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- W4313331504 abstract "Abstract Using a lymphocyte binding assay, we have previously demonstrated that the CD4 protein can mediate cell adhesion by direct interaction with MHC class II molecules. In this report, we have used this assay to test whether synthetic peptides, corresponding to DRβ sequences, could inhibit CD4-class II adhesion. A peptide derived from sequences within the β1 domain (DRβ41–55), as well as two peptides derived from sequences within the β2 domain (DRβ121–135 and DRβ141–155), were shown to inhibit CD4-class II adhesion. Inasmuch as a site for CD4 binding in the β2 domain had been previously documented, these studies were designed to investigate the role of the β1 domain as an additional site of interaction with CD4. Sixteen site-specific mutations were engineered within the β1 domain of DRβ1*0101. Several mutations were shown to disrupt CD4-dependent T cell activation. Based on these results, we propose a model for the molecular interaction of CD4 with MHC class II proteins in which both the β1 and β2 domains of class II interact with the two amino-terminal Ig-like domains of CD4." @default.
- W4313331504 created "2023-01-06" @default.
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- W4313331504 date "1998-11-15" @default.
- W4313331504 modified "2023-10-11" @default.
- W4313331504 title "A Site for CD4 Binding in the β1 Domain of the MHC Class II Protein HLA-DR1" @default.
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- W4313331504 doi "https://doi.org/10.4049/jimmunol.161.10.5472" @default.
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