Ecto-Fc MS identifies ligand-receptor interactions through extracellular domain Fc fusion protein baits and shotgun proteomic analysis

Jeffrey N. Savas; Joris De Wit; Davide Comoletti; Roland Zemla; Anirvan Ghosh; John R. Yates

doi:10.1038/nprot.2014.140

Ecto-Fc MS identifies ligand-receptor interactions through extracellular domain Fc fusion protein baits and shotgun proteomic analysis

Jeffrey N. Savas, Joris De Wit, Davide Comoletti, Roland Zemla, Anirvan Ghosh, John R. Yates

Research output: Contribution to journal › Article › peer-review

16 Scopus citations

Abstract

Ligand-receptor interactions represent essential biological triggers that regulate many diverse and important cellular processes. We have developed a discovery-based proteomic biochemical protocol that couples affinity purification with multidimensional liquid chromatographic tandem mass spectrometry (LCLC-MS/MS) and bioinformatic analysis. Compared with previous approaches, our analysis increases sensitivity, shortens analysis duration and boosts comprehensiveness. In this protocol, receptor extracellular domains are fused with the Fc region of IgG to generate fusion proteins that are purified from transfected HEK293T cells. These 'ecto-Fcs' are coupled to protein A beads and serve as baits for binding assays with prey proteins extracted from rodent brain. After capture, the affinity-purified proteins are digested into peptides and comprehensively analyzed by LCLC-MS/MS with ion-trap mass spectrometers. In 4 working days, this protocol can generate shortlists of candidate ligand-receptor protein-protein interactions. Our 'ecto-Fc MS' approach outperforms antibody-based approaches and provides a reproducible and robust framework for identifying extracellular ligand-receptor interactions.

Original language	English (US)
Pages (from-to)	2061-2074
Number of pages	14
Journal	Nature Protocols
Volume	9
Issue number	9
DOIs	https://doi.org/10.1038/nprot.2014.140
State	Published - Sep 2014

All Science Journal Classification (ASJC) codes

General Biochemistry, Genetics and Molecular Biology

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10.1038/nprot.2014.140

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@article{8260023295e8484787e8ac16c7610e97,

title = "Ecto-Fc MS identifies ligand-receptor interactions through extracellular domain Fc fusion protein baits and shotgun proteomic analysis",

abstract = "Ligand-receptor interactions represent essential biological triggers that regulate many diverse and important cellular processes. We have developed a discovery-based proteomic biochemical protocol that couples affinity purification with multidimensional liquid chromatographic tandem mass spectrometry (LCLC-MS/MS) and bioinformatic analysis. Compared with previous approaches, our analysis increases sensitivity, shortens analysis duration and boosts comprehensiveness. In this protocol, receptor extracellular domains are fused with the Fc region of IgG to generate fusion proteins that are purified from transfected HEK293T cells. These 'ecto-Fcs' are coupled to protein A beads and serve as baits for binding assays with prey proteins extracted from rodent brain. After capture, the affinity-purified proteins are digested into peptides and comprehensively analyzed by LCLC-MS/MS with ion-trap mass spectrometers. In 4 working days, this protocol can generate shortlists of candidate ligand-receptor protein-protein interactions. Our 'ecto-Fc MS' approach outperforms antibody-based approaches and provides a reproducible and robust framework for identifying extracellular ligand-receptor interactions.",

author = "Savas, {Jeffrey N.} and {De Wit}, Joris and Davide Comoletti and Roland Zemla and Anirvan Ghosh and Yates, {John R.}",

note = "Funding Information: acKnoWleDGMents We thank M. O{\textquoteright}Sullivan, B. Fonslow, B. Stein and J. Moresco, and members of the Yates and Ghosh laboratories for their feedback on the project, and S. Von Daake for suggestions on the manuscript. We thank T. S{\"u}dhof (Stanford University) for his generosity in providing the original plasmids of β-NRXN1. This plasmid has been modified to accommodate many different genes and suit a variety of applications, but the original high-expression backbone remains unchanged. J.N.S. is supported by a US National Institutes of Health (NIH) Pathway to Independence Award K99DC013805-01. The Yates laboratory is supported by R01 MH068770, P41 GM103533, R01MH100175 and HHSN268201000035C grants from NIH. We also acknowledge support from NIH grants R01NS067216 and R01MH068578 to A.G. and NIH RO1-MH092906 to D.C., as well as the Robert Wood Johnson Foundation (grant no. 67038) for their support of the Child Health Institute of New Jersey. J.D.W. is funded by a NARSAD Young Investigator Award from the Brain and Behavior Research Foundation, a European Research Council (ERC) Starting Grant (no. 311083) and a Research Foundation Flanders (FWO) Odysseus Grant.",

year = "2014",

month = sep,

doi = "10.1038/nprot.2014.140",

language = "English (US)",

volume = "9",

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AU - Savas, Jeffrey N.

AU - De Wit, Joris

AU - Comoletti, Davide

AU - Zemla, Roland

AU - Ghosh, Anirvan

AU - Yates, John R.

N1 - Funding Information: acKnoWleDGMents We thank M. O’Sullivan, B. Fonslow, B. Stein and J. Moresco, and members of the Yates and Ghosh laboratories for their feedback on the project, and S. Von Daake for suggestions on the manuscript. We thank T. Südhof (Stanford University) for his generosity in providing the original plasmids of β-NRXN1. This plasmid has been modified to accommodate many different genes and suit a variety of applications, but the original high-expression backbone remains unchanged. J.N.S. is supported by a US National Institutes of Health (NIH) Pathway to Independence Award K99DC013805-01. The Yates laboratory is supported by R01 MH068770, P41 GM103533, R01MH100175 and HHSN268201000035C grants from NIH. We also acknowledge support from NIH grants R01NS067216 and R01MH068578 to A.G. and NIH RO1-MH092906 to D.C., as well as the Robert Wood Johnson Foundation (grant no. 67038) for their support of the Child Health Institute of New Jersey. J.D.W. is funded by a NARSAD Young Investigator Award from the Brain and Behavior Research Foundation, a European Research Council (ERC) Starting Grant (no. 311083) and a Research Foundation Flanders (FWO) Odysseus Grant.

PY - 2014/9

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N2 - Ligand-receptor interactions represent essential biological triggers that regulate many diverse and important cellular processes. We have developed a discovery-based proteomic biochemical protocol that couples affinity purification with multidimensional liquid chromatographic tandem mass spectrometry (LCLC-MS/MS) and bioinformatic analysis. Compared with previous approaches, our analysis increases sensitivity, shortens analysis duration and boosts comprehensiveness. In this protocol, receptor extracellular domains are fused with the Fc region of IgG to generate fusion proteins that are purified from transfected HEK293T cells. These 'ecto-Fcs' are coupled to protein A beads and serve as baits for binding assays with prey proteins extracted from rodent brain. After capture, the affinity-purified proteins are digested into peptides and comprehensively analyzed by LCLC-MS/MS with ion-trap mass spectrometers. In 4 working days, this protocol can generate shortlists of candidate ligand-receptor protein-protein interactions. Our 'ecto-Fc MS' approach outperforms antibody-based approaches and provides a reproducible and robust framework for identifying extracellular ligand-receptor interactions.

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Ecto-Fc MS identifies ligand-receptor interactions through extracellular domain Fc fusion protein baits and shotgun proteomic analysis

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