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Difference between revisions of "Glycoside Hydrolase Family 173"
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* [[Author]]s: [[User:Clelton Santos|Clelton Aparecido dos Santos]] and [[User:Gabriela Persinoti|Gabriela Felix Persinoti]] | * [[Author]]s: [[User:Clelton Santos|Clelton Aparecido dos Santos]] and [[User:Gabriela Persinoti|Gabriela Felix Persinoti]] | ||
* [[Responsible Curator]]: [[User:Mario Murakami|Mario Murakami]] | * [[Responsible Curator]]: [[User:Mario Murakami|Mario Murakami]] | ||
| Line 15: | Line 15: | ||
|- | |- | ||
|'''Mechanism''' | |'''Mechanism''' | ||
| − | | | + | |retaining (inferred) |
|- | |- | ||
|'''Active site residues''' | |'''Active site residues''' | ||
| Line 29: | Line 29: | ||
== Substrate specificities == | == Substrate specificities == | ||
| − | The GH173 family comprises members with β-galactosidase activity <cite>Cabral2022</cite>. The founding member of the GH173 family named herein as CapGH173 (PBMDCECB_44807), was identified in a | + | The GH173 family comprises so far members with β-galactosidase activity <cite>Cabral2022</cite>. The founding member of the GH173 family named herein as CapGH173 ([https://www.ncbi.nlm.nih.gov/nuccore/2205462651 PBMDCECB_44807]), was identified in a metagenome-assembled genome (''Bacteroidales bacterium'' MAG42) recovered from capybara gut microbiota, which potentially represents a novel genus from the UBA932 family. The enzyme CapGH173 was found in a Polysaccharide Utilization Loci (PUL) that includes enzymes from the families [[GH2]] and [[GH78]], yet the target carbohydrate remains unclear. GH173 members often exhibit a modular architecture including a [[GH36]] domain. Substrate kinetics characterization of CapGH173 was demonstrated on synthetic substrate ''p''-nitrophenyl-β-D-galactopyranoside (pNP-β-D-Gal). Phylogenetic analysis showed that this family belongs to the GH-A clan, being remotely related to the families [[GH30]] and [[GH5]] <cite>Cabral2022</cite>. |
== Kinetics and Mechanism == | == Kinetics and Mechanism == | ||
| − | + | GH173 members are inferred to be retaining enzymes <cite>Cabral2022</cite>. | |
== Catalytic Residues == | == Catalytic Residues == | ||
| − | The residues E305 and E207 correspond to the nucleophile and acid/base, respectively | + | The residues E305 and E207 (sequence numbering based on the founding member, CapGH173) was inferred to correspond to the nucleophile and acid/base, respectively, based on the structural analysis of AlphaFold models <cite>Cabral2022</cite>. |
== Three-dimensional structures == | == Three-dimensional structures == | ||
| − | Protein modeling and threading performed using AlphaFold and PDBsum, respectively, | + | Protein modeling and threading performed using AlphaFold and PDBsum, respectively, suggest that CapGH173 consists of an (α/β)<sub>8</sub>-barrel structure, which is an archetypal scaffold of the clan GH-A. According to structural predictions, CapGH173 exhibits a two-domain architecture including an appended β-sandwich domain, which is a similar structural organization found in the [[GH30]] family. Except for the residues defining the clan GH-A, sequence alignment with [[GH5]] and [[GH30]] members revealed very low sequence conservation, below the criterium for significant similarity detection (using an e-value < 0.05), demonstrating that although the domains in the tertiary structure can be similar, the sequences between these families are remarkably diverse <cite>Cabral2022</cite>. |
== Family Firsts == | == Family Firsts == | ||
| − | ;First stereochemistry determination: | + | ;First stereochemistry determination: CapGH173 is inferred to operate by a retaining mechanism. |
;First catalytic nucleophile identification: E305 (inferred). | ;First catalytic nucleophile identification: E305 (inferred). | ||
;First general acid/base residue identification: E207 (inferred). | ;First general acid/base residue identification: E207 (inferred). | ||
Latest revision as of 15:01, 5 July 2023
This page has been approved by the Responsible Curator as essentially complete. CAZypedia is a living document, so further improvement of this page is still possible. If you would like to suggest an addition or correction, please contact the page's Responsible Curator directly by e-mail.
- Authors: Clelton Aparecido dos Santos and Gabriela Felix Persinoti
- Responsible Curator: Mario Murakami
| Glycoside Hydrolase Family GH173 | |
| Clan | GH-A |
| Mechanism | retaining (inferred) |
| Active site residues | known (inferred) |
| CAZy DB link | |
| http://www.cazy.org/GH173.html | |
Substrate specificities
The GH173 family comprises so far members with β-galactosidase activity [1]. The founding member of the GH173 family named herein as CapGH173 (PBMDCECB_44807), was identified in a metagenome-assembled genome (Bacteroidales bacterium MAG42) recovered from capybara gut microbiota, which potentially represents a novel genus from the UBA932 family. The enzyme CapGH173 was found in a Polysaccharide Utilization Loci (PUL) that includes enzymes from the families GH2 and GH78, yet the target carbohydrate remains unclear. GH173 members often exhibit a modular architecture including a GH36 domain. Substrate kinetics characterization of CapGH173 was demonstrated on synthetic substrate p-nitrophenyl-β-D-galactopyranoside (pNP-β-D-Gal). Phylogenetic analysis showed that this family belongs to the GH-A clan, being remotely related to the families GH30 and GH5 [1].
Kinetics and Mechanism
GH173 members are inferred to be retaining enzymes [1].
Catalytic Residues
The residues E305 and E207 (sequence numbering based on the founding member, CapGH173) was inferred to correspond to the nucleophile and acid/base, respectively, based on the structural analysis of AlphaFold models [1].
Three-dimensional structures
Protein modeling and threading performed using AlphaFold and PDBsum, respectively, suggest that CapGH173 consists of an (α/β)8-barrel structure, which is an archetypal scaffold of the clan GH-A. According to structural predictions, CapGH173 exhibits a two-domain architecture including an appended β-sandwich domain, which is a similar structural organization found in the GH30 family. Except for the residues defining the clan GH-A, sequence alignment with GH5 and GH30 members revealed very low sequence conservation, below the criterium for significant similarity detection (using an e-value < 0.05), demonstrating that although the domains in the tertiary structure can be similar, the sequences between these families are remarkably diverse [1].
Family Firsts
- First stereochemistry determination
- CapGH173 is inferred to operate by a retaining mechanism.
- First catalytic nucleophile identification
- E305 (inferred).
- First general acid/base residue identification
- E207 (inferred).
- First 3-D structure
- Currently no experimental structure is available for GH173 members.
References
- Cabral L, Persinoti GF, Paixão DAA, Martins MP, Morais MAB, Chinaglia M, Domingues MN, Sforca ML, Pirolla RAS, Generoso WC, Santos CA, Maciel LF, Terrapon N, Lombard V, Henrissat B, and Murakami MT. (2022). Gut microbiome of the largest living rodent harbors unprecedented enzymatic systems to degrade plant polysaccharides. Nat Commun. 2022;13(1):629. DOI:10.1038/s41467-022-28310-y |