HEK293T/Human SARM1 Stable Cell Line
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货号:CSB-SC750971HU
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规格:1 vial contains approximately 5x106 cells in 1 ml
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价格:¥30000
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活性:
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Untransfected HEK293T cells (green line) and transfected Human SARM1 HEK293T Stable cells (red line) were stained with anti-Flag antibody (2µg/1*106cells), washed and then followed by FITC-conjugated anti-Mouse IgG Fc antibody and analyzed with flow cytometry.
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Western Blot
Positive WB detected in: Lane1:20 µg HEK293T cells, Lane2:40 µg Human SARM1 HEK293T Stable cells, Lane3:20 µg Human SARM1 HEK293T Stable cells
All lanes: Anti-Flag antibody at 1:1000
Secondary
Goat polyclonal to mouse IgG at 1/50000 dilution
Predicted band size: 77.5 KDa
Observed band size: 77 KDa
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其他:
产品详情
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Uniprot No.:Q6SZW1
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生长类型:Adherent
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抗性:Puromycin
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培养基:DMEM + 10% FBS + 2μg/mL Puromycin
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别名:SARM1
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蛋白标签:C-terminal Flag-tagged
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保存缓冲液:35% FBS + 55% DMEM + 10% DMSO
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应用范围:Binding assay by FACS and Western blot
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储存条件:Frozen in liquid nitrogen or stored at -80°C
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货期:Basically, we can dispatch the products out in 1-3 working days after receiving your orders. Delivery time maybe differs from different purchasing way or location, please kindly consult your local distributors for specific delivery time.
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靶点详情
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功能:NAD(+) hydrolase, which plays a key role in axonal degeneration following injury by regulating NAD(+) metabolism. Acts as a negative regulator of MYD88- and TRIF-dependent toll-like receptor signaling pathway by promoting Wallerian degeneration, an injury-induced form of programmed subcellular death which involves degeneration of an axon distal to the injury site. Wallerian degeneration is triggered by NAD(+) depletion: in response to injury, SARM1 is activated and catalyzes cleavage of NAD(+) into ADP-D-ribose (ADPR), cyclic ADPR (cADPR) and nicotinamide; NAD(+) cleavage promoting cytoskeletal degradation and axon destruction. Also able to hydrolyze NADP(+), but not other NAD(+)-related molecules. Can activate neuronal cell death in response to stress. Regulates dendritic arborization through the MAPK4-JNK pathway. Involved in innate immune response: inhibits both TICAM1/TRIF- and MYD88-dependent activation of JUN/AP-1, TRIF-dependent activation of NF-kappa-B and IRF3, and the phosphorylation of MAPK14/p38.
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基因功能参考文献:
- we identify a physical interaction between the autoinhibitory N terminus and the TIR domain of SARM1, revealing a previously unrecognized direct connection between these domains that we propose mediates autoinhibition and activation upon injury. PMID: 27671644
- Active nerve degeneration requires SARM1 and MAP kinases, including DLK, while the NAD+ synthetic enzyme NMNAT2 prevents degeneration. PMID: 26844829
- Data show that sterile alpha- and armadillo-motif-containing protein (SARM) modulates MyD88 protein-mediated Toll-like receptors (TLRs) activation through BB-loop dependent interleukin-1 receptor (TIR) TIR-TIR interactions. PMID: 26592460
- These results indicate that association of PINK1 with SARM1 and TRAF6 is an important step for mitophagy. PMID: 23885119
- The innate immunity adaptor SARM translocates to the nucleus to stabilize lamins and prevent DNA fragmentation in response to pro-apoptotic signaling. PMID: 23923041
- Rapid Wallerian degeneration requires the pro-degenerative molecules SARM1. PMID: 24840802
- Data found that the UXT isoforms elicit dual opposing regulatory effects on SARM-induced apoptosis. PMID: 24021647
- SARM overexpression caused mitochondrial clustering which has also been observed in several cell death phenomenon. PMID: 23175186
- The N-terminal 27 amino acids (S27) of SARM, which is hydrophobic and polybasic, acts as a mitochondria-targeting signal sequence, associating SARM to the mitochondria. The S27 peptide has an inherent ability to bind to lipids and mitochondria. PMID: 22145856
- SARM-mediated inhibition may not be exclusively directed at TRIF or MyD88, but that SARM may also directly inhibit MAPK phosphorylation PMID: 20306472
- Candidate gene in the onset of hereditary infectious/inflammatory diseases. PMID: 15893701
- TIR adaptor SARM is a negative regulator of Toll-like receptor signaling. PMID: 16964262
- confirmed the co-localization of retinoschisin with Na/K ATPase and SARM1 in photoreceptors and bipolar cells of retina tissue PMID: 17804407
- SARM1 deficiencies may uncover unexpected similarities between the ways in which neurons and immune cells sense and respond to danger. PMID: 18089857
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亚细胞定位:Cytoplasm. Cell projection, axon. Cell projection, dendrite. Cell junction, synapse. Mitochondrion.
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组织特异性:Predominantly expressed in brain, kidney and liver. Expressed at lower level in placenta.
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数据库链接:
HGNC: 17074
OMIM: 607732
KEGG: hsa:23098
STRING: 9606.ENSP00000406738
UniGene: Hs.743510
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