Literature DB >> 10688205

Shiga-like toxins are neutralized by tailored multivalent carbohydrate ligands.

P I Kitov1, J M Sadowska, G Mulvey, G D Armstrong, H Ling, N S Pannu, R J Read, D R Bundle.   

Abstract

The diseases caused by Shiga and cholera toxins account for the loss of millions of lives each year. Both belong to the clinically significant subset of bacterial AB5 toxins consisting of an enzymatically active A subunit that gains entry to susceptible mammalian cells after oligosaccharide recognition by the B5 homopentamer. Therapies might target the obligatory oligosaccharide-toxin recognition event, but the low intrinsic affinity of carbohydrate-protein interactions hampers the development of low-molecular-weight inhibitors. The toxins circumvent low affinity by binding simultaneously to five or more cell-surface carbohydrates. Here we demonstrate the use of the crystal structure of the B5 subunit of Escherichia coli O157:H7 Shiga-like toxin I (SLT-I) in complex with an analogue of its carbohydrate receptor to design an oligovalent, water-soluble carbohydrate ligand (named STARFISH), with subnanomolar inhibitory activity. The in vitro inhibitory activity is 1-10-million-fold higher than that of univalent ligands and is by far the highest molar activity of any inhibitor yet reported for Shiga-like toxins I and II. Crystallography of the STARFISH/Shiga-like toxin I complex explains this activity. Two trisaccharide receptors at the tips of each of five spacer arms simultaneously engage all five B subunits of two toxin molecules.

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Year:  2000        PMID: 10688205     DOI: 10.1038/35001095

Source DB:  PubMed          Journal:  Nature        ISSN: 0028-0836            Impact factor:   49.962


  164 in total

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Journal:  EMBO J       Date:  2000-11-15       Impact factor: 11.598

Review 2.  Affinity enhancement by multivalent lectin-carbohydrate interaction.

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Journal:  Glycoconj J       Date:  2000 Jul-Sep       Impact factor: 2.916

3.  Application of click-click chemistry to the synthesis of new multivalent RGD conjugates.

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4.  Using modularly assembled ligands to bind RNA internal loops separated by different distances.

Authors:  Jessica L Childs-Disney; Pavel B Tsitovich; Matthew D Disney
Journal:  Chembiochem       Date:  2011-08-09       Impact factor: 3.164

5.  Polyvalent inhibitors of anthrax toxin that target host receptors.

Authors:  Saleem Basha; Prakash Rai; Vincent Poon; Arundhati Saraph; Kunal Gujraty; Mandy Y Go; Skanda Sadacharan; Mia Frost; Jeremy Mogridge; Ravi S Kane
Journal:  Proc Natl Acad Sci U S A       Date:  2006-08-28       Impact factor: 11.205

6.  Synthesis of potent inhibitors of anthrax toxin based on poly-L-glutamic acid.

Authors:  Amit Joshi; Arundhati Saraph; Vincent Poon; Jeremy Mogridge; Ravi S Kane
Journal:  Bioconjug Chem       Date:  2006 Sep-Oct       Impact factor: 4.774

7.  Polymer-Based Therapeutics.

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Review 8.  Antibody therapy in the management of shiga toxin-induced hemolytic uremic syndrome.

Authors:  Saul Tzipori; Abhineet Sheoran; Donna Akiyoshi; Arthur Donohue-Rolfe; Howard Trachtman
Journal:  Clin Microbiol Rev       Date:  2004-10       Impact factor: 26.132

Review 9.  Multivalent glycoconjugates as anti-pathogenic agents.

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Journal:  Chem Soc Rev       Date:  2012-12-19       Impact factor: 54.564

10.  Controlling the specificity of modularly assembled small molecules for RNA via ligand module spacing: targeting the RNAs that cause myotonic muscular dystrophy.

Authors:  Melissa M Lee; Jessica L Childs-Disney; Alexei Pushechnikov; Jonathan M French; Krzysztof Sobczak; Charles A Thornton; Matthew D Disney
Journal:  J Am Chem Soc       Date:  2009-12-02       Impact factor: 15.419

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