1998
DOI: 10.1002/jlb.64.6.767
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Expression of a structural domain of the β2 subunit essential for αMβ2 ligand recognition

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Cited by 8 publications
(9 citation statements)
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References 45 publications
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“…CD18 function-blocking mAbs may competitively block integrin-ligand contact, as contact sites recognized by these blocking mAbs lie in the I-like domain of the CD18 subunit that is necessary for ligand binding (14,15). We found that several function-blocking CD18 mAbs prevented the stimulus-induced binding of 327A, 327C, and 330E activation epitope mAbs.…”
Section: Discussionmentioning
confidence: 78%
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“…CD18 function-blocking mAbs may competitively block integrin-ligand contact, as contact sites recognized by these blocking mAbs lie in the I-like domain of the CD18 subunit that is necessary for ligand binding (14,15). We found that several function-blocking CD18 mAbs prevented the stimulus-induced binding of 327A, 327C, and 330E activation epitope mAbs.…”
Section: Discussionmentioning
confidence: 78%
“…One truncation encoded the amino terminus corresponding to aa 23-457, which consists of the CD18 subunit I-like domain and a critical intrachain disulfide bond (14). A second truncation expressed the cysteine-rich extracellular stalk, residues 411-700.…”
Section: Cd18-blocking Abs Prevent the Induction Of The Activation Epmentioning
confidence: 99%
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“…However, because additional sites contributing to ligand binding are predicted in both the ␣L subunit (Stanley et al, 1994) and the ␤2 subunit (Goodman and Bajt, 1996;Goodman et al, 1998), it was possible that an I domaindeleted LFA-1 might bind ligand similarly to a non-I domain-containing integrin. The data in the present study clearly demonstrate that there is no residual ICAM-1 or ICAM-3 ligand binding capacity in ⌬I-LFA-1.…”
Section: Discussionmentioning
confidence: 99%
“…1) does not directly contribute to ligand binding although it may contain regulatory elements (27). Analogously, the ␤ 3 -and ␤ 2 -subunit C termini have been shown to be unnecessary for ligand binding, since removal of these domains by truncation followed by co-expression with the relevant full-length ␣-subunit generated functional integrins (8,51). Interestingly, both of these ␤-subunit truncations maintained conserved cysteine residues and thereby retained a disulfide knot between the N terminus and mid-section of the ␤-subunit, which was proposed to aid structural integrity (52).…”
mentioning
confidence: 99%