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Difference between revisions of "Carbohydrate Binding Module Family 14"

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== Ligand specificities ==
 
== Ligand specificities ==
Family 14 CBMs are modules composed of approximately 70 residues. These modules have been reported to be associated with chitinases <cite>Fadel2016</cite> and as chitin-binding lectins e.g. an effector protein from the tomato pathogen ''Pseudoercospora fuligena'' or ''Cladosporium fulvum''<cite>Kohler2016 Hurlburt2018</cite>, as an antimicrobial lectin-like protein from horseshoe crab haemocytes (tachycitin) <cite>Kawabata1996</cite> and in peritrophic matrix proteins from Malaria vector ''Anopheles gambia''. <cite>Shen1998</cite>  
+
Family 14 CBMs are modules composed of approximately 70 residues. These modules have been reported to be associated with chitinases <cite>Fadel2016</cite> and as chitin-binding lectins e.g. an effector protein from the tomato pathogen ''Pseudoercospora fuligena'' or ''Cladosporium fulvum'' <cite>Kohler2016 Hurlburt2018</cite>, as an antimicrobial lectin-like protein from horseshoe crab haemocytes (tachycitin) <cite>Kawabata1996</cite> and in peritrophic matrix proteins from Malaria vector ''Anopheles gambia''. <cite>Shen1998</cite> Members of CBM14 have been shown to bind chitin <cite>Shen1998 Vandevenne2011 Madland2019</cite> and chitooligomers. <cite>Crasson2016 Hurlburt2018</cite> Binding to 50 % acetylated hyaluronan has also been demonstrated. <cite>Crasson2016</cite>  
  
  
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<biblio>
 
<biblio>
 
#Fadel2016 pmid=27111557
 
#Fadel2016 pmid=27111557
#Kohler2016 pmid: 27401545
+
#Kohler2016 pmid=27401545
#Hurlburt2018 pmid: 30148881
+
#Hurlburt2018 pmid=30148881
#Kawabata1996 pmid: 9010778
+
#Kawabata1996 pmid=9010778
#Shen1998 pmid: 9651363
+
#Shen1998 pmid=9651363
#Vandevenne2011 pmid: 21674664
+
#Vandevenne2011 pmid=21674664
#Madland2019 pmid: 31891077
+
#Madland2019 pmid=31891077
#Crasson2016 pmid: 28584264
+
#Crasson2016 pmid=28584264
#Suetake2000 pmid: 10770921
+
#Suetake2000 pmid=10770921
 
#Boraston2004 pmid=15214846
 
#Boraston2004 pmid=15214846
  
 +
#Burg2004 pmid=14769793
 +
#Hollak1994 pmid=8132768
 +
#Kzhyshkowska2007 pmid=19662198
 +
#Gordon-Thomson2009 pmid=19169854
 +
#Joosten1997 pmid=9090881
 +
#Burg2006 pmid=17153926
 
</biblio>
 
</biblio>
  
 
[[Category:Carbohydrate Binding Module Families|CBM014]]
 
[[Category:Carbohydrate Binding Module Families|CBM014]]

Revision as of 06:46, 26 November 2020

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CAZy DB link
https://www.cazy.org/CBMnn.html

Ligand specificities

Family 14 CBMs are modules composed of approximately 70 residues. These modules have been reported to be associated with chitinases [1] and as chitin-binding lectins e.g. an effector protein from the tomato pathogen Pseudoercospora fuligena or Cladosporium fulvum [2, 3], as an antimicrobial lectin-like protein from horseshoe crab haemocytes (tachycitin) [4] and in peritrophic matrix proteins from Malaria vector Anopheles gambia. [5] Members of CBM14 have been shown to bind chitin [5, 6, 7] and chitooligomers. [3, 8] Binding to 50 % acetylated hyaluronan has also been demonstrated. [8]


Structural Features

Content in this section should include, in paragraph form, a description of:

  • Fold: Structural fold (beta trefoil, beta sandwich, etc.)
  • Type: Include here Type A, B, or C and properties
  • Features of ligand binding: Describe CBM binding pocket location (Side or apex) important residues for binding (W, Y, F, subsites), interact with reducing end, non-reducing end, planar surface or within polysaccharide chains. Include examples pdb codes. Metal ion dependent. Etc.

Functionalities

Content in this section should include, in paragraph form, a description of:

  • Functional role of CBM: Describe common functional roles such as targeting, disruptive, anchoring, proximity/position on substrate.
  • Most Common Associated Modules: 1. Glycoside Hydrolase Activity; 2. Additional Associated Modules (other CBM, FNIII, cohesin, dockerins, expansins, etc.)
  • Novel Applications: Include here if CBM has been used to modify another enzyme, or if a CBM was used to label plant/mammalian tissues? Etc.

Family Firsts

First Identified
Insert archetype here, possibly including very brief synopsis.
First Structural Characterization
Insert archetype here, possibly including very brief synopsis.

References

  1. Fadel F, Zhao Y, Cousido-Siah A, Ruiz FX, Mitschler A, and Podjarny A. (2016). X-Ray Crystal Structure of the Full Length Human Chitotriosidase (CHIT1) Reveals Features of Its Chitin Binding Domain. PLoS One. 2016;11(4):e0154190. DOI:10.1371/journal.pone.0154190 | PubMed ID:27111557 [Fadel2016]
  2. Kohler AC, Chen LH, Hurlburt N, Salvucci A, Schwessinger B, Fisher AJ, and Stergiopoulos I. (2016). Structural Analysis of an Avr4 Effector Ortholog Offers Insight into Chitin Binding and Recognition by the Cf-4 Receptor. Plant Cell. 2016;28(8):1945-65. DOI:10.1105/tpc.15.00893 | PubMed ID:27401545 [Kohler2016]
  3. Hurlburt NK, Chen LH, Stergiopoulos I, and Fisher AJ. (2018). Structure of the Cladosporium fulvum Avr4 effector in complex with (GlcNAc)6 reveals the ligand-binding mechanism and uncouples its intrinsic function from recognition by the Cf-4 resistance protein. PLoS Pathog. 2018;14(8):e1007263. DOI:10.1371/journal.ppat.1007263 | PubMed ID:30148881 [Hurlburt2018]
  4. Kawabata S, Nagayama R, Hirata M, Shigenaga T, Agarwala KL, Saito T, Cho J, Nakajima H, Takagi T, and Iwanaga S. (1996). Tachycitin, a small granular component in horseshoe crab hemocytes, is an antimicrobial protein with chitin-binding activity. J Biochem. 1996;120(6):1253-60. DOI:10.1093/oxfordjournals.jbchem.a021549 | PubMed ID:9010778 [Kawabata1996]
  5. Shen Z and Jacobs-Lorena M. (1998). A type I peritrophic matrix protein from the malaria vector Anopheles gambiae binds to chitin. Cloning, expression, and characterization. J Biol Chem. 1998;273(28):17665-70. DOI:10.1074/jbc.273.28.17665 | PubMed ID:9651363 [Shen1998]
  6. Vandevenne M, Campisi V, Freichels A, Gillard C, Gaspard G, Frère JM, Galleni M, and Filée P. (2011). Comparative functional analysis of the human macrophage chitotriosidase. Protein Sci. 2011;20(8):1451-63. DOI:10.1002/pro.676 | PubMed ID:21674664 [Vandevenne2011]
  7. Madland E, Crasson O, Vandevenne M, Sørlie M, and Aachmann FL. (2019). NMR and Fluorescence Spectroscopies Reveal the Preorganized Binding Site in Family 14 Carbohydrate-Binding Module from Human Chitotriosidase. ACS Omega. 2019;4(26):21975-21984. DOI:10.1021/acsomega.9b03043 | PubMed ID:31891077 [Madland2019]
  8. Crasson O, Courtade G, Léonard RR, Aachmann FL, Legrand F, Parente R, Baurain D, Galleni M, Sørlie M, and Vandevenne M. (2017). Human Chitotriosidase: Catalytic Domain or Carbohydrate Binding Module, Who's Leading HCHT's Biological Function. Sci Rep. 2017;7(1):2768. DOI:10.1038/s41598-017-02382-z | PubMed ID:28584264 [Crasson2016]
  9. Suetake T, Tsuda S, Kawabata S, Miura K, Iwanaga S, Hikichi K, Nitta K, and Kawano K. (2000). Chitin-binding proteins in invertebrates and plants comprise a common chitin-binding structural motif. J Biol Chem. 2000;275(24):17929-32. DOI:10.1074/jbc.C000184200 | PubMed ID:10770921 [Suetake2000]
  10. Boraston AB, Bolam DN, Gilbert HJ, and Davies GJ. (2004). Carbohydrate-binding modules: fine-tuning polysaccharide recognition. Biochem J. 2004;382(Pt 3):769-81. DOI:10.1042/BJ20040892 | PubMed ID:15214846 [Boraston2004]
  11. van den Burg HA, Spronk CA, Boeren S, Kennedy MA, Vissers JP, Vuister GW, de Wit PJ, and Vervoort J. (2004). Binding of the AVR4 elicitor of Cladosporium fulvum to chitotriose units is facilitated by positive allosteric protein-protein interactions: the chitin-binding site of AVR4 represents a novel binding site on the folding scaffold shared between the invertebrate and the plant chitin-binding domain. J Biol Chem. 2004;279(16):16786-96. DOI:10.1074/jbc.M312594200 | PubMed ID:14769793 [Burg2004]
  12. Hollak CE, van Weely S, van Oers MH, and Aerts JM. (1994). Marked elevation of plasma chitotriosidase activity. A novel hallmark of Gaucher disease. J Clin Invest. 1994;93(3):1288-92. DOI:10.1172/JCI117084 | PubMed ID:8132768 [Hollak1994]
  13. Kzhyshkowska J, Gratchev A, and Goerdt S. (2007). Human chitinases and chitinase-like proteins as indicators for inflammation and cancer. Biomark Insights. 2007;2:128-46. | Google Books | Open Library PubMed ID:19662198 [Kzhyshkowska2007]
  14. Gordon-Thomson C, Kumari A, Tomkins L, Holford P, Djordjevic JT, Wright LC, Sorrell TC, and Moore GP. (2009). Chitotriosidase and gene therapy for fungal infections. Cell Mol Life Sci. 2009;66(6):1116-25. DOI:10.1007/s00018-009-8765-7 | PubMed ID:19169854 [Gordon-Thomson2009]
  15. Joosten MH, Vogelsang R, Cozijnsen TJ, Verberne MC, and De Wit PJ. (1997). The biotrophic fungus Cladosporium fulvum circumvents Cf-4-mediated resistance by producing unstable AVR4 elicitors. Plant Cell. 1997;9(3):367-79. DOI:10.1105/tpc.9.3.367 | PubMed ID:9090881 [Joosten1997]
  16. van den Burg HA, Harrison SJ, Joosten MH, Vervoort J, and de Wit PJ. (2006). Cladosporium fulvum Avr4 protects fungal cell walls against hydrolysis by plant chitinases accumulating during infection. Mol Plant Microbe Interact. 2006;19(12):1420-30. DOI:10.1094/MPMI-19-1420 | PubMed ID:17153926 [Burg2006]

All Medline abstracts: PubMed