-
Something wrong with this record ?
RAD18 directs DNA double-strand break repair by homologous recombination to post-replicative chromatin
M. Palek, N. Palkova, consortium CZECANCA , P. Kleiblova, Z. Kleibl, L. Macurek
Language English Country England, Great Britain
Document type Journal Article
Grant support
NU20-03-00285
Ministry of Health
LX22NPO5102
European Union Next Generation EU
352822
Grant Agency of the Charles University
LM2018129
MEYS
68378050-KAV-NPUI
RVO
CEP Register
NLK
Directory of Open Access Journals
from 2005
Free Medical Journals
from 1996
PubMed Central
from 1974
Europe PubMed Central
from 1974
Open Access Digital Library
from 1996-01-01 to 2030-12-31
Open Access Digital Library
from 1974-01-01
Open Access Digital Library
from 1996-01-01
Open Access Digital Library
from 1996-01-01
Medline Complete (EBSCOhost)
from 1996-01-01
Oxford Journals Open Access Collection
from 1996-01-01
ROAD: Directory of Open Access Scholarly Resources
from 1974
PubMed
38884202
DOI
10.1093/nar/gkae499
Knihovny.cz E-resources
- MeSH
- Tumor Suppressor p53-Binding Protein 1 * metabolism genetics MeSH
- Chromatin * metabolism genetics MeSH
- DNA-Binding Proteins * metabolism genetics MeSH
- DNA Breaks, Double-Stranded * MeSH
- Histones * metabolism MeSH
- Homologous Recombination genetics MeSH
- Humans MeSH
- DNA End-Joining Repair MeSH
- DNA Repair MeSH
- Cell Cycle Proteins metabolism genetics MeSH
- Recombinational DNA Repair MeSH
- DNA Replication MeSH
- Ubiquitination * MeSH
- Ubiquitin-Protein Ligases * metabolism genetics MeSH
- Check Tag
- Humans MeSH
- Publication type
- Journal Article MeSH
RAD18 is an E3 ubiquitin ligase that prevents replication fork collapse by promoting DNA translesion synthesis and template switching. Besides this classical role, RAD18 has been implicated in homologous recombination; however, this function is incompletely understood. Here, we show that RAD18 is recruited to DNA lesions by monoubiquitination of histone H2A at K15 and counteracts accumulation of 53BP1. Super-resolution microscopy revealed that RAD18 localizes to the proximity of DNA double strand breaks and limits the distribution of 53BP1 to the peripheral chromatin nanodomains. Whereas auto-ubiquitination of RAD18 mediated by RAD6 inhibits its recruitment to DNA breaks, interaction with SLF1 promotes RAD18 accumulation at DNA breaks in the post-replicative chromatin by recognition of histone H4K20me0. Surprisingly, suppression of 53BP1 function by RAD18 is not involved in homologous recombination and rather leads to reduction of non-homologous end joining. Instead, we provide evidence that RAD18 promotes HR repair by recruiting the SMC5/6 complex to DNA breaks. Finally, we identified several new loss-of-function mutations in RAD18 in cancer patients suggesting that RAD18 could be involved in cancer development.
References provided by Crossref.org
- 000
- 00000naa a2200000 a 4500
- 001
- bmc24019705
- 003
- CZ-PrNML
- 005
- 20241024110643.0
- 007
- ta
- 008
- 241015s2024 enk f 000 0|eng||
- 009
- AR
- 024 7_
- $a 10.1093/nar/gkae499 $2 doi
- 035 __
- $a (PubMed)38884202
- 040 __
- $a ABA008 $b cze $d ABA008 $e AACR2
- 041 0_
- $a eng
- 044 __
- $a enk
- 100 1_
- $a Palek, Matous $u Cancer Cell Biology, Institute of Molecular Genetics of the Czech Academy of Sciences, Prague CZ-14220, Czech Republic $u Department of Cell Biology, Faculty of Science, Charles University, Prague, Czech Republic
- 245 10
- $a RAD18 directs DNA double-strand break repair by homologous recombination to post-replicative chromatin / $c M. Palek, N. Palkova, consortium CZECANCA , P. Kleiblova, Z. Kleibl, L. Macurek
- 520 9_
- $a RAD18 is an E3 ubiquitin ligase that prevents replication fork collapse by promoting DNA translesion synthesis and template switching. Besides this classical role, RAD18 has been implicated in homologous recombination; however, this function is incompletely understood. Here, we show that RAD18 is recruited to DNA lesions by monoubiquitination of histone H2A at K15 and counteracts accumulation of 53BP1. Super-resolution microscopy revealed that RAD18 localizes to the proximity of DNA double strand breaks and limits the distribution of 53BP1 to the peripheral chromatin nanodomains. Whereas auto-ubiquitination of RAD18 mediated by RAD6 inhibits its recruitment to DNA breaks, interaction with SLF1 promotes RAD18 accumulation at DNA breaks in the post-replicative chromatin by recognition of histone H4K20me0. Surprisingly, suppression of 53BP1 function by RAD18 is not involved in homologous recombination and rather leads to reduction of non-homologous end joining. Instead, we provide evidence that RAD18 promotes HR repair by recruiting the SMC5/6 complex to DNA breaks. Finally, we identified several new loss-of-function mutations in RAD18 in cancer patients suggesting that RAD18 could be involved in cancer development.
- 650 _2
- $a lidé $7 D006801
- 650 12
- $a dvouřetězcové zlomy DNA $7 D053903
- 650 12
- $a chromatin $x metabolismus $x genetika $7 D002843
- 650 12
- $a DNA vazebné proteiny $x metabolismus $x genetika $7 D004268
- 650 12
- $a ubikvitinligasy $x metabolismus $x genetika $7 D044767
- 650 12
- $a 53BP1 $x metabolismus $x genetika $7 D000071857
- 650 12
- $a histony $x metabolismus $7 D006657
- 650 12
- $a ubikvitinace $7 D054875
- 650 _2
- $a homologní rekombinace $x genetika $7 D059765
- 650 _2
- $a rekombinační oprava DNA $7 D059767
- 650 _2
- $a replikace DNA $7 D004261
- 650 _2
- $a oprava DNA $7 D004260
- 650 _2
- $a proteiny buněčného cyklu $x metabolismus $x genetika $7 D018797
- 650 _2
- $a oprava DNA spojením konců $7 D059766
- 655 _2
- $a časopisecké články $7 D016428
- 700 1_
- $a Palkova, Natalie $u Cancer Cell Biology, Institute of Molecular Genetics of the Czech Academy of Sciences, Prague CZ-14220, Czech Republic $u Department of Cell Biology, Faculty of Science, Charles University, Prague, Czech Republic
- 700 1_
- $a Kleiblova, Petra $u Institute of Medical Biochemistry and Laboratory Diagnostics, First Faculty of Medicine, Charles University and General University Hospital in Prague, Prague, Czech Republic $1 https://orcid.org/0000000248069854 $7 xx0125463
- 700 1_
- $a Kleibl, Zdenek $u Institute of Medical Biochemistry and Laboratory Diagnostics, First Faculty of Medicine, Charles University and General University Hospital in Prague, Prague, Czech Republic
- 700 1_
- $a Macurek, Libor $u Cancer Cell Biology, Institute of Molecular Genetics of the Czech Academy of Sciences, Prague CZ-14220, Czech Republic $1 https://orcid.org/0000000209871238 $7 xx0128728
- 710 2_
- $a consortium CZECANCA
- 773 0_
- $w MED00003554 $t Nucleic acids research $x 1362-4962 $g Roč. 52, č. 13 (2024), s. 7687-7703
- 856 41
- $u https://pubmed.ncbi.nlm.nih.gov/38884202 $y Pubmed
- 910 __
- $a ABA008 $b sig $c sign $y - $z 0
- 990 __
- $a 20241015 $b ABA008
- 991 __
- $a 20241024110637 $b ABA008
- 999 __
- $a ok $b bmc $g 2202124 $s 1231678
- BAS __
- $a 3
- BAS __
- $a PreBMC-MEDLINE
- BMC __
- $a 2024 $b 52 $c 13 $d 7687-7703 $e 20240722 $i 1362-4962 $m Nucleic acids research $n Nucleic Acids Res $x MED00003554
- GRA __
- $a NU20-03-00285 $p Ministry of Health
- GRA __
- $a LX22NPO5102 $p European Union Next Generation EU
- GRA __
- $a 352822 $p Grant Agency of the Charles University
- GRA __
- $a LM2018129 $p MEYS
- GRA __
- $a 68378050-KAV-NPUI $p RVO
- LZP __
- $a Pubmed-20241015
