BAIT

EPHA2

ARCC2, CTPA, CTPP1, CTRCT6, ECK

EPH receptor A2

Synthetic Protein Interaction Project

GO Process (23)

GO Function (2)

GO Component (5)

Gene Ontology Biological Process

activation of Rac GTPase activity [IMP]

bone remodeling [ISS]

branching involved in mammary gland duct morphogenesis [ISS]

cell chemotaxis [IMP]

cell migration [IMP]

ephrin receptor signaling pathway [IDA]

intrinsic apoptotic signaling pathway in response to DNA damage [IDA]

keratinocyte differentiation [IMP]

lens fiber cell morphogenesis [ISS]

mammary gland epithelial cell proliferation [ISS]

multicellular organismal development [TAS]

negative regulation of protein kinase B signaling [IDA]

osteoblast differentiation [ISS]

osteoclast differentiation [ISS]

peptidyl-tyrosine phosphorylation [IDA]

positive regulation of establishment of protein localization to plasma membrane [IMP]

protein kinase B signaling [IDA]

regulation of ERK1 and ERK2 cascade [IMP]

regulation of angiogenesis [ISS]

regulation of blood vessel endothelial cell migration [ISS]

regulation of cell adhesion mediated by integrin [IDA]

regulation of lamellipodium assembly [IMP]

response to growth factor [IMP]

Gene Ontology Molecular Function

protein binding [IPI]
transmembrane receptor protein tyrosine kinase activity [IDA]

Gene Ontology Cellular Component

cell surface [IDA]

focal adhesion [IDA]

integral component of plasma membrane [IDA]

leading edge membrane [IDA]

plasma membrane [IDA]

CRISPR Database OMIM HGNC Alliance of Genome Resources VEGA Entrez Gene RefSeq UniprotKB Ensembl HPRD

Homo sapiens

PREY

HCK

JTK9, p59Hck, p61Hck, RP5-836N17.3

HCK proto-oncogene, Src family tyrosine kinase

GO Process (30)

GO Function (4)

GO Component (6)

Gene Ontology Biological Process

Fc-gamma receptor signaling pathway involved in phagocytosis [TAS]

cell adhesion [TAS]

cell differentiation [IBA]

cellular response to peptide hormone stimulus [IBA]

cytokine-mediated signaling pathway [TAS]

innate immune response [IBA, TAS]

innate immune response-activating signal transduction [TAS]

integrin-mediated signaling pathway [TAS]

interferon-gamma-mediated signaling pathway [TAS]

leukocyte degranulation [TAS]

leukocyte migration involved in immune response [TAS]

lipopolysaccharide-mediated signaling pathway [TAS]

mesoderm development [TAS]

negative regulation of apoptotic process [IMP]

peptidyl-tyrosine autophosphorylation [IBA]

peptidyl-tyrosine phosphorylation [IMP]

positive regulation of actin cytoskeleton reorganization [IDA, IMP]

positive regulation of actin filament polymerization [TAS]

positive regulation of cell proliferation [IMP]

protein autophosphorylation [IMP]

protein phosphorylation [TAS]

regulation of cell shape [IMP]

regulation of defense response to virus by virus [TAS]

regulation of inflammatory response [TAS]

regulation of phagocytosis [IMP]

regulation of podosome assembly [IDA]

regulation of sequence-specific DNA binding transcription factor activity [IMP]

respiratory burst after phagocytosis [TAS]

transmembrane receptor protein tyrosine kinase signaling pathway [IBA]

viral process [TAS]

Gene Ontology Molecular Function

non-membrane spanning protein tyrosine kinase activity [IBA]
protein binding [IPI]
protein tyrosine kinase activity [IMP]
receptor binding [IBA]

Gene Ontology Cellular Component

actin filament [IDA]

extrinsic component of cytoplasmic side of plasma membrane [IMP]

focal adhesion [IMP]

CRISPR Database VEGA OMIM HGNC Alliance of Genome Resources Entrez Gene RefSeq UniprotKB Ensembl HPRD

Homo sapiens

Positive Genetic

Mutations/deletions in separate genes, each of which alone causes a minimal phenotype, but when combined in the same cell results in a less severe fitness defect than expected under a given condition. This term is reserved for high or low throughput studies with scores.

Publication

Synergistic drug combinations for cancer identified in a CRISPR screen for pairwise genetic interactions.

Han K, Jeng EE, Hess GT, Morgens DW, Li A, Bassik MC

Identification of effective combination therapies is critical to address the emergence of drug-resistant cancers, but direct screening of all possible drug combinations is infeasible. Here we introduce a CRISPR-based double knockout (CDKO) system that improves the efficiency of combinatorial genetic screening using an effective strategy for cloning and sequencing paired single guide RNA (sgRNA) libraries and a robust statistical scoring ... [more]

Nat. Biotechnol. Mar. 20, 2017; 0(); [Pubmed: 28319085]

Quantitative Score

2.86 [Confidence Score]

Throughput

High Throughput

Ontology Terms

growth abnormality (HP:0001507)

Additional Notes

CRISPR GI screen
Cell Line:K562 (EFO:0002067)
Experimental Setup:Timecourse
GIST: A-phenotypic positive genetic interaction
Library:Drug Target-CDKO CRISPRn library
Significance Threshold: q-value<0.05

Curated By

BioGRID