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Cited 4 time in webofscience Cited 5 time in scopus
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Structural transformation-mediated dimerization of caspase recruitment domain revealed by the crystal structure of CARD-only protein in frog virus 3

Authors
Kim, Chang MinHa, Hyun JiKwon, SungharkJeong, Jae-HeeLee, Sung HoonKim, Yeon-GilLee, Chang SupLee, Jun HyuckPark, Hyun Ho
Issue Date
1-Feb-2019
Publisher
Academic Press
Keywords
Apoptosis; Death domain superfamily; Caspase recruitment domain; CARD-only protein; Crystal structure; Domain swapping
Citation
Journal of Structural Biology, v.205, no.2, pp 189 - 195
Pages
7
Indexed
SCI
SCIE
SCOPUS
Journal Title
Journal of Structural Biology
Volume
205
Number
2
Start Page
189
End Page
195
URI
https://scholarworks.gnu.ac.kr/handle/sw.gnu/9450
DOI
10.1016/j.jsb.2018.12.006
ISSN
1047-8477
1095-8657
Abstract
Caspase recruitment domain (CARD)-only proteins (COPs), regulate apoptosis, inflammation, and innate immunity. They inhibit the assembly of NOD-like receptor complexes such as the inflammasome and NODosome, which are molecular complexes critical for caspase-1 activation. COPs are known to interact with either caspase-1 CARD or RIP2 CARD via a CARD-CARD interaction, and inhibit caspase-1 activation or further downstream signaling. In addition to the human COPs, Pseudo-ICE, INCA, and ICEBERG, several viruses also contain viral COPs that help them escape the host immune system. To elucidate the molecular mechanism of host immunity inhibition by viral COPs, we solved the structure of a viral COP for the first time. Our structure showed that viral COP forms a structural transformation-mediated dimer, which is unique and has not been reported in any structural study of a CARD domain. Based on the current structure, and the previously solved structures of other death domain superfamily members, we propose that structural transformation-mediated dimerization might be a new strategy for dimer assembly in the death domain superfamily.
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