BAIT

POL1

CDC17, CRT5, HPR3, DNA-directed DNA polymerase alpha catalytic subunit POL1, L000000257, YNL102W

Catalytic subunit of the DNA polymerase I alpha-primase complex; required for the initiation of DNA replication during mitotic DNA synthesis and premeiotic DNA synthesis

GO Process (11)

GO Function (1)

GO Component (3)

Gene Ontology Molecular Function

DNA-directed DNA polymerase activity [IDA]

Gene Ontology Cellular Component

alpha DNA polymerase:primase complex [IDA]

mitochondrion [IDA]

replication fork [IDA]

SGD Alliance of Genome Resources Entrez Gene RefSeq UniprotKB

Saccharomyces cerevisiae (S288c)

PREY

URA7

CTP synthase URA7, L000002436, YBL039C

Major CTP synthase isozyme (see also URA8); catalyzes the ATP-dependent transfer of the amide nitrogen from glutamine to UTP, forming CTP, the final step in de novo biosynthesis of pyrimidines; involved in phospholipid biosynthesis; capable of forming cytoplasmic filaments termed cytoophidium, especially during conditions of glucose depletion; URA7 has a paralog, URA8, that arose from the whole genome duplication

GO Process (3)

GO Function (1)

GO Component (2)

Gene Ontology Biological Process

CTP biosynthetic process [IDA]

phospholipid biosynthetic process [IMP]

pyrimidine nucleobase biosynthetic process [IMP]

Gene Ontology Molecular Function

CTP synthase activity [IDA, IMP, ISS]

Gene Ontology Cellular Component

cytoophidium [IDA]

cytoplasm [IDA]

SGD Alliance of Genome Resources Entrez Gene RefSeq UniprotKB

Saccharomyces cerevisiae (S288c)

Phenotypic Enhancement

A genetic interaction is inferred when mutation or overexpression of one gene results in enhancement of any phenotype (other than lethality/growth defect) associated with mutation or over expression of another gene.

Publication

Alterations in cellular metabolism triggered by URA7 or GLN3 inactivation cause imbalanced dNTP pools and increased mutagenesis.

Schmidt TT, Reyes G, Gries K, Ceylan C Ue, Sharma S, Meurer M, Knop M, Chabes A, Hombauer H

Eukaryotic DNA replication fidelity relies on the concerted action of DNA polymerase nucleotide selectivity, proofreading activity, and DNA mismatch repair (MMR). Nucleotide selectivity and proofreading are affected by the balance and concentration of deoxyribonucleotide (dNTP) pools, which are strictly regulated by ribonucleotide reductase (RNR). Mutations preventing DNA polymerase proofreading activity or MMR function cause mutator phenotypes and consequently increased cancer ... [more]

Proc. Natl. Acad. Sci. U.S.A. May. 30, 2017; 114(22);E4442-E4451 [Pubmed: 28416670]

Throughput

Low Throughput

Ontology Terms

mutation frequency (APO:0000198)

Additional Notes

double mutants show increased mutator phenotypes

Related interactions

Interaction	Experimental Evidence Code	Dataset	Throughput	Score	Curated By	Notes
POL1 URA7	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	-0.202	BioGRID	2008931

Curated By

BioGRID

Interaction Summary

POL1

Gene Ontology Biological Process

Gene Ontology Molecular Function

DNA-directed DNA polymerase activity [IDA]

Gene Ontology Cellular Component

URA7

Gene Ontology Biological Process

Gene Ontology Molecular Function

CTP synthase activity [IDA, IMP, ISS]

Gene Ontology Cellular Component

Phenotypic Enhancement

Publication

Alterations in cellular metabolism triggered by URA7 or GLN3 inactivation cause imbalanced dNTP pools and increased mutagenesis.

Throughput

Ontology Terms

Additional Notes

Related interactions

Curated By