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The 12 function of BRCT of the protein

S.NOUniprot IDProtein Name Sequence LengthBRCT Repeated RegionFunction
1 Q8NEM0 Microcephalin835Implicated in chromosome condensation and DNA damage induced cellular responses.
May play a role in neurogenesis and regulation of the size of the cerebral cortex.
2 Q92547 DNA topoisomerase 2-binding protein 1 1522Required for DNA replication.
Plays a role in the rescue of stalled replication forks and checkpoint control.
Binds double-stranded DNA breaks and nicks as well as single-stranded DNA.
Recruits the SWI/SNF chromatin remodeling complex to E2F1-responsive promoters.
Down-regulates E2F1 activity and inhibits E2F1-dependent apoptosis during G1/S transition and after DNA damage.
Induces a large increase in the kinase activity of ATR (PubMed:16530042).
3 Q9BQI6 SMC5-SMC6 complex localization factor protein 1 1058Plays a role in the DNA damage response (DDR) pathway by regulating postreplication repair of UV-damaged DNA and genomic stability maintenance (PubMed:25931565).
The SLF1-SLF2 complex acts to link RAD18 with the SMC5-SMC6 complex at replication-coupled interstrand cross-links (ICL) and DNA double-strand breaks (DSBs) sites on chromatin during DNA repair in response to stalled replication forks (PubMed:25931565).
Promotes the recruitment of SLF2 and the SMC5-SMC6 complex to DNA lesions (PubMed:25931565).
4 P38398 Breast cancer type 1 susceptibility protein 1863"E3 ubiquitin-protein ligase that specifically mediates the formation of 'Lys-6'-linked polyubiquitin chains and plays a central role in DNA repair by facilitating cellular responses to DNA damage.
It is unclear whether it also mediates the formation of other types of polyubiquitin chains.
The E3 ubiquitin-protein ligase activity is required for its tumor suppressor function.
The BRCA1-BARD1 heterodimer coordinates a diverse range of cellular pathways such as DNA damage repair, ubiquitination and transcriptional regulation to maintain genomic stability.
Regulates centrosomal microtubule nucleation.
Required for normal cell cycle progression from G2 to mitosis.
Required for appropriate cell cycle arrests after ionizing irradiation in both the S-phase and the G2 phase of the cell cycle.
Involved in transcriptional regulation of P21 in response to DNA damage.
Required for FANCD2 targeting to sites of DNA damage.
May function as a transcriptional regulator.
Inhibits lipid synthesis by binding to inactive phosphorylated ACACA and preventing its dephosphorylation.
Contributes to homologous recombination repair (HRR) via its direct interaction with PALB2, fine-tunes recombinational repair partly through its modulatory role in the PALB2-dependent loading of BRCA2-RAD51 repair machinery at DNA breaks.
Component of the BRCA1-RBBP8 complex which regulates CHEK1 activation and controls cell cycle G2/M checkpoints on DNA damage via BRCA1-mediated ubiquitination of RBBP8.
Acts as a transcriptional activator (PubMed:20160719)".
5 Q9H8V3 Protein ECT2 914"Guanine nucleotide exchange factor (GEF) that catalyzes the exchange of GDP for GTP.
Promotes guanine nucleotide exchange on the Rho family members of small GTPases, like RHOA, RHOC, RAC1 and CDC42.
Required for signal transduction pathways involved in the regulation of cytokinesis.
Component of the centralspindlin complex that serves as a microtubule-dependent and Rho-mediated signaling required for the myosin contractile ring formation during the cell cycle cytokinesis.
Regulates the translocation of RHOA from the central spindle to the equatorial region.
Plays a role in the control of mitotic spindle assembly; regulates the activation of CDC42 in metaphase for the process of spindle fibers attachment to kinetochores before chromosome congression.
Involved in the regulation of epithelial cell polarity; participates in the formation of epithelial tight junctions in a polarity complex PARD3-PARD6-protein kinase PRKCQ-dependent manner.
Plays a role in the regulation of neurite outgrowth.
Inhibits phenobarbital (PB)-induced NR1I3 nuclear translocation.
Stimulates the activity of RAC1 through its association with the oncogenic PARD6A-PRKCI complex in cancer cells, thereby acting to coordinately drive tumor cell proliferation and invasion.
Also stimulates genotoxic stress-induced RHOB activity in breast cancer cells leading to their cell death".
6 Q12888 TP53-binding protein 1 1972"Double-strand break (DSB) repair protein involved in response to DNA damage, telomere dynamics and class-switch recombination (CSR) during antibody genesis (PubMed:12364621, PubMed:22553214, PubMed:23333306, PubMed:17190600, PubMed:21144835, PubMed:28241136).
Plays a key role in the repair of double-strand DNA breaks (DSBs) in response to DNA damage by promoting non-homologous end joining (NHEJ)-mediated repair of DSBs and specifically counteracting the function of the homologous recombination (HR) repair protein BRCA1 (PubMed:22553214, PubMed:23727112, PubMed:23333306).
In response to DSBs, phosphorylation by ATM promotes interaction with RIF1 and dissociation from NUDT16L1/TIRR, leading to recruitment to DSBs sites (PubMed:28241136).
Recruited to DSBs sites by recognizing and binding histone H2A monoubiquitinated at 'Lys-15' (H2AK15Ub) and histone H4 dimethylated at 'Lys-20' (H4K20me2), two histone marks that are present at DSBs sites (PubMed:23760478, PubMed:28241136, PubMed:17190600).
Required for immunoglobulin class-switch recombination (CSR) during antibody genesis, a process that involves the generation of DNA DSBs (PubMed:23345425).
Participates to the repair and the orientation of the broken DNA ends during CSR (By similarity).
In contrast, it is not required for classic NHEJ and V(D)J recombination (By similarity).
Promotes NHEJ of dysfunctional telomeres via interaction with PAXIP1 (PubMed:23727112)".
7 P18887 DNA repair protein XRCC1 633"Involved in DNA single-strand break repair by mediating the assembly of DNA break repair protein complexes.
Probably during DNA repair, negatively regulates ADP-ribose levels by modulating ADP-ribosyltransferase PARP1 activity".
8 Q9UBU7 Protein DBF4 homolog A 674Regulatory subunit for CDC7 which activates its kinase activity thereby playing a central role in DNA replication and cell proliferation.
Required for progression of S phase.
The complex CDC7-DBF4A selectively phosphorylates MCM2 subunit at 'Ser-40' and 'Ser-53' and then is involved in regulating the initiation of DNA replication during cell cycle.
9 Q14676 Mediator of DNA damage checkpoint protein 1 2089"Required for checkpoint mediated cell cycle arrest in response to DNA damage within both the S phase and G2/M phases of the cell cycle.
May serve as a scaffold for the recruitment of DNA repair and signal transduction proteins to discrete foci of DNA damage marked by 'Ser-139' phosphorylation of histone H2AFX.
Also required for downstream events subsequent to the recruitment of these proteins.
These include phosphorylation and activation of the ATM, CHEK1 and CHEK2 kinases, and stabilization of TP53 and apoptosis.
ATM and CHEK2 may also be activated independently by a parallel pathway mediated by TP53BP1".
10 Q99728 BRCA1-associated RING domain protein 1 777"E3 ubiquitin-protein ligase.
The BRCA1-BARD1 heterodimer specifically mediates the formation of 'Lys-6'-linked polyubiquitin chains and coordinates a diverse range of cellular pathways such as DNA damage repair, ubiquitination and transcriptional regulation to maintain genomic stability.
Plays a central role in the control of the cell cycle in response to DNA damage.
Acts by mediating ubiquitin E3 ligase activity that is required for its tumor suppressor function.
Also forms a heterodimer with CSTF1/CSTF-50 to modulate mRNA processing and RNAP II stability by inhibiting pre-mRNA 3' cleavage".
11 P49917 DNA ligase 4 911"Efficiently joins single-strand breaks in a double-stranded polydeoxynucleotide in an ATP-dependent reaction.
Involved in DNA non-homologous end joining (NHEJ) required for double-strand break repair and V(D)J recombination.
The LIG4-XRCC4 complex is responsible for the NHEJ ligation step, and XRCC4 enhances the joining activity of LIG4.
Binding of the LIG4-XRCC4 complex to DNA ends is dependent on the assembly of the DNA-dependent protein kinase complex DNA-PK to these DNA ends".
12 Q6ZW49 PAX-interacting protein 1 1069"Involved in DNA damage response and in transcriptional regulation through histone methyltransferase (HMT) complexes.
Plays a role in early development.
In DNA damage response is required for cell survival after ionizing radiation.
In vitro shown to be involved in the homologous recombination mechanism for the repair of double-strand breaks (DSBs).
Its localization to DNA damage foci requires RNF8 and UBE2N.
Recruits TP53BP1 to DNA damage foci and, at least in particular repair processes, effective DNA damage response appears to require the association with TP53BP1 phosphorylated by ATM at 'Ser-25'.
Together with TP53BP1 regulates ATM association.
Proposed to recruit PAGR1 to sites of DNA damage and the PAGR1:PAXIP1 complex is required for cell survival in response to DNA damage; the function is probably independent of MLL-containing histone methyltransferase (HMT) complexes.
However, this function has been questioned (By similarity).
Promotes ubiquitination of PCNA following UV irradiation and may regulate recruitment of polymerase eta and RAD51 to chromatin after DNA damage.
Proposed to be involved in transcriptional regulation by linking MLL-containing histone methyltransferase (HMT) complexes to gene promoters by interacting with promoter-bound transcription factors such as PAX2.
Associates with gene promoters that are known to be regulated by KMT2D/MLL2.
During immunoglobulin class switching in activated B-cells is involved in trimethylation of histone H3 at 'Lys-4' and in transcription initiation of downstream switch regions at the immunoglobulin heavy-chain (Igh) locus; this function appears to involve the recruitment of MLL-containing HMT complexes.
Conflictingly, its function in transcriptional regulation during immunoglobulin class switching is reported to be independent of the MLL2/MLL3 complex (By similarity)".