XRCC6

Gene Information

Official Symbol: XRCC6
Official Name: X-ray repair cross complementing 6
Aliases and Previous Symbols: N/A
Entrez ID: 2547
UniProt: P12956
Interactions: BioGRID
PubMed articles: Open PubMed
OMIM: Open OMIM

Function Summary

Entrez Summary: N/A
UniProt Summary: Single-stranded DNA-dependent ATP-dependent helicase. Has a role in chromosome translocation. The DNA helicase II complex binds preferentially to fork-like ends of double-stranded DNA in a cell cycle-dependent manner. It works in the 3'-5' direction. Binding to DNA may be mediated by XRCC6. Involved in DNA non-homologous end joining (NHEJ) required for double-strand break repair and V(D)J recombination. The XRCC5/6 dimer acts as regulatory subunit of the DNA-dependent protein kinase complex DNA-PK by increasing the affinity of the catalytic subunit PRKDC to DNA by 100-fold. The XRCC5/6 dimer is probably involved in stabilizing broken DNA ends and bringing them together. The assembly of the DNA-PK complex to DNA ends is required for the NHEJ ligation step. Required for osteocalcin gene expression. Probably also acts as a 5'-deoxyribose-5-phosphate lyase (5'-dRP lyase), by catalyzing the beta-elimination of the 5' deoxyribose- 5-phosphate at an abasic site near double-strand breaks. 5'-dRP lyase activity allows to 'clean' the termini of abasic sites, a class of nucleotide damage commonly associated with strand breaks, before such broken ends can be joined. The XRCC5/6 dimer together with APEX1 acts as a negative regulator of transcription. Plays a role in the regulation of DNA virus-mediated innate immune response by assembling into the HDP-RNP complex, a complex that serves as a platform for IRF3 phosphorylation and subsequent innate immune response activation through the cGAS-STING pathway. {ECO:0000269|PubMed:12145306, ECO:0000269|PubMed:20383123, ECO:0000269|PubMed:20493174, ECO:0000269|PubMed:2466842, ECO:0000269|PubMed:28712728, ECO:0000269|PubMed:7957065, ECO:0000269|PubMed:8621488, ECO:0000269|PubMed:9742108}.

Pfam Domains GO Terms

CRISPR Data

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

Screen	Score
CI-1040 9.5μM R08 exp472	-2.08
BI-2536 0.02μM R03 exp96	-1.82
Etoposide 1μM R00 exp19	-1.75
RS-1 10μM R08 exp519	1.76
Temozolomide 200μM R04 exp189	1.85
Tubastatin-A 2.5μM R07 exp417	2.02

Global Fraction of Cell Lines Where Essential: 734/739

Tissue	Fraction Of Cell Lines Where Essential
1290807.0	1/1
909776.0	1/1
bile duct	28/28
blood	28/28
bone	26/26
breast	32/33
central nervous system	56/56
cervix	4/4
colorectal	17/17
esophagus	13/13
fibroblast	1/1
gastric	16/16
kidney	21/21
liver	19/20
lung	75/75
lymphocyte	16/16
ovary	26/26
pancreas	24/24
peripheral nervous system	16/16
plasma cell	15/15
prostate	1/1
skin	24/24
soft tissue	9/9
thyroid	2/2
upper aerodigestive	21/22
urinary tract	29/29
uterus	5/5

Essentiality in NALM6

Essentiality Rank: 596
Expression level (log2 read counts): 9.04

Expression Distribution

Gene	Correlation
RRM1	0.534
CHD4	0.426
TBC1D3G	0.417
PSMC1	0.407
RBM8A	0.405

SAP
Ku
Ku N
Ku C

Ku70:Ku80 complex
cellular hyperosmotic salinity response
double-strand break repair via classical nonhomologous end joining
5-deoxyribose-5-phosphate lyase activity
establishment of integrated proviral latency
cellular response to salt stress
nonhomologous end joining complex
establishment of viral latency
double-stranded telomeric DNA binding
hyperosmotic salinity response
nuclear telomere cap complex
cellular response to X-ray
cellular hyperosmotic response
viral latency
DNA ligation
response to salt stress
hyperosmotic response
telomeric DNA binding
response to X-ray
cellular response to gamma radiation
cyclin binding
protein heterotetramerization
cellular response to osmotic stress
protein-DNA complex
damaged DNA binding
response to gamma radiation
double-strand break repair via nonhomologous end joining
DNA helicase activity
non-recombinational repair
cellular response to ionizing radiation
response to osmotic stress
positive regulation of type I interferon production
telomere maintenance
telomere organization
double-stranded DNA binding
protein heterooligomerization
nuclear chromosome, telomeric region
DNA duplex unwinding
secretory granule lumen
DNA geometric change