POLQ

Gene Information

Official Symbol: POLQ
Official Name: DNA polymerase theta
Aliases and Previous Symbols: N/A
Entrez ID: 10721
UniProt: O75417
Interactions: BioGRID
PubMed articles: Open PubMed
OMIM: Open OMIM

Function Summary

Entrez Summary: N/A
UniProt Summary: DNA polymerase that promotes microhomology-mediated end- joining (MMEJ), an alternative non-homologous end-joining (NHEJ) machinery triggered in response to double-strand breaks in DNA (PubMed:25642963, PubMed:25643323). MMEJ is an error-prone repair pathway that produces deletions of sequences from the strand being repaired and promotes genomic rearrangements, such as telomere fusions, some of them leading to cellular transformation (PubMed:25642963, PubMed:25643323). POLQ acts as an inhibitor of homology-recombination repair (HR) pathway by limiting RAD51 accumulation at resected ends (PubMed:25642963). POLQ-mediated MMEJ may be required to promote the survival of cells with a compromised HR repair pathway, thereby preventing genomic havoc by resolving unrepaired lesions (By similarity). The polymerase acts by binding directly the 2 ends of resected double-strand breaks, allowing microhomologous sequences in the overhangs to form base pairs. It then extends each strand from the base-paired region using the opposing overhang as a template. Requires partially resected DNA containing 2 to 6 base pairs of microhomology to perform MMEJ (PubMed:25643323). The polymerase activity is highly promiscuous: unlike most polymerases, promotes extension of ssDNA and partial ssDNA (pssDNA) substrates (PubMed:18503084, PubMed:21050863, PubMed:22135286). Also exhibits low-fidelity DNA synthesis, translesion synthesis and lyase activity, and it is implicated in interstrand-cross-link repair, base excision repair and DNA end-joining (PubMed:14576298, PubMed:18503084, PubMed:19188258, PubMed:24648516). Involved in somatic hypermutation of immunoglobulin genes, a process that requires the activity of DNA polymerases to ultimately introduce mutations at both A/T and C/G base pairs (By similarity). {ECO:0000250|UniProtKB:Q8CGS6, ECO:0000269|PubMed:14576298, ECO:0000269|PubMed:18503084, ECO:0000269|PubMed:19188258, ECO:0000269|PubMed:21050863, ECO:0000269|PubMed:22135286, ECO:0000269|PubMed:24648516, ECO:0000269|PubMed:25642963, ECO:0000269|PubMed:25643323}.

Pfam Domains GO Terms

CRISPR Data

Compound Hit Most Correlated Genes in Chemogenomics Tissues where Essential in the Avana Dataset (DepMap 20Q1)

Global Fraction of Cell Lines Where Essential: 7/739

Tissue	Fraction Of Cell Lines Where Essential
1290807.0	0/1
909776.0	0/1
bile duct	1/28
blood	1/28
bone	0/26
breast	1/33
central nervous system	0/56
cervix	0/4
colorectal	1/17
esophagus	0/13
fibroblast	0/1
gastric	1/16
kidney	0/21
liver	0/20
lung	0/75
lymphocyte	1/16
ovary	0/26
pancreas	0/24
peripheral nervous system	0/16
plasma cell	0/15
prostate	0/1
skin	0/24
soft tissue	0/9
thyroid	0/2
upper aerodigestive	0/22
urinary tract	0/29
uterus	0/5

Essentiality in NALM6

Essentiality Rank: 6059
Expression level (log2 read counts): 7.26

Expression Distribution

Screen	Score
Nutlin-3A 1.6μM R06 exp294	-2.89
Genistein 15μM R07 exp360	-1.74

Helicase C
DNA pol A
DEAD

double-strand break repair via alternative nonhomologous end joining
5-deoxyribose-5-phosphate lyase activity
single-stranded DNA helicase activity
somatic hypermutation of immunoglobulin genes
negative regulation of double-strand break repair via homologous recombination
somatic diversification of immune receptors via somatic mutation
DNA-directed DNA polymerase activity
negative regulation of double-strand break repair
negative regulation of DNA repair
somatic diversification of immunoglobulins
base-excision repair
negative regulation of DNA recombination
regulation of double-strand break repair via homologous recombination
somatic diversification of immune receptors
damaged DNA binding
double-strand break repair via nonhomologous end joining
non-recombinational repair
regulation of double-strand break repair
negative regulation of response to DNA damage stimulus
double-strand break repair via homologous recombination
recombinational repair
regulation of DNA recombination
DNA biosynthetic process
DNA duplex unwinding
DNA geometric change
DNA-dependent DNA replication
negative regulation of DNA metabolic process
chromosome
regulation of DNA repair
immunoglobulin production
production of molecular mediator of immune response
double-strand break repair
DNA replication
regulation of response to DNA damage stimulus
DNA recombination
DNA conformation change
protein homooligomerization
regulation of DNA metabolic process
chromatin binding
DNA repair