产品: | RUNX1 / AML1 抗体 |
货号: | AF6934 |
描述: | Rabbit polyclonal antibody to RUNX1 / AML1 |
应用: | WB |
反应: | Human |
分子量: | 49kD(Calculated). |
蛋白号: | Q01196 |
RRID: | AB_2847724 |
产品描述
*The optimal dilutions should be determined by the end user.
*Tips:
WB: 适用于变性蛋白样本的免疫印迹检测. IHC: 适用于组织样本的石蜡(IHC-p)或冰冻(IHC-f)切片样本的免疫组化/荧光检测. IF/ICC: 适用于细胞样本的荧光检测. ELISA(peptide): 适用于抗原肽的ELISA检测.
引用格式: Affinity Biosciences Cat# AF6934, RRID:AB_2847724.
展开/折叠
Acute myeloid leukemia 1; Acute myeloid leukemia 1 protein; alpha subunit core binding factor; AML 1; AML1; AML1 EVI 1; AML1 EVI 1 fusion protein; Aml1 oncogene; AMLCR 1; AMLCR1; CBF alpha 2; CBF-alpha-2; CBFA 2; CBFA2; Core binding factor alpha 2 subunit; Core binding factor runt domain alpha subunit 2; Core-binding factor subunit alpha-2; EVI 1; EVI1; HGNC; Oncogene AML 1; Oncogene AML-1; OTTHUMP00000108696; OTTHUMP00000108697; OTTHUMP00000108699; OTTHUMP00000108700; OTTHUMP00000108702; PEA2 alpha B; PEA2-alpha B; PEBP2 alpha B; PEBP2-alpha B; PEBP2A2; PEBP2aB; Polyomavirus enhancer binding protein 2 alpha B subunit; Polyomavirus enhancer-binding protein 2 alpha B subunit; Run1; Runt related transcription factor 1; Runt-related transcription factor 1; RUNX 1; Runx1; RUNX1_HUMAN; SL3 3 enhancer factor 1 alpha B subunit; SL3-3 enhancer factor 1 alpha B subunit; SL3/AKV core binding factor alpha B subunit; SL3/AKV core-binding factor alpha B subunit;
抗原和靶标
A synthesized peptide derived from human RUNX1 / AML1.
Expressed in all tissues examined except brain and heart. Highest levels in thymus, bone marrow and peripheral blood.
- Q01196 RUNX1_HUMAN:
- Protein BLAST With
- NCBI/
- ExPASy/
- Uniprot
MRIPVDASTSRRFTPPSTALSPGKMSEALPLGAPDAGAALAGKLRSGDRSMVEVLADHPGELVRTDSPNFLCSVLPTHWRCNKTLPIAFKVVALGDVPDGTLVTVMAGNDENYSAELRNATAAMKNQVARFNDLRFVGRSGRGKSFTLTITVFTNPPQVATYHRAIKITVDGPREPRRHRQKLDDQTKPGSLSFSERLSELEQLRRTAMRVSPHHPAPTPNPRASLNHSTAFNPQPQSQMQDTRQIQPSPPWSYDQSYQYLGSIASPSVHPATPISPGRASGMTTLSAELSSRLSTAPDLTAFSDPRQFPALPSISDPRMHYPGAFTYSPTPVTSGIGIGMSAMGSATRYHTYLPPPYPGSSQAQGGPFQASSPSYHLYYGASAGSYQFSMVGGERSPPRILPPCTNASTGSALLNPSLPNQSDVVEAEGSHSNSPTNMAPSARLEEAVWRPY
翻译修饰 - Q01196 作为底物
Site | PTM Type | Enzyme | Source |
---|---|---|---|
T14 | Phosphorylation | Uniprot | |
S17 | Phosphorylation | Uniprot | |
T18 | Phosphorylation | Uniprot | |
S21 | Phosphorylation | Q00534 (CDK6) , P06493 (CDK1) | Uniprot |
K24 | Acetylation | Uniprot | |
K24 | Ubiquitination | Uniprot | |
K43 | Acetylation | Uniprot | |
K43 | Ubiquitination | Uniprot | |
S50 | Phosphorylation | Uniprot | |
S67 | Phosphorylation | Uniprot | |
K83 | Ubiquitination | Uniprot | |
K90 | Ubiquitination | Uniprot | |
K125 | Ubiquitination | Uniprot | |
K144 | Ubiquitination | Uniprot | |
K167 | Ubiquitination | Uniprot | |
K182 | Ubiquitination | Uniprot | |
K188 | Acetylation | Uniprot | |
K188 | Ubiquitination | Uniprot | |
S191 | Phosphorylation | Uniprot | |
S193 | Phosphorylation | Uniprot | |
S199 | Phosphorylation | Uniprot | |
R206 | Methylation | Uniprot | |
T207 | Phosphorylation | Uniprot | |
R210 | Methylation | Uniprot | |
S212 | Phosphorylation | Uniprot | |
T219 | Phosphorylation | Uniprot | |
R223 | Methylation | Uniprot | |
S225 | Phosphorylation | Uniprot | |
S229 | Phosphorylation | Uniprot | |
T230 | Phosphorylation | Uniprot | |
S238 | Phosphorylation | Uniprot | |
S249 | Phosphorylation | P28482 (MAPK1) , Q00534 (CDK6) , Q9H2X6 (HIPK2) , P24941 (CDK2) , P06493 (CDK1) | Uniprot |
S253 | Phosphorylation | Uniprot | |
Y254 | Phosphorylation | Uniprot | |
S257 | Phosphorylation | Uniprot | |
Y258 | Phosphorylation | Uniprot | |
S263 | Phosphorylation | Uniprot | |
S266 | Phosphorylation | P28482 (MAPK1) , P24941 (CDK2) , Q00534 (CDK6) , P06493 (CDK1) | Uniprot |
S268 | Phosphorylation | Uniprot | |
T273 | Phosphorylation | Q9H2X6 (HIPK2) , P24941 (CDK2) , P06493 (CDK1) , P28482 (MAPK1) , Q00534 (CDK6) | Uniprot |
S276 | Phosphorylation | P24941 (CDK2) , P28482 (MAPK1) , P06493 (CDK1) , Q00534 (CDK6) , Q9H2X6 (HIPK2) | Uniprot |
S292 | Phosphorylation | Uniprot | |
S295 | Phosphorylation | Uniprot | |
T296 | Phosphorylation | Uniprot | |
R319 | Methylation | Uniprot | |
S329 | Phosphorylation | Uniprot | |
T331 | Phosphorylation | Uniprot | |
S397 | Phosphorylation | P06493 (CDK1) , Q00534 (CDK6) | Uniprot |
S423 | Phosphorylation | Uniprot | |
S433 | Phosphorylation | Uniprot | |
S435 | Phosphorylation | Uniprot | |
Y453 | Phosphorylation | Uniprot |
研究背景
Forms the heterodimeric complex core-binding factor (CBF) with CBFB. RUNX members modulate the transcription of their target genes through recognizing the core consensus binding sequence 5'-TGTGGT-3', or very rarely, 5'-TGCGGT-3', within their regulatory regions via their runt domain, while CBFB is a non-DNA-binding regulatory subunit that allosterically enhances the sequence-specific DNA-binding capacity of RUNX. The heterodimers bind to the core site of a number of enhancers and promoters, including murine leukemia virus, polyomavirus enhancer, T-cell receptor enhancers, LCK, IL3 and GM-CSF promoters (Probable). Essential for the development of normal hematopoiesis. Acts synergistically with ELF4 to transactivate the IL-3 promoter and with ELF2 to transactivate the BLK promoter. Inhibits KAT6B-dependent transcriptional activation (By similarity). Involved in lineage commitment of immature T cell precursors. CBF complexes repress ZBTB7B transcription factor during cytotoxic (CD8+) T cell development. They bind to RUNX-binding sequence within the ZBTB7B locus acting as transcriptional silencer and allowing for cytotoxic T cell differentiation. CBF complexes binding to the transcriptional silencer is essential for recruitment of nuclear protein complexes that catalyze epigenetic modifications to establish epigenetic ZBTB7B silencing (By similarity). Controls the anergy and suppressive function of regulatory T-cells (Treg) by associating with FOXP3. Activates the expression of IL2 and IFNG and down-regulates the expression of TNFRSF18, IL2RA and CTLA4, in conventional T-cells. Positively regulates the expression of RORC in T-helper 17 cells (By similarity).
Isoform AML-1G shows higher binding activities for target genes and binds TCR-beta-E2 and RAG-1 target site with threefold higher affinity than other isoforms. It is less effective in the context of neutrophil terminal differentiation.
Isoform AML-1L interferes with the transactivation activity of RUNX1.
Phosphorylated in its C-terminus upon IL-6 treatment. Phosphorylation enhances interaction with KAT6A.
Methylated.
Phosphorylated in Ser-249 Thr-273 and Ser-276 by HIPK2 when associated with CBFB and DNA. This phosphorylation promotes subsequent EP300 phosphorylation.
Nucleus.
Expressed in all tissues examined except brain and heart. Highest levels in thymus, bone marrow and peripheral blood.
Heterodimer with CBFB. RUNX1 binds DNA as a monomer and through the Runt domain. DNA-binding is increased by heterodimerization. Isoform AML-1L can neither bind DNA nor heterodimerize. Interacts with TLE1 and ALYREF/THOC4. Interacts with ELF1, ELF2 and SPI1. Interacts via its Runt domain with the ELF4 N-terminal region. Interaction with ELF2 isoform 2 (NERF-1a) may act to repress RUNX1-mediated transactivation. Interacts with KAT6A and KAT6B. Interacts with SUV39H1, leading to abrogation of transactivating and DNA-binding properties of RUNX1. Interacts with YAP1. Interacts with HIPK2 (By similarity). Interaction with CDK6 prevents myeloid differentiation, reducing its transcription transactivation activity. Found in a complex with PRMT5, RUNX1 and CBFB. Interacts with FOXP3. Interacts with TBX21 (By similarity). Interacts with DPF2.
A proline/serine/threonine rich region at the C-terminus is necessary for transcriptional activation of target genes.
研究领域
· Cellular Processes > Cellular community - eukaryotes > Tight junction. (View pathway)
· Human Diseases > Cancers: Overview > Pathways in cancer. (View pathway)
· Human Diseases > Cancers: Overview > Transcriptional misregulation in cancer.
· Human Diseases > Cancers: Specific types > Chronic myeloid leukemia. (View pathway)
· Human Diseases > Cancers: Specific types > Acute myeloid leukemia. (View pathway)
· Organismal Systems > Immune system > Th17 cell differentiation. (View pathway)
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