 (+)	LR131278.1:20832-21534	-
-	-	VDS02506.1	21526 - 22741 (-)	LR131278.1:21602-22817	3.5.1.25
-	-	VDS02507.1	22864 - 25369 (-)	LR131278.1:22940-25445	3.2.1.23
-	-	VDS02508.1	25371 - 27624 (-)	LR131278.1:25447-27700	-
-	-	VDS02509.1	27650 - 29705 (-)	LR131278.1:27726-29781	3.2.1.52
-	-	VDS02510.1	29701 - 30916 (-)	LR131278.1:29777-30992	-
-	-	VDS02511.1	31015 - 33328 (-)	LR131278.1:31091-33404	3.2.1.52
-	-	VDS02512.1	33356 - 35924 (-)	LR131278.1:33432-36000	3.2.1.25
-	-	VDS02513.1	35950 - 36757 (-)	LR131278.1:36026-36833	-

Cluster number	1
Gene name	Gene position	Gene type	Found by CGCFinder?
-	77 - 1312 (+)	TC: gnl\|TC-DB\|Q8FDB7\|2.A.1.14.14	Yes
-	1358 - 2149 (+)	other	Yes
-	2153 - 4141 (+)	STP: STP\|PIG-L	Yes
-	4317 - 5051 (-)	other	Yes
-	5147 - 6025 (-)	TF: DBD-Pfam\|HTH_AraC,DBD-SUPERFAMILY\|0035607	Yes
-	6202 - 7269 (+)	other	Yes
-	7269 - 10394 (+)	TC: gnl\|TC-DB\|A6P7H1\|2.A.6.2.37	Yes
-	10439 - 11806 (+)	other	Yes
-	12021 - 12647 (-)	other	Yes
-	12968 - 13801 (+)	other	Yes
-	13939 - 14868 (+)	other	Yes
-	14865 - 15542 (+)	TC: gnl\|TC-DB\|Q18BL2\|3.A.1.124.6	Yes
-	15599 - 18259 (-)	TC: gnl\|TC-DB\|E6X5M3\|1.C.105.2.12	Yes
-	18264 - 19130 (-)	other	Yes
-	19415 - 20734 (+)	STP: STP\|HATPase_c	Yes
-	20757 - 21458 (+)	TF: DBD-Pfam\|Trans_reg_C	Yes
-	21527 - 22741 (-)	CAZyme: CE9	Yes
-	22865 - 25369 (-)	CAZyme: GH2	Yes
-	25372 - 27624 (-)	CAZyme: GH92	Yes
-	27651 - 29705 (-)	CAZyme: GH20	Yes
-	29702 - 30916 (-)	other	Yes
-	31016 - 33328 (-)	CAZyme: GH20	Yes
-	33357 - 35924 (-)	CAZyme: GH2	Yes
-	35951 - 36757 (-)	CDS	No

PUL ID	PUL0093
PubMed	31275257, Front Microbiol. 2019 Jun 7;10:1286. doi: 10.3389/fmicb.2019.01286. eCollection 2019.
Title	Investigating Host Microbiota Relationships Through Functional Metagenomics.
Author	Laville E, Perrier J, Bejar N, Maresca M, Esque J, Tauzin AS, Bouhajja E, Leclerc M, Drula E, Henrissat B, Berdah S, Di Pasquale E, Robe P, Potocki-Veronese G
Abstract	The human Intestinal mucus is formed by glycoproteins, the O- and N-linked glycans which constitute a crucial source of carbon for commensal gut bacteria, especially when deprived of dietary glycans of plant origin. In recent years, a dozen carbohydrate-active enzymes from cultivated mucin degraders have been characterized. But yet, considering the fact that uncultured species predominate in the human gut microbiota, these biochemical data are far from exhaustive. In this study, we used functional metagenomics to identify new metabolic pathways in uncultured bacteria involved in harvesting mucin glycans. First, we performed a high-throughput screening of a fosmid metagenomic library constructed from the ileum mucosa microbiota using chromogenic substrates. The screening resulted in the isolation of 124 clones producing activities crucial in the degradation of human O- and N-glycans, namely sialidases, beta-D-N-acetyl-glucosaminidase, beta-D-N-acetyl-galactosaminidase, and/or beta-D-mannosidase. Thirteen of these clones were selected based on their diversified functional profiles and were further analyzed on a secondary screening. This step consisted of lectin binding assays to demonstrate the ability of the clones to degrade human intestinal mucus. In total, the structural modification of several mucin motifs, sialylated mucin ones in particular, was evidenced for nine clones. Sequencing their metagenomic loci highlighted complex catabolic pathways involving the complementary functions of glycan sensing, transport, hydrolysis, deacetylation, and deamination, which were sometimes associated with amino acid metabolism machinery. These loci are assigned to several Bacteroides and Feacalibacterium species highly prevalent and abundant in the gut microbiome and explain the metabolic flexibility of gut bacteria feeding both on dietary and human glycans.

PUL General Information

Literature Information

Genomic Location Information

CGCFinder Result

Homologus Loci

Nucelotide position range

Substrate

Loci

Species

Degradation or Biosynthesis

Gene Name

Locus Tag

Protein ID

Gene Position

GenBank Contig Range

EC Number

Cluster number

Gene name

Gene position

Gene type

Found by CGCFinder?