Unknown

Dataset Information

0

Structural Basis of CD160:HVEM Recognition.

ABSTRACT: CD160 is a signaling molecule that interacts with herpes virus entry mediator (HVEM) and contributes to a wide range of immune responses, including T cell inhibition, natural killer cell activation, and mucosal immunity. GPI-anchored and transmembrane isoforms of CD160 share the same ectodomain responsible for HVEM engagement, which leads to bidirectional signaling. Despite the importance of the CD160:HVEM signaling axis and its therapeutic relevance, the structural and mechanistic basis underlying CD160-HVEM engagement has not been described. We report the crystal structures of the human CD160 extracellular domain and its complex with human HVEM. CD160 adopts a unique variation of the immunoglobulin fold and exists as a monomer in solution. The CD160:HVEM assembly exhibits a 1:1 stoichiometry and a binding interface similar to that observed in the BTLA:HVEM complex. Our work reveals the chemical and physical determinants underlying CD160:HVEM recognition and initiation of associated signaling processes.

SUBMITTER: Liu W 

PROVIDER: S-EPMC7477951 | biostudies-literature | 2019 Aug

REPOSITORIES: biostudies-literature

Json Xml
altmetric image

Publications

Structural Basis of CD160:HVEM Recognition.

Liu Weifeng W   Garrett Sarah C SC   Fedorov Elena V EV   Ramagopal Udupi A UA   Garforth Scott J SJ   Bonanno Jeffrey B JB   Almo Steven C SC  

Structure (London, England : 1993) 20190620 8

CD160 is a signaling molecule that interacts with herpes virus entry mediator (HVEM) and contributes to a wide range of immune responses, including T cell inhibition, natural killer cell activation, and mucosal immunity. GPI-anchored and transmembrane isoforms of CD160 share the same ectodomain responsible for HVEM engagement, which leads to bidirectional signaling. Despite the importance of the CD160:HVEM signaling axis and its therapeutic relevance, the structural and mechanistic basis underly  ...[more]

Similar Datasets

Unknown HVEM and CD160: Regulators of Immunopathology During Malaria Blood-Stage.
| S-EPMC6243049 | biostudies-literature
Unknown Redesigning HVEM Interface for Selective Binding to LIGHT, BTLA, and CD160.
| S-EPMC7642093 | biostudies-literature
Unknown A structural model of the immune checkpoint CD160-HVEM complex derived from HDX-mass spectrometry and molecular modeling.
| S-EPMC6355189 | biostudies-literature
Unknown HVEM structures and mutants reveal distinct functions of binding to LIGHT and BTLA/CD160.
| S-EPMC8558838 | biostudies-literature
Unknown Allosteric regulation of binding specificity of HVEM for CD160 and BTLA ligands upon G89F mutation.
| S-EPMC8666650 | biostudies-literature
Genomics Structural basis of H2A.Z recognition and H4K20 methylation by SUV420H2
2023-12-04 | GSE210197 | GEO
Genomics Structural basis of nucleosomal H4K20 recognition and methylation by SUV420H1 methyltransferase
2023-12-04 | GSE236249 | GEO
Genomics Structural basis for the recognition of GC-motifs by Smad4 transcription factor
2017-11-03 | GSE102784 | GEO
Unknown Associations between HVEM/LIGHT/BTLA/CD160 polymorphisms and the occurrence of antibody-mediate rejection in renal transplant recipients.
| S-EPMC5725004 | biostudies-literature
Unknown Structural basis for DNA recognition by FOXC2.
| S-EPMC6468292 | biostudies-literature