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Glycoside Hydrolase Family 5

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Glycoside Hydrolase Family GH5
Clan GH-A
Mechanism retaining
Active site residues Glu/Glu
CAZy DB link
http://www.cazy.org/fam/GH5.html


Substrate specificities

GH5 is one of the largest of all CAZy hydrolase families with severa thousand distinct sequence entries and with (23-Sept 2009) 36 different proteins having a 3-D structure deposited. A variety of specificties are annotated to this family notably endoglucanase (cellulase) and endomannanase as well as exoglucanases, exomannanases and β-glucodsidase and β-mannosidase. Other activities include 1,6 galactanase, 1,3 mannanase, 1,4 xylanase as well as high specificity xyloglucanases. The Rhodococcal endoglycoceramidase II (EGC) in this family has found application in the chemoenzymatic synthesis of ceramide derivatives.

Family GH5 enzymes are found widely distributed across Archae, bacteria and eukaryotes, notably fungi and plants. There are no known human enzymes in GH5.


Kinetics and Mechanism

Family GH5 enzymes are retaining enzymes, as first shown by NMR [XXX] and follow a classical Koshland double-displacement mechanism.

Catalytic Residues

Content is to be added.


Three-dimensional structures

Three-dimensional structures are available for a very large number of Family GH5 enzymes, the first solved being that of the Clostridium thermocellum endoglucanase CelC [1]. As members of Clan GH-A they have a classical (α/β)8 TIM barrel fold with the two key active site glutamic acids being approximately 200 residues apart in sequence and located at the C-terminal ends of β-strands 4 (acid/base) and 7 (nucleophile) [12]. With so many 3D structures in this family, covering many specificities it is clearly hard to pick out notable structural papers. The Bacillus agaradhaerens Cel5A has been extensively studied, notably in the trapping of enzymatic snapshots along the reaction coordinate [2]but also as a testbed for glycosidase inhibitor design as crystals often diffract to atomic resolution (for example [3]).

Family Firsts

First sterochemistry determination
The curator believes this to be the stereochemical determination for EGZ from Erwinia chrysanthemi [4]. GH5 enzymes were also in the comprehensive Gebler study [5].
First catalytic nucleophile identification
Trapped using the classical Withers 2-fluoromethod, here with 2',4'-dinitrophenyl-2-deoxy-2-fluoro-beta-D-cellobioside, reported in Wang and Withers in 1993 [6].
First general acid/base residue identification
Cite some reference here, with a short (1-2 senetence) explanation [7].
First 3-D structure
The first 3D structures in family GH5 was an endoglucanase (cellulase) from Clostridium thermocellum reported by the Alzari in 1995 (in a paper which also reported a family GH10 xylanase structure and the similarities between them) [8]. Subsequently, Ducros and colleagues reported the Clostridium cellulolyticum Cel5A also in 1995 [9].

References

  1. Davies GJ, Mackenzie L, Varrot A, Dauter M, Brzozowski AM, Schülein M, and Withers SG. (1998). Snapshots along an enzymatic reaction coordinate: analysis of a retaining beta-glycoside hydrolase. Biochemistry. 1998;37(34):11707-13. DOI:10.1021/bi981315i | PubMed ID:9718293 [Davies1998]
  2. Varrot A, Tarling CA, Macdonald JM, Stick RV, Zechel DL, Withers SG, and Davies GJ. (2003). Direct observation of the protonation state of an imino sugar glycosidase inhibitor upon binding. J Am Chem Soc. 2003;125(25):7496-7. DOI:10.1021/ja034917k | PubMed ID:12812472 [Varrot2003]
  3. Barras F, Bortoli-German I, Bauzan M, Rouvier J, Gey C, Heyraud A, and Henrissat B. (1992). Stereochemistry of the hydrolysis reaction catalyzed by endoglucanase Z from Erwinia chrysanthemi. FEBS Lett. 1992;300(2):145-8. DOI:10.1016/0014-5793(92)80183-h | PubMed ID:1563515 [Barras1992]
  4. Gebler J, Gilkes NR, Claeyssens M, Wilson DB, Béguin P, Wakarchuk WW, Kilburn DG, Miller RC Jr, Warren RA, and Withers SG. (1992). Stereoselective hydrolysis catalyzed by related beta-1,4-glucanases and beta-1,4-xylanases. J Biol Chem. 1992;267(18):12559-61. | Google Books | Open Library PubMed ID:1618761 [Gebler1992]
  5. Wang Q, Tull D, Meinke A, Gilkes NR, Warren RA, Aebersold R, and Withers SG. (1993). Glu280 is the nucleophile in the active site of Clostridium thermocellum CelC, a family A endo-beta-1,4-glucanase. J Biol Chem. 1993;268(19):14096-102. | Google Books | Open Library PubMed ID:8100226 [Wang1993]
  6. Dominguez R, Souchon H, Spinelli S, Dauter Z, Wilson KS, Chauvaux S, Béguin P, and Alzari PM. (1995). A common protein fold and similar active site in two distinct families of beta-glycanases. Nat Struct Biol. 1995;2(7):569-76. DOI:10.1038/nsb0795-569 | PubMed ID:7664125 [Dominguez1995]
  7. Ducros V, Czjzek M, Belaich A, Gaudin C, Fierobe HP, Belaich JP, Davies GJ, and Haser R. (1995). Crystal structure of the catalytic domain of a bacterial cellulase belonging to family 5. Structure. 1995;3(9):939-49. DOI:10.1016/S0969-2126(01)00228-3 | PubMed ID:8535787 [Ducros1995]
  8. Comfort DA, Bobrov KS, Ivanen DR, Shabalin KA, Harris JM, Kulminskaya AA, Brumer H, and Kelly RM. (2007). Biochemical analysis of Thermotoga maritima GH36 alpha-galactosidase (TmGalA) confirms the mechanistic commonality of clan GH-D glycoside hydrolases. Biochemistry. 2007;46(11):3319-30. DOI:10.1021/bi061521n | PubMed ID:17323919 [1]
  9. Sinnott, M.L. (1990) Catalytic mechanisms of enzymic glycosyl transfer. Chem. Rev. 90, 1171-1202. DOI: 10.1021/cr00105a006

    [4]

All Medline abstracts: PubMed

[[Category:Glycoside Hydrolase Families|GHnnn]]