AI Article Synopsis

  • VLRs are specialized proteins that play a key role in the immune response of jawless vertebrates by recognizing complex sugar structures, like the Thomsen-Friedenreich antigen (TFα).
  • Through detailed binding studies, researchers found that the VLRB.aGPA.23 has a unique structural setup, involving a hydrophobic cage formed by tryptophan residues that precisely fits the TFα disaccharide.
  • Unlike traditional lectins or antibodies that use long grooves for binding, VLRB.aGPA.23 has a distinctive concave surface that captures sugars, indicating a different mechanism for glycan recognition in this adaptive immune system.

Article Abstract

Variable lymphocyte receptors (VLRs) are leucine-rich repeat proteins that mediate adaptive immunity in jawless vertebrates. VLRs were recently shown to recognize glycans, such as the tumor-associated Thomsen-Friedenreich antigen (TFα; Galβ1-3GalNAcα), with a selectivity rivaling or exceeding that of lectins and antibodies. To understand the basis for TFα recognition by one such VLR (VLRB.aGPA.23), we measured thermodynamic parameters for the binding interaction and determined the structure of the VLRB.aGPA.23-TFα complex to 2.2 Å resolution. In the structure, four tryptophan residues form a tight hydrophobic cage encasing the TFα disaccharide that completely excludes buried water molecules. This cage together with hydrogen bonding of sugar hydroxyls to polar side chains explains the exquisite selectivity of VLRB.aGPA.23. The topology of the glycan-binding site of VLRB.aGPA.23 differs markedly from those of lectins or antibodies, which typically consist of long, convex grooves for accommodating the oligosaccharide. Instead, the TFα disaccharide is sandwiched between a variable loop and the concave surface of the VLR formed by the β-strands of the leucine-rich repeat modules. Longer oligosaccharides are predicted to extend perpendicularly across the β-strands, requiring them to bend to match the concavity of the VLR solenoid.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3949333PMC
http://dx.doi.org/10.1074/jbc.M113.480467DOI Listing

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