| Literature DB >> 27881823 |
Welbeck Danquah1, Catherine Meyer-Schwesinger2, Björn Rissiek1,3, Carolina Pinto1, Arnau Serracant-Prat1, Miriam Amadi1, Domenica Iacenda1,3, Jan-Hendrik Knop1,2, Anna Hammel1,2, Philine Bergmann1,4, Nicole Schwarz1, Joana Assunção5, Wendy Rotthier5, Friedrich Haag1, Eva Tolosa1, Peter Bannas1,6, Eric Boué-Grabot4, Tim Magnus3, Toon Laeremans5, Catelijne Stortelers5, Friedrich Koch-Nolte7.
Abstract
Ion channels are desirable therapeutic targets, yet ion channel-directed drugs with high selectivity and few side effects are still needed. Unlike small-molecule inhibitors, antibodies are highly selective for target antigens but mostly fail to antagonize ion channel functions. Nanobodies-small, single-domain antibody fragments-may overcome these problems. P2X7 is a ligand-gated ion channel that, upon sensing adenosine 5'-triphosphate released by damaged cells, initiates a proinflammatory signaling cascade, including release of cytokines, such as interleukin-1β (IL-1β). To further explore its function, we generated and characterized nanobodies against mouse P2X7 that effectively blocked (13A7) or potentiated (14D5) gating of the channel. Systemic injection of nanobody 13A7 in mice blocked P2X7 on T cells and macrophages in vivo and ameliorated experimental glomerulonephritis and allergic contact dermatitis. We also generated nanobody Dano1, which specifically inhibited human P2X7. In endotoxin-treated human blood, Dano1 was 1000 times more potent in preventing IL-1β release than small-molecule P2X7 antagonists currently in clinical development. Our results show that nanobody technology can generate potent, specific therapeutics against ion channels, confirm P2X7 as a therapeutic target for inflammatory disorders, and characterize a potent new drug candidate that targets P2X7.Entities:
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Year: 2016 PMID: 27881823 DOI: 10.1126/scitranslmed.aaf8463
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956