Difference between revisions of "Carbohydrate Binding Module Family 42"

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• Author: ^^^Shinya Fushinobu^^^
• Responsible Curator: ^^^Shinya Fushinobu^^^

Ligand specificities

This module was originally identified as a non-catalytic xylan-binding domain in GH54 α-L-arabinofuranosidase from Trichoderma reesei PC-3-7 [1]. In 2004, it was found to be a CBM specific for an L-arabinofuranosyl group because L-arabinofuranose molecules were bound to a non-catalytic domain of GH54 α-L-arabinofuranosidase B from Aspergillus kawachii (AkAbfB) [2]. CBM42 members have multivalent (usually divalent or trivalent) binding ability to non-reducing end L-arabinofuranosyl residues, which are present in plant polysaccharides (hemicelluloses) such as arabinoxylan, arabinan, and arabinogalactan. Most of CBM42s are associated with α-L-arabinofuranosidases in fungi (GH54) or bacteria (GH43).

Structural Features

• Fold: CBM42s have a β-trefoil fold that is similar to CBM13 and R(ricin)-type lectins. The module has a sequential 3-fold internal repeat of approximately 45 amino acid residues comprising three subdomains. The three subdomains are denoted as α, β, and γ. Each subdomain contains a discrete ligand binding site, but one of the three subdomains sometimes loses its function due to mutations at critical residues for ligand binding.
• Type: CBM42s are typical Type C CBMs that bind termini of glycans with pocket-type binding sites for short oligosaccharides. The binding pockets are small but can accommodate the branched side chain L-arabinofuranosyl moiety attached to the xylan backbone of arabinoxylans [2].
• Features of ligand binding: The binding sites are located at side pockets of the triangular structure of the β-trefoil fold. Residues important for the binding to a non-reducing end L-arabinofuranosyl group are as follows: an aspartate forming hydrogen bonds to the O2 and O3 hydroxyls, a histidine forming a hydrogen bond to the O5 hydroxyl, and a tyrosine stacking to the furanose ring. They are D425, H416, and Y456 in the β-subdomain of AkAbfB and are conserved in functional CBM42 subdomains.
• Available structures: Several crystal structures including complex structures with compounds containing an L-arabinofuranosyl group are available. For example, AkAbfB (α-subdomain is non-functional) 1WD3 1WD4 [3], 2D43 2D44 [2]; Exo-1,5-α-L-arabinofuranosidase from Sreptomyces avermitilis (all subdomains are functional)3AKF 3AKG 3AKH 3AKI [4]; CBM42A in Cthe_0015 from Clostridium thermocellum (β-subdomain is non-functional) 3KMV [5].

Functionalities

• Functional role of CBM: CBM42s are thought to target catalytic modules (usually α-L-arabinofuranosidases) helicelluloses that have L-arabinofuranosyl termini or branches. Mutations at the binding sites of CBM42 significantly reduced the catalytic activity toward natural polysaccharides in these enzymes whereas the activity toward p-nitrophenyl α-L-arabinofuranoside was not affected [6].
• Most Common Associated Modules: α-L-Arabinofuranosidases or exo-arabinanases of GH2, GH43, GH54, GH93, or non-classified GHs [5]. A survey using the GH-CBM tool shows that CBM42s are also associated with GH16 or GH30.

• Novel Applications: A CBM42 was used to create a chimeric enzyme with a feruloyl esterase [7].

Family Firsts

First Identified

The L-arabinofuranose-binding function of CBM42 was first suggested by crystallography of α-L-arabinofuranosidase B from Aspergillus kawachii (AkAbfB) [3].

First Structural Characterization

The first structure of CBM42 was revealed in 2004 in the x-ray crystal structure of AkAbfB in complex with arabinose [3].

References

1. Nogawa M, Yatsui K, Tomioka A, Okada H, and Morikawa Y. (1999). An alpha-L-arabinofuranosidase from Trichoderma reesei containing a noncatalytic xylan-binding domain. Appl Environ Microbiol. 1999;65(9):3964-8. DOI:10.1128/AEM.65.9.3964-3968.1999 | PubMed ID:10473402 [Nogawa1999]
2. Miyanaga A, Koseki T, Miwa Y, Mese Y, Nakamura S, Kuno A, Hirabayashi J, Matsuzawa H, Wakagi T, Shoun H, and Fushinobu S. (2006). The family 42 carbohydrate-binding module of family 54 alpha-L-arabinofuranosidase specifically binds the arabinofuranose side chain of hemicellulose. Biochem J. 2006;399(3):503-11. DOI:10.1042/BJ20060567 | PubMed ID:16846393 [Miyanaga2006]
3. Miyanaga A, Koseki T, Matsuzawa H, Wakagi T, Shoun H, and Fushinobu S. (2004). Crystal structure of a family 54 alpha-L-arabinofuranosidase reveals a novel carbohydrate-binding module that can bind arabinose. J Biol Chem. 2004;279(43):44907-14. DOI:10.1074/jbc.M405390200 | PubMed ID:15292273 [Miyanaga2004]
5. Ribeiro T, Santos-Silva T, Alves VD, Dias FM, Luís AS, Prates JA, Ferreira LM, Romão MJ, and Fontes CM. (2010). Family 42 carbohydrate-binding modules display multiple arabinoxylan-binding interfaces presenting different ligand affinities. Biochim Biophys Acta. 2010;1804(10):2054-62. DOI:10.1016/j.bbapap.2010.07.006 | PubMed ID:20637315 [Ribeiro2010]
7. Koseki T, Mochizuki K, Kisara H, Miyanaga A, Fushinobu S, Murayama T, and Shiono Y. (2010). Characterization of a chimeric enzyme comprising feruloyl esterase and family 42 carbohydrate-binding module. Appl Microbiol Biotechnol. 2010;86(1):155-61. DOI:10.1007/s00253-009-2224-0 | PubMed ID:19756576 [Koseki2010]
8. Fujimoto Z, Ichinose H, Maehara T, Honda M, Kitaoka M, and Kaneko S. (2010). Crystal structure of an Exo-1,5-{alpha}-L-arabinofuranosidase from Streptomyces avermitilis provides insights into the mechanism of substrate discrimination between exo- and endo-type enzymes in glycoside hydrolase family 43. J Biol Chem. 2010;285(44):34134-43. DOI:10.1074/jbc.M110.164251 | PubMed ID:20739278 [Fujimot2010]

All Medline abstracts: PubMed