FITC标记的磷酸化急性髓细胞白血病1蛋白抗体-抗体-抗体-生物在线

FITC标记的磷酸化急性髓细胞白血病1蛋白抗体

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产品名称： FITC标记的磷酸化急性髓细胞白血病1蛋白抗体

英文名称： Anti-phospho-RUNX1 (Ser266)/FITC

产品编号： HZ-3024R-FITC

产品价格： null

产品产地：中国/上海

品牌商标： HZbscience

更新时间： 2023-08-17T10:24:20

使用范围： ICC=1:50-200 IF=1:50-200

上海沪震实业有限公司

联系人 : 鲍丽雯
地址 : 上海市闵行区闵北路88弄1-30号第22幢AQ136室
邮编 : 200612
所在区域 : 上海
电话 : 139****0749
传真 : 021-60345367
邮箱 : www.shzbio.net

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产品详情

Rabbit Anti-phospho-RUNX1 (Ser266)/FITC Conjugated antibody

FITC标记的磷酸化急性髓细胞白血病1蛋白抗体

英文名称	Anti-phospho-RUNX1 (Ser266)/FITC
中文名称	FITC标记的磷酸化急性髓细胞白血病1蛋白抗体
别名	RUNX1 (phospho-Ser266); p-RUNX1 (Ser266); RUNX1 (phospho S266); RUNX1 (phospho Ser266); Acute myeloid leukemia 1; Acute myeloid leukemia 1 protein; alpha subunit core binding factor; AML 1; AML1 EVI 1; Aml1 oncogene; AMLCR 1; AMLCR1; CBFA 2; CBFA2; Core binding factor alpha 2 subunit; Core binding factor runt domain alpha subunit 2; EVI 1; EVI1; HGNC; Oncogene AML 1; PEA2 alpha; PEBP2 alpha B; PEBP2A2; PEBP2aB; Polyomavirus enhancer binding protein 2 alpha B subunit; Run1; Runt related transcription factor 1; RUNX 1; SL3 3 enhancer factor 1 alpha B subunit; SL3/AKV core binding factor alpha B subunit; RUNX1_HUMAN.
规格价格	100ul/2980元购买大包装/询价
说明书	100ul
产品类型	磷酸化抗体
研究领域	肿瘤细胞生物细胞凋亡
抗体来源	Rabbit
克隆类型	Polyclonal
交叉反应	Human, Dog, Pig, Cow, Rabbit,
产品应用	ICC=1:50-200 IF=1:50-200 not yet tested in other applications. optimal dilutions/concentrations should be determined by the end user.
分子量	50kDa
性状	Lyophilized or Liquid
浓度	1mg/ml
免疫原	KLH conjugated Synthesised phosphopeptide derived from human RUNX1 around the phosphorylation site of Ser266
亚型	IgG
纯化方法	affinity purified by Protein A
储存液	0.01M TBS(pH7.4) with 1% BSA, 0.03% Proclin300 and 50% Glycerol.
保存条件	Store at -20 °C for one year. Avoid repeated freeze/thaw cycles. The lyophilized antibody is stable at room temperature for at least one month and for greater than a year when kept at -20°C. When reconstituted in sterile pH 7.4 0.01M PBS or diluent of antibody the antibody is stable for at least two weeks at 2-4 °C.
产品介绍	background: AML1/Runx1 binds DNA as a monomer and through the Runt domain. DNA binding is increased by heterodimerization with CBFB. Isoform AML1L can neither bind DNA nor heterodimerize and interferes with the transactivation activity of AML1/Runx1. CBF binds to the core site, 5'-PYGPYGGT-3', of a number of enhancers and promoters, including murine leukemia virus, polyomavirus enhancer, T cell receptor enhancers, LCK, IL3 and GMCSF promoters. The alpha subunit binds DNA and appears to have a role in the development of normal hematopoiesis. AML1/Runx1 is expressed in a wide variety of tissues and is expressed at the highest levels in thymus, bone marrow and peripheral blood. Defects in AML1/Runx1 are the cause of familial platelet disorder with associated myeloid malignancy, an autosomal dominant disease characterized by qualitative and quantitative platelet defects, and propensity to develop acute myelogenous leukemia. Function: CBF binds to the core site, 5'-PYGPYGGT-3', of a number of enhancers and promoters, including murine leukemia virus, polyomavirus enhancer, T-cell receptor enhancers, LCK, IL-3 and GM-CSF promoters. The alpha subunit binds DNA and appears to have a role in the development of normal hematopoiesis. Isoform AML-1L interferes with the transactivation activity of RUNX1. Acts synergistically with ELF4 to transactivate the IL-3 promoter and with ELF2 to transactivate the mouse BLK promoter. Inhibits KAT6B-dependent transcriptional activation. Subunit: 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. Subcellular Location: Nucleus. Tissue Specificity: Expressed in all tissues examined except brain and heart. Highest levels in thymus, bone marrow and peripheral blood. Post-translational modifications: 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. DISEASE: Note=A chromosomal aberration involving RUNX1/AML1 is a cause of chronic myelogenous leukemia (CML). Translocation t(3;21)(q26;q22) with EAP or MECOM. Note=A chromosomal aberration involving RUNX1/AML1 is found in childhood acute lymphoblastic leukemia (ALL). Translocation t(12;21)(p13;q22) with TEL. The translocation fuses the 3'-end of TEL to the alternate 5'-exon of AML-1H. Note=A chromosomal aberration involving RUNX1 is found in acute leukemia. Translocation t(11,21)(q13;q22) that forms a MACROD1-RUNX1 fusion protein. Defects in RUNX1 are the cause of familial platelet disorder with associated myeloid malignancy (FPDMM) [MIM:601399]. FPDMM is an autosomal dominant disease characterized by qualitative and quantitative platelet defects, and propensity to develop acute myelogenous leukemia. Note=A chromosomal aberration involving RUNX1/AML1 is found in therapy-related myeloid malignancies. Translocation t(16;21)(q24;q22) that forms a RUNX1-CBFA2T3 fusion protein. Note=A chromosomal aberration involving RUNX1/AML1 is a cause of chronic myelomonocytic leukemia. Inversion inv(21)(q21;q22) with USP16. Similarity: Contains 1 Runt domain. Database links: Entrez Gene: 861 Human Omim: 151385 Human SwissProt: Q01196 Human Unigene: 149261 Human Unigene: 612648 Human Important Note: This product as supplied is intended for research use only, not for use in human, therapeutic or diagnostic applications.

AML1/Runx1结合DNA作为单体，并通过RUNT结构域。通过与CBFB异源二聚反应增加DNA结合。异构体AML1L既不结合DNA也不异源二聚，并干扰AML1/Runx1的反式激活活性。CBF结合核心位点，5’-PygPGGT-3’，含有多种增强子和启动子，包括小鼠白血病病毒、多瘤病毒增强子、T细胞受体增强剂、LCK、IL3和GMCSF启动子。α亚基结合DNA，似乎在正常造血的发育中起作用。AML1/Runx1在多种组织中表达，在胸腺、骨髓和外周血中最高表达。AML1/Runx1的缺陷是家族性血小板紊乱伴相关髓系恶性肿瘤的原因，常染色体显性疾病以定性和定量血小板缺陷为特征，并有发展急性髓性白血病的倾向。