dbCAN-PUL

PUL ID	PUL0416
PubMed	22205877, PLoS Biol. 2011 Dec;9(12):e1001221. doi: 10.1371/journal.pbio.1001221. Epub 2011 Dec 20.
Characterization method	microarray
Genomic accession number	AAXF02000045.1
Nucelotide position range	159078-179453
Substrate	plant polysaccharide
Loci	BACOVA_01792-BACOVA_01803
Species	Bacteroides ovatus/28116
Degradation or Biosynthesis	degradation

Gene Name	Locus Tag	Protein ID	Gene Position	GenBank Contig Range	EC Number
-	BACOVA_01792	EDO12649.1	0 - 1875 (+)	AAXF02000045.1:159078-160953	-
-	BACOVA_01793	EDO12650.1	1919 - 3017 (+)	AAXF02000045.1:160997-162095	-
-	BACOVA_01794	EDO12651.1	3022 - 4426 (+)	AAXF02000045.1:162100-163504	-
-	BACOVA_01795	EDO12652.1	4466 - 5630 (+)	AAXF02000045.1:163544-164708	-
-	BACOVA_01796	EDO12653.1	5682 - 8907 (+)	AAXF02000045.1:164760-167985	-
-	BACOVA_01797	EDO12654.1	8925 - 10587 (+)	AAXF02000045.1:168003-169665	-
-	BACOVA_01798	EDO12655.1	10605 - 12303 (+)	AAXF02000045.1:169683-171381	-
-	BACOVA_01799	EDO12656.1	12393 - 13392 (+)	AAXF02000045.1:171471-172470	-
-	BACOVA_01800	EDO12657.1	13445 - 14849 (+)	AAXF02000045.1:172523-173927	-
-	BACOVA_01801	EDO12658.1	14871 - 16305 (+)	AAXF02000045.1:173949-175383	-
-	BACOVA_01802	EDO12659.1	16273 - 18967 (+)	AAXF02000045.1:175351-178045	-
-	BACOVA_01803	EDO12660.1	18963 - 20376 (+)	AAXF02000045.1:178041-179454	-

Cluster number	1
Gene name	Gene position	Gene type	Found by CGCFinder?
-	1 - 1875 (+)	CDS	No
-	1920 - 3017 (+)	CDS	No
-	3023 - 4426 (+)	TC: gnl\|TC-DB\|P96710\|2.A.1.1.55	Yes
-	4467 - 5630 (+)	other	Yes
-	5683 - 8907 (+)	TC: gnl\|TC-DB\|Q93TH9\|1.B.14.6.2	Yes
-	8926 - 10587 (+)	other	Yes
-	10606 - 12303 (+)	other	Yes
-	12394 - 13392 (+)	other	Yes
-	13446 - 14849 (+)	other	Yes
-	14872 - 16305 (+)	other	Yes
-	16274 - 18967 (+)	CAZyme: CE6\|GH105\|GH151	Yes
-	18964 - 20376 (+)	CDS	No

PUL ID	PUL0416
PubMed	22205877, PLoS Biol. 2011 Dec;9(12):e1001221. doi: 10.1371/journal.pbio.1001221. Epub 2011 Dec 20.
Title	Recognition and degradation of plant cell wall polysaccharides by two human gut symbionts.
Author	Martens EC, Lowe EC, Chiang H, Pudlo NA, Wu M, McNulty NP, Abbott DW, Henrissat B, Gilbert HJ, Bolam DN, Gordon JI
Abstract	Symbiotic bacteria inhabiting the human gut have evolved under intense pressure to utilize complex carbohydrates, primarily plant cell wall glycans in our diets. These polysaccharides are not digested by human enzymes, but are processed to absorbable short chain fatty acids by gut bacteria. The Bacteroidetes, one of two dominant bacterial phyla in the adult gut, possess broad glycan-degrading abilities. These species use a series of membrane protein complexes, termed Sus-like systems, for catabolism of many complex carbohydrates. However, the role of these systems in degrading the chemically diverse repertoire of plant cell wall glycans remains unknown. Here we show that two closely related human gut Bacteroides, B. thetaiotaomicron and B. ovatus, are capable of utilizing nearly all of the major plant and host glycans, including rhamnogalacturonan II, a highly complex polymer thought to be recalcitrant to microbial degradation. Transcriptional profiling and gene inactivation experiments revealed the identity and specificity of the polysaccharide utilization loci (PULs) that encode individual Sus-like systems that target various plant polysaccharides. Comparative genomic analysis indicated that B. ovatus possesses several unique PULs that enable degradation of hemicellulosic polysaccharides, a phenotype absent from B. thetaiotaomicron. In contrast, the B. thetaiotaomicron genome has been shaped by increased numbers of PULs involved in metabolism of host mucin O-glycans, a phenotype that is undetectable in B. ovatus. Binding studies of the purified sensor domains of PUL-associated hybrid two-component systems in conjunction with transcriptional analyses demonstrate that complex oligosaccharides provide the regulatory cues that induce PUL activation and that each PUL is highly specific for a defined cell wall polymer. These results provide a view of how these species have diverged into different carbohydrate niches by evolving genes that target unique suites of available polysaccharides, a theme that likely applies to disparate bacteria from the gut and other habitats.

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