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Antibodies expand the scope of angiotensin receptor pharmacology.

Meredith A SkibaSarah M SterlingShaun RawsonShuhao ZhangHuixin XuHaoran JiangGenevieve R NemethMorgan S A GilmanJoseph D HurleyPeng-Xiang ShenDean P StausJihee KimConor McMahonMaria K LehtinenHoward A RockmanPatrick BarthLaura M WinglerAndrew C Kruse
Published in: Nature chemical biology (2024)
G-protein-coupled receptors (GPCRs) are key regulators of human physiology and are the targets of many small-molecule research compounds and therapeutic drugs. While most of these ligands bind to their target GPCR with high affinity, selectivity is often limited at the receptor, tissue and cellular levels. Antibodies have the potential to address these limitations but their properties as GPCR ligands remain poorly characterized. Here, using protein engineering, pharmacological assays and structural studies, we develop maternally selective heavy-chain-only antibody ('nanobody') antagonists against the angiotensin II type I receptor and uncover the unusual molecular basis of their receptor antagonism. We further show that our nanobodies can simultaneously bind to angiotensin II type I receptor with specific small-molecule antagonists and demonstrate that ligand selectivity can be readily tuned. Our work illustrates that antibody fragments can exhibit rich and evolvable pharmacology, attesting to their potential as next-generation GPCR modulators.
Keyphrases
  • angiotensin ii
  • small molecule
  • angiotensin converting enzyme
  • vascular smooth muscle cells
  • protein protein
  • binding protein
  • endothelial cells
  • risk assessment
  • transcription factor
  • climate change
  • single cell