BAIT

CHL1

CTF1, LPA9, MCM12, L000000318, YPL008W

Probable DNA helicase; involved in sister-chromatid cohesion and genome integrity and interstrand cross-link repair; interacts with ECO1 and CTF18; mutants are defective in silencing, rDNA recombination, aging and the heat shock response; FANCJ-like helicase family member; mutations in the human homolog, DDX11/ChLR1, cause Warsaw breakage syndrome

GO Process (3)

GO Function (1)

GO Component (2)

Gene Ontology Biological Process

establishment of sister chromatid cohesion [IMP]

interstrand cross-link repair [IGI]

mitotic sister chromatid cohesion [IGI, IMP, IPI]

Gene Ontology Molecular Function

DNA helicase activity [IMP, ISS]

Gene Ontology Cellular Component

nuclear chromatin [IMP]

nucleus [IDA]

SGD Alliance of Genome Resources Entrez Gene RefSeq UniprotKB

Saccharomyces cerevisiae (S288c)

PREY

BIM1

YEB1, microtubule-binding protein BIM1, EB1, L000003272, YER016W

Microtubule plus end-tracking protein; together with Kar9p makes up the cortical microtubule capture site and delays the exit from mitosis when the spindle is oriented abnormally

GO Process (7)

GO Function (3)

GO Component (6)

Gene Ontology Biological Process

microtubule depolymerization [IMP]

microtubule nucleation [IPI]

mitotic sister chromatid cohesion [IGI, IMP]

mitotic spindle assembly checkpoint [TAS]

negative regulation of microtubule depolymerization [IMP]

nuclear migration along microtubule [IMP]

positive regulation of microtubule polymerization [IDA]

Gene Ontology Molecular Function

microtubule plus-end binding [IDA]
protein homodimerization activity [IDA]
structural constituent of cytoskeleton [IPI]

Gene Ontology Cellular Component

cytoplasmic microtubule [IDA]

microtubule plus-end [IDA]

spindle [IDA]

spindle midzone [IDA]

spindle pole [IDA]

spindle pole body [IDA]

SGD Alliance of Genome Resources Entrez Gene RefSeq UniprotKB

Saccharomyces cerevisiae (S288c)

Synthetic Lethality

A genetic interaction is inferred when mutations or deletions in separate genes, each of which alone causes a minimal phenotype, result in lethality when combined in the same cell under a given condition.

Publication

Modeling DNA trapping of anticancer therapeutic targets using missense mutations identifies dominant synthetic lethal interactions.

Hamza A, Amitzi L, Ma L, Driessen MRM, O'Neil NJ, Hieter P

Genetic screens can identify synthetic lethal (SL) interactions and uncover potential anticancer therapeutic targets. However, most SL screens have utilized knockout or knockdown approaches that do not accurately mimic chemical inhibition of a target protein. Here, we test whether missense mutations can be utilized as a model for a type of protein inhibition that creates a dominant gain-of-function cytotoxicity. We ... [more]

Proc Natl Acad Sci U S A Dec. 06, 2020; 118(14); [Pubmed: 33782138]

Throughput

Low Throughput

Ontology Terms

phenotype: viability (APO:0000111)

Related interactions

Interaction	Experimental Evidence Code	Dataset	Throughput	Score	Curated By	Notes
CHL1 BIM1	Negative Genetic Negative Genetic Mutations/deletions in separate genes, each of which alone causes a minimal phenotype, but when combined in the same cell results in a more severe fitness defect or lethality under a given condition. This term is reserved for high or low throughput studies with scores.	Collins SR (2007)	High	-15.0052	BioGRID	213439
BIM1 CHL1	Negative Genetic Negative Genetic Mutations/deletions in separate genes, each of which alone causes a minimal phenotype, but when combined in the same cell results in a more severe fitness defect or lethality under a given condition. This term is reserved for high or low throughput studies with scores.	Costanzo M (2016)	High	-0.3517	BioGRID	2107092
CHL1 BIM1	Negative Genetic Negative Genetic Mutations/deletions in separate genes, each of which alone causes a minimal phenotype, but when combined in the same cell results in a more severe fitness defect or lethality under a given condition. This term is reserved for high or low throughput studies with scores.	Ming Sun S (2020)	High	-	BioGRID	3492217
CHL1 BIM1	Synthetic Growth Defect Synthetic Growth Defect A genetic interaction is inferred when mutations in separate genes, each of which alone causes a minimal phenotype, result in a significant growth defect under a given condition when combined in the same cell.	Dixon SJ (2008)	High	-	BioGRID	341388
BIM1 CHL1	Synthetic Lethality Synthetic Lethality A genetic interaction is inferred when mutations or deletions in separate genes, each of which alone causes a minimal phenotype, result in lethality when combined in the same cell under a given condition.	Pan X (2004)	High	-	BioGRID	166500
BIM1 CHL1	Synthetic Lethality Synthetic Lethality A genetic interaction is inferred when mutations or deletions in separate genes, each of which alone causes a minimal phenotype, result in lethality when combined in the same cell under a given condition.	Tong AH (2004)	High	-	BioGRID	109369
CHL1 BIM1	Synthetic Lethality Synthetic Lethality A genetic interaction is inferred when mutations or deletions in separate genes, each of which alone causes a minimal phenotype, result in lethality when combined in the same cell under a given condition.	Tong AH (2004)	High	-	BioGRID	109370

Curated By

BioGRID

Interaction Summary

CHL1

Gene Ontology Biological Process

Gene Ontology Molecular Function

DNA helicase activity [IMP, ISS]

Gene Ontology Cellular Component

BIM1

Gene Ontology Biological Process

Gene Ontology Molecular Function

microtubule plus-end binding [IDA]protein homodimerization activity [IDA]structural constituent of cytoskeleton [IPI]

Gene Ontology Cellular Component

Synthetic Lethality

Publication

Modeling DNA trapping of anticancer therapeutic targets using missense mutations identifies dominant synthetic lethal interactions.

Throughput

Ontology Terms

Related interactions

Curated By

microtubule plus-end binding [IDA]
protein homodimerization activity [IDA]
structural constituent of cytoskeleton [IPI]