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Structural basis for selectivity and antagonism in extracellular GPCR-nanobodies

Nat Commun. 2024-05; 
Roman R Schlimgen, Francis C Peterson, Raimond Heukers, Martine J Smit, John D McCorvy, Brian F Volkman
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Molecular Biology Reagents … coli expression and ordered from GenScript. VUN701 was cloned into a pET28a-6xHis-SUMO3 vector and expressed in BL21 DE3 E.coli. Amino acid substitutions were made using … Get A Quote

摘要

G protein-coupled receptors (GPCRs) are pivotal therapeutic targets, but their complex structure poses challenges for effective drug design. Nanobodies, or single-domain antibodies, have emerged as a promising therapeutic strategy to target GPCRs, offering advantages over traditional small molecules and antibodies. However, an incomplete understanding of the structural features enabling GPCR-nanobody interactions has limited their development. In this study, we investigate VUN701, a nanobody antagonist targeting the atypical chemokine receptor 3 (ACKR3). We determine that an extended CDR3 loop is required for ACKR3 binding. Uncommon in most nanobodies, an extended CDR3 is prevalent in GPCR-targeting nanobodies.... More

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