Carbohydrate Esterase Family 1

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• Author: ^^^Casper Wilkens^^^
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Substrate specificities

Carbohydrate esterase family 1 (CE1) is one of the biggest and most diverse CE families including acetylxylan esterases (EC 3.1.1.72), feruloyl esterases (EC 3.1.1.73), cinnamoyl esterases (EC 3.1.1.-), carboxylesterases (EC 3.1.1.1), S-formylglutathione hydrolases (EC 3.1.2.12), diacylglycerol O-acyltransferases (EC 2.3.1.20), and thehalose 6-O-mycolyltransferases (EC 2.3.1.122) and others [1].

Kinetics and Mechanism

CE1 enzymes target a large variety of substrates, however, the general mechanism of hydrolysis, involving the serine nucleophile, an activating histidine, and a catalytic acid, appears to be conserved. After substrate binding, the serine is activated by the histidine, which allows the nucleophilic attack of the substrate’s carbonyl carbon atom leading to the formation of a covalent acyl-enzyme intermediate via tetrahedral transition states sometimes known as the “tetrahedral intermediates.” Simultaneously, a proton is transferred from the serine to the histidine. The resulting tetrahydral intermediate, negatively charged carbonyl oxygen atom (“oxyanion”) is stabilized through interactions with two main chain NH groups in the “oxyanion hole”, while the positively charged histidine is stabilized by a hydrogen bond to the catalytic acid. In the next step, the formed alcohol is released from the substrate and the acid part forms an ester bond with the serine oxygen. This bond, in turn, is hydrolyzed in a two- step mechanism involving a water molecule, and the enzyme is returned to the starting point [2, 3].

Catalytic Residues

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Three-dimensional structures

CE1's are members of the α/β-hydrolase superfamily [4], which are comprised of a central β-sheet with 8 or 9 strands connected by α-helices [5]. The crystal structure of 9 CE1s have been determined - 4 mycosyltransferases, 4 ferulic acid esterases and 1 acetyl xylan esterase [1].

Family Firsts

First characterized

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First mechanistic insight

The crystal structure of Mycobacterium tuberculosis H37Rv mycolyltransferase in complex with the covalently bound inhibitor, diethyl phosphate gave the first insight into the mechanism, which involved the highly conserved catalytic Ser-Glu-His triad [4].

First 3-D structure

Mycobacterium tuberculosis H37Rv mycolyltransferase crystal structure in 2000 [4].

References

1. Lombard V, Golaconda Ramulu H, Drula E, Coutinho PM, and Henrissat B. (2014). The carbohydrate-active enzymes database (CAZy) in 2013. Nucleic Acids Res. 2014;42(Database issue):D490-5. DOI:10.1093/nar/gkt1178 | PubMed ID:24270786 [Lombard2014]
2. Schubot FD, Kataeva IA, Blum DL, Shah AK, Ljungdahl LG, Rose JP, and Wang BC. (2001). Structural basis for the substrate specificity of the feruloyl esterase domain of the cellulosomal xylanase Z from Clostridium thermocellum. Biochemistry. 2001;40(42):12524-32. DOI:10.1021/bi011391c | PubMed ID:11601976 [Schubot2001]
3. Prates JA, Tarbouriech N, Charnock SJ, Fontes CM, Ferreira LM, and Davies GJ. (2001). The structure of the feruloyl esterase module of xylanase 10B from Clostridium thermocellum provides insights into substrate recognition. Structure. 2001;9(12):1183-90. DOI:10.1016/s0969-2126(01)00684-0 | PubMed ID:11738044 [Prates2001]
4. Ronning DR, Klabunde T, Besra GS, Vissa VD, Belisle JT, and Sacchettini JC. (2000). Crystal structure of the secreted form of antigen 85C reveals potential targets for mycobacterial drugs and vaccines. Nat Struct Biol. 2000;7(2):141-6. DOI:10.1038/72413 | PubMed ID:10655617 [Ronning2000]
5. Ollis DL, Cheah E, Cygler M, Dijkstra B, Frolow F, Franken SM, Harel M, Remington SJ, Silman I, and Schrag J. (1992). The alpha/beta hydrolase fold. Protein Eng. 1992;5(3):197-211. DOI:10.1093/protein/5.3.197 | PubMed ID:1409539 [Ollis1992]
6. Belisle JT, Vissa VD, Sievert T, Takayama K, Brennan PJ, and Besra GS. (1997). Role of the major antigen of Mycobacterium tuberculosis in cell wall biogenesis. Science. 1997;276(5317):1420-2. DOI:10.1126/science.276.5317.1420 | PubMed ID:9162010 [Belisle1997]

All Medline abstracts: PubMed