| Literature DB >> 30581043 |
Anna-Katharina Apel1, Robert K Y Cheng2, Christofer S Tautermann1, Michael Brauchle2, Chia-Ying Huang3, Alexander Pautsch1, Michael Hennig2, Herbert Nar1, Gisela Schnapp4.
Abstract
We determined two crystal structures of the chemokine receptor CCR2A in complex with the orthosteric antagonist MK-0812. Full-length CCR2A, stabilized by rubredoxin and a series of five mutations were resolved at 3.3 Å. An N- and C-terminally truncated CCR2A construct was crystallized in an alternate crystal form, which yielded a 2.7 Å resolution structure using serial synchrotron crystallography. Our structures provide a clear structural explanation for the observed key role of residue E2917.39 in high-affinity binding of several orthosteric CCR2 antagonists. By combining all the structural information collected, we generated models of co-structures for the structurally diverse pyrimidine amide class of CCR2 antagonists. Even though the representative Ex15 overlays well with MK-0812, it also interacts with the non-conserved H1213.33, resulting in a significant selectivity over CCR5. Insights derived from this work will facilitate drug discovery efforts directed toward highly selective CCR2 antagonists with potentially superior efficacy.Entities:
Keywords: CCR2; GPCR; IMISX in situ crystallization; MK-0812; chemokine receptor; protein engineering; serial crystallography
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Year: 2018 PMID: 30581043 DOI: 10.1016/j.str.2018.10.027
Source DB: PubMed Journal: Structure ISSN: 0969-2126 Impact factor: 5.006