AB-type lectin (toxin/agglutinin) from mistletoe: differences in affinity of the two galactoside-binding Trp/Tyr-sites and regulation of their functionality by monomer/dimer equilibrium

doi:10.1093/glycob/cwl017

Glycobiology Advance Access originally published online on June 14, 2006
Glycobiology 2006 16(10):926-937; doi:10.1093/glycob/cwl017

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AB-type lectin (toxin/agglutinin) from mistletoe: differences in affinity of the two galactoside-binding Trp/Tyr-sites and regulation of their functionality by monomer/dimer equilibrium

Marta Jiménez², Sabine André³, Hans-C. Siebert³, Hans-J. Gabius³ and Dolores Solís¹^,2

² Instituto de Química Física Rocasolano, CSIC, Serrano 119, E-28006 Madrid, Spain; and ³ Institut für Physiologische Chemie, Tierärztliche Fakultät, Ludwig-Maximilians-Universität, Veterinärstrasse 13, D-80539 München, Germany

¹ To whom correspondence should be addressed; e-mail: d.solis{at}iqfr.csic.es

Received on February 8, 2006; revised on June 5, 2006; accepted on June 12, 2006

Viscumin of mistletoe (Viscum album L.) has a concentration-dependentactivity profile unique to plant AB-toxins. It starts with lectin-dependentmitogenicity and then covers toxicity and cell agglutination,associated with shifts in the monomer/dimer equilibrium. Eachlectin subunit harbors two sections for ligand contact. In thedimer, the B-chain sites in subdomain 2 ${gamma}$ (designated as the Tyr-sites)appear fully accessible, whereas Trp-sites in subdomain 1 ${alpha}$ areclose to the dimer interface. It is unclear whether both typesof sites operate similarly in binding glycoligands in solution.By systematically covering a broad range of lactose/lectin ratioin isothermal titration calorimetry, we obtained evidence fortwo sites showing dissimilar binding affinity. Intriguingly,the site with higher affinity was only partially occupied. Toassign the observed properties to the Trp/Tyr-sites, we nextperformed chemically induced dynamic nuclear polarization measurementsof Trp and Tyr accessibility. A Tyr signal, but not distinctTrp peaks, was recorded when testing the dimer. Lactose-quenchableTrp peaks became visible on the destabilization of the dimerby citraconylation, intimating Trp involvement in ligand contactin the monomer. Fittingly, Tyr acetylation but not mild Trpoxidation reduced the dimer hemagglutination activity and theextent of binding to asialofetuin–Sepharose 4B. Altogether,the results attribute lectin activity in the dimer primarilyto Tyr-sites. Full access to Trp-sites is gained on dimer dissociation.Thus, the monomer/dimer equilibrium of viscumin regulates theoperativity of these sites. Their structural divergence affordsthe possibility for differences in ligand selection when comparingmonomers (Tyr- and Trp-sites) with dimers (primarily Tyr-sites).

Key words: agglutinin / glycans / lectin / mistletoe / ribosome-inactivating protein

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