Literature DB >> 15618227

A clostridial endo-beta-galactosidase that cleaves both blood group A and B glycotopes: the first member of a new glycoside hydrolase family, GH98.

Kimberly M Anderson1, Hisashi Ashida, Karol Maskos, Anne Dell, Su-Chen Li, Yu-Teh Li.   

Abstract

We have isolated an endo-beta-galactosidase designated E-ABase from Clostridium perfringens ATCC 10543 capable of liberating both the A trisaccharide (A-Tri; GalNAcalpha1-->3(Fucalpha1-->2)Gal) and B trisaccharide (B-Tri; Galalpha1-->3(Fucalpha1-->2)Gal) from glycoconjugates containing blood group A and B glycotopes, respectively. We have subsequently cloned the gene (eabC) that encodes E-ABase from this organism. This gene was found to be identical to the CPE0329 gene of C. perfringens strain 13, whose product was labeled as a hypothetical protein (Shimizu, T., Ohtani, K., Hirakawa, H., Ohshima, K., Yamashita, A., Shiba, T., Ogasawara, N., Hattori, M., Kuhara, S., and Hayashi, H. (2002) Proc. Natl. Acad. Sci. U. S. A. 99, 996-1001). Since the amino acid sequence of E-ABase does not bear detectable similarity to any of the 97 existing families of glycoside hydrolases, we have proposed to assign this unusual enzyme to a new family, GH98. We also expressed eabC in Escherichia coli BL21(DE3) and obtained 27 mg of fully active recombinant E-ABase from 1 liter of culture. Recombinant E-ABase not only destroyed the blood group A and B antigenicity of human type A and B erythrocytes, but also released A-Tri and B-Tri from blood group A(+)- and B(+)- containing glycoconjugates. The structures of A-Tri and B-Tri liberated from A(+) porcine gastric mucin and B(+) human ovarian cyst glycoprotein were established by NMR spectroscopy. The unique specificity of E-ABase should make it useful for studying the structure and function of blood group A- and B-containing glycoconju-gates as well as for identifying other glycosidases belonging to the new GH98 family.

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Year:  2004        PMID: 15618227     DOI: 10.1074/jbc.M414099200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  16 in total

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2.  Glycoside hydrolase family 89 alpha-N-acetylglucosaminidase from Clostridium perfringens specifically acts on GlcNAc alpha1,4Gal beta1R at the non-reducing terminus of O-glycans in gastric mucin.

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3.  Differential recognition and hydrolysis of host carbohydrate antigens by Streptococcus pneumoniae family 98 glycoside hydrolases.

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4.  Divergent modes of glycan recognition by a new family of carbohydrate-binding modules.

Authors:  Katie J Gregg; Ron Finn; D Wade Abbott; Alisdair B Boraston
Journal:  J Biol Chem       Date:  2008-02-21       Impact factor: 5.157

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Review 6.  Toward universal donor blood: Enzymatic conversion of A and B to O type.

Authors:  Peter Rahfeld; Stephen G Withers
Journal:  J Biol Chem       Date:  2019-12-02       Impact factor: 5.157

Review 7.  Mucin glycan foraging in the human gut microbiome.

Authors:  Louise E Tailford; Emmanuelle H Crost; Devon Kavanaugh; Nathalie Juge
Journal:  Front Genet       Date:  2015-03-19       Impact factor: 4.599

Review 8.  Exo- and endoglycosidases revisited.

Authors:  Akira Kobata
Journal:  Proc Jpn Acad Ser B Phys Biol Sci       Date:  2013       Impact factor: 3.493

9.  Secretor Status Is Strongly Associated with Microbial Alterations Observed during Pregnancy.

Authors:  Himanshu Kumar; Pirjo Wacklin; Massalin Nakphaichit; Eliisa Loyttyniemi; Somak Chowdhury; Yogesh Shouche; Jaana Mättö; Erika Isolauri; Seppo Salminen
Journal:  PLoS One       Date:  2015-07-31       Impact factor: 3.240

10.  Faecal microbiota composition in adults is associated with the FUT2 gene determining the secretor status.

Authors:  Pirjo Wacklin; Jarno Tuimala; Janne Nikkilä; Harri Mäkivuokko; Noora Alakulppi; Pia Laine; Mirjana Rajilic-Stojanovic; Lars Paulin; Willem M de Vos; Jaana Mättö
Journal:  PLoS One       Date:  2014-04-14       Impact factor: 3.240

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