The Solution and Crystal Structures of a Module Pair from the Staphylococcus aureus-Binding Site of Human Fibronectin-A Tale with a Twist.

E Rudino-Pinera, RB Ravelli, GM Sheldrick, MH Nanao, VV Korostelev, JM Werner, Ulrich Schwarz-Linek, JR Potts, EF Garman

Research output: Contribution to journalArticlepeer-review

Abstract

An important goal of structural studies of modular proteins is to determine the inter-module orientation, which often influences biological function. The N-terminal domain of human fibronectin (Fn) is composed of a string of five type I modules (F1). Despite their small size, to date F1 modules have proved intractable to X-ray structure solution, although there are several NMR structures available. Here, we present the first structures (two X-ray models and an NMR-derived model) of the (2)F1(3)F1 module pair, which forms part of the binding site for Fn-binding proteins from pathogenic bacteria. The crystallographic structure determination was aided by the novel technique of UV radiation damage-induced phasing. The individual module structures are very similar in all three models. In the NMR structure and one of the X-ray structures, a similar but smaller interdomain interface than that observed previously for (4)F1(5)F1 is seen. The other X-ray structure has a different interdomain orientation. This work underlines the benefits of combining X-ray and NMR data in the studies of multi-domain proteins. (c) 2007 Elsevier Ltd. All rights reserved.

Original languageEnglish
Pages (from-to)833-844
Number of pages12
JournalJournal of Molecular Biology
Volume368
Issue number3
DOIs
Publication statusPublished - 4 May 2007

Keywords

  • fibronectin
  • crystallography
  • NMR
  • multidomains
  • domain orientation
  • MACROMOLECULAR STRUCTURES
  • MOLECULAR REPLACEMENT
  • PLASMINOGEN-ACTIVATOR
  • BACKBONE DYNAMICS
  • DIPOLAR COUPLINGS
  • GELATIN-BINDING
  • GROWTH-FACTOR
  • PROTEIN
  • DOMAINS
  • REFINEMENT

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