CDB25:0004038 OMG — PTPRF

Experimentally validated in Human; Orthology-inferred in Mouse, Rat, Frog, Zebrafish, Chicken, Macaque, Pig, Dog, Cow, Chimp, Horse, Marmoset, Sheep

Title

Journal:; Year Published:

Abstract

Identification of orphan ligand-receptor relationships using a cell-based CRISPRa enrichment screening platform.

eLife, 2022; PubMed, Homo sapiens OMG — Homo sapiens PTPRF
ABSTRACT: Secreted proteins, which include cytokines, hormones, and growth factors, are extracellular ligands that control key signaling pathways mediating cell-cell communication within and between tissues and organs. Many drugs target secreted ligands and their cell surface receptors. Still, there are hundreds of secreted human proteins that either have no identified receptors ('orphans') or are likely to act through cell surface receptors that have not yet been characterized. Discovery of secreted ligand-receptor interactions by high-throughput screening has been problematic, because the most commonly used high-throughput methods for protein-protein interaction (PPI) screening are not optimized for extracellular interactions. Cell-based screening is a promising technology for the deorphanization of ligand-receptor interactions, because multimerized ligands can enrich for cells expressing low affinity cell surface receptors, and such methods do not require purification of receptor extracellular domains. Here, we present a proteo-genomic cell-based CRISPR activation (CRISPRa) enrichment screening platform employing customized pooled cell surface receptor sgRNA libraries in combination with a magnetic bead selection-based enrichment workflow for rapid, parallel ligand-receptor deorphanization. We curated 80 potentially high-value orphan secreted proteins and ultimately screened 20 secreted ligands against two cell sgRNA libraries with targeted expression of all single-pass (TM1) or multi-pass transmembrane (TM2+) receptors by CRISPRa. We identified previously unknown interactions in 12 of these screens, and validated several of them using surface plasmon resonance and/or cell binding assays. The newly deorphanized ligands include three receptor protein tyrosine phosphatase (RPTP) ligands and a chemokine-like protein that binds to killer immunoglobulin-like receptors (KIRs). These new interactions provide a resource for future investigations of interactions between the human-secreted and membrane proteomes.
Basic Information on OMG
Ligand Name: oligodendrocyte myelin glycoprotein
Other Symbols: OMGP
Ligand Location: cell membrane based on perplexity, uniprot
HGNC Gene Symbol Report: OMG
GeneCards: OMG
HGNC Gene Group: unknown
Functional Annotations for OMG
Gene Ontologies: PAN-GO, AmiGO 2
Expression Profile: Human Protein Atlas (RNA and protein), Human Cell Atlas (RNA), GEPIA cancer vs normal (RNA), GeneCards (RNA and protein)
Disease Annotations: MalaCards, OMIM, Open Targets Platform, DISEASES (text mining), AI summary (LLM)
Interactions with other Receptors for OMG
OMG — LINGO1OMG — RTN4ROMG — RTN4RL1OMG — PTPRDOMG — PTPRSOMG — PTPRU
Basic Information on PTPRF
Receptor Name: protein tyrosine phosphatase receptor type F
Other Symbols: LAR
Receptor Location: cell membrane based on perplexity
HGNC Gene Symbol Report: PTPRF
GeneCards: PTPRF
Functional Annotations for PTPRF
Gene Ontologies: PAN-GO, AmiGO 2
Expression Profile: Human Protein Atlas (RNA and protein), Human Cell Atlas (RNA), GEPIA cancer vs normal (RNA), GeneCards (RNA and protein)
Disease Annotations: MalaCards, OMIM, Open Targets Platform, DISEASES (text mining), AI summary (LLM)
Interactions with other Ligands for PTPRF
NID1 — PTPRFLRRC4B — PTPRFLAMC1 — PTPRFLRFN4 — PTPRFLRFN5 — PTPRF
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