| Literature DB >> 30638538 |
Sinem Ozgul1, Sventja von Daake1, Sumie Kakehi1, Davide Sereni1, Natalia Denissova2, Carlie Hanlon2, Yuanpeng Janet Huang2, John K Everett2, Cuifeng Yin2, Gaetano T Montelione3, Davide Comoletti4.
Abstract
Cell surface molecules are important for development and function of multicellular organisms. Although several methods are available to identify ligand-receptor pairs, ELISA-based methods are particularly amenable to high-throughput screens. ELISA-based methods have high sensitivity and low false-positive rates for detecting protein-protein interaction (PPI) complexes. Here, we provide a detailed protocol for a 384-well ELISA-based PPI screening protocol for the identification of novel cell surface ligand-receptor interactions, together with considerations for validation of PPIs by biophysical methods. This PPI screen has been developed and tested for discovery of novel ligand-receptor pairs between human synaptic adhesion proteins, believed to play crucial roles in many steps of neurodevelopment, from neuronal maturation, to axon guidance, synapse connectivity, and pruning.Entities:
Keywords: Gene synthesis; Glycosylation; HEK cells; Mammalian cell surface proteins; NMR spectroscopy; Protein–protein interaction screen; Small-angle X-ray scattering; X-ray crystallography
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Year: 2018 PMID: 30638538 DOI: 10.1016/bs.mie.2018.10.001
Source DB: PubMed Journal: Methods Enzymol ISSN: 0076-6879 Impact factor: 1.600