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PDBsum entry 4y8a
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Cell adhesion
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PDB id
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4y8a
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References listed in PDB file
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Key reference
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Title
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Diverse oligomeric states of ceacam igv domains.
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Authors
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D.A.Bonsor,
S.Günther,
R.Beadenkopf,
D.Beckett,
E.J.Sundberg.
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Ref.
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Proc Natl Acad Sci U S A, 2015,
112,
13561-13566.
[DOI no: ]
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PubMed id
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Abstract
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Carcinoembryonic antigen-related cell adhesion molecules (CEACAMs) comprise a
large family of cell surface adhesion molecules that bind to themselves and
other family members to carry out numerous cellular functions, including
proliferation, signaling, differentiation, tumor suppression, and survival. They
also play diverse and significant roles in immunity and infection. The formation
of CEACAM oligomers is caused predominantly by interactions between their
N-terminal IgV domains. Although X-ray crystal structures of CEACAM IgV domain
homodimers have been described, how CEACAMs form heterodimers or remain monomers
is poorly understood. To address this key aspect of CEACAM function, we
determined the crystal structures of IgV domains that form a homodimeric CEACAM6
complex, monomeric CEACAM8, and a heterodimeric CEACAM6-CEACAM8 complex. To
confirm and quantify these interactions in solution, we used analytical
ultracentrifugation to measure the dimerization constants of CEACAM homodimers
and isothermal titration calorimetry to determine the thermodynamic parameters
and binding affinities of CEACAM heterodimers. We found the CEACAM6-CEACAM8
heterodimeric state to be substantially favored energetically relative to the
CEACAM6 homodimer. Our data provide a molecular basis for the adoption of the
diverse oligomeric states known to exist for CEACAMs and suggest ways in which
CEACAM6 and CEACAM8 regulate the biological functions of one another, as well as
of additional CEACAMs with which they interact, both in cis and in trans.
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