Selected article for: "crystal structure and key residue"

Author: Laing, Eric D.; Navaratnarajah, Chanakha K.; Cheliout Da Silva, Sofia; Petzing, Stephanie R.; Xu, Yan; Sterling, Spencer L.; Marsh, Glenn A.; Wang, Lin-Fa; Amaya, Moushimi; Nikolov, Dimitar B.; Cattaneo, Roberto; Broder, Christopher C.; Xu, Kai
Title: Structural and functional analyses reveal promiscuous and species specific use of ephrin receptors by Cedar virus
  • Cord-id: d22fs0fx
  • Document date: 2019_10_8
  • ID: d22fs0fx
    Snippet: Cedar virus (CedV) is a bat-borne henipavirus related to Nipah virus (NiV) and Hendra virus (HeV), zoonotic agents of fatal human disease. CedV receptor-binding protein (G) shares only ∼30% sequence identity with those of NiV and HeV, although they can all use ephrin-B2 as an entry receptor. We demonstrate that CedV also enters cells through additional B- and A-class ephrins (ephrin-B1, ephrin-A2, and ephrin-A5) and report the crystal structure of the CedV G ectodomain alone and in complex wit
    Document: Cedar virus (CedV) is a bat-borne henipavirus related to Nipah virus (NiV) and Hendra virus (HeV), zoonotic agents of fatal human disease. CedV receptor-binding protein (G) shares only ∼30% sequence identity with those of NiV and HeV, although they can all use ephrin-B2 as an entry receptor. We demonstrate that CedV also enters cells through additional B- and A-class ephrins (ephrin-B1, ephrin-A2, and ephrin-A5) and report the crystal structure of the CedV G ectodomain alone and in complex with ephrin-B1 or ephrin-B2. The CedV G receptor-binding site is structurally distinct from other henipaviruses, underlying its capability to accommodate additional ephrin receptors. We also show that CedV can enter cells through mouse ephrin-A1 but not human ephrin-A1, which differ by 1 residue in the key contact region. This is evidence of species specific ephrin receptor usage by a henipavirus, and implicates additional ephrin receptors in potential zoonotic transmission.

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