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Selisistat

CAS号

49843-98-3

分子式

C13H13ClN2O

主要靶点

Sirtuin

仅限科研使用

Cat No : CM00041

Print datasheet

Synonyms

deacetylation|Drosophila|disease|inhibit|Huntington's|EX527|EX-527|EX 527|Inhibitor|mammalian|pathology|SIRT1|Sirtuin|Selisistat|SEN0014196|SEN-0014196|SEN 0014196|司来司他

验证数据展示

  • CAS No.: 49843-98-3

    Selisistat
    CAS#: 49843-98-3

产品信息

CAS号 49843-98-3
分子式 C13H13ClN2O
主要靶点 Sirtuin
主要通路 表观遗传|DNA 损伤和修复
分子量 248.71
纯度 99.79%, 此纯度可做参考,具体纯度与批次有关系,可咨询客服
储存条件 Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice.
别名 deacetylation|Drosophila|disease|inhibit|Huntington's|EX527|EX-527|EX 527|Inhibitor|mammalian|pathology|SIRT1|Sirtuin|Selisistat|SEN0014196|SEN-0014196|SEN 0014196|司来司他

靶点活性

SIRT1:38 nM(cell free)

体内活性

方法:为研究对肺损伤的作用,将 Selisistat (10 mg/kg) 腹腔注射给 Balb/C 小鼠,0.5 h 后注射 LPS 诱导肝损伤。 结果:Selisistat 对 SIRT1 的选择性抑制可能部分通过抑制 mTOR 来减轻内毒素血症相关的急性肺损伤。[3] 方法:为研究对亨廷顿舞蹈症 (HD) 的作用,将 Selisistat (5-20 mg/kg,0.5% HPMC) 灌胃给药给 R6/2 小鼠,每天一次,直至死亡。 结果:Selisistat 治疗导致接受 20 mg/kg 剂量的小鼠的存活率显著增加,中位寿命显著增加了 3 周,在检查自主运动活动时也观察到显著的改善。[4]

体外活性

方法:人结直肠癌细胞 HCT116 用 0.1% 血清和 Selisistat (1-2 μM) 培养 7 天,检测细胞数量。 结果:当 HCT116 细胞在 0.1% 血清中培养时,添加 Selisistat 导致 7 天后细胞数量增加 90%。在生长因子缺乏条件下,SirT1 是细胞增殖的重要调节因子。[1] 方法:人肺癌细胞 NCI-H460 用 etoposide (20 μM) 和 Selisistat (1 μM) 处理 6 h,使用 Western Blot 检测靶点蛋白表达水平。 结果:在用 DNA 损伤剂 etoposide 处理的细胞中,Selisistat 产生乙酰化 p53 的增加。[2]

溶解度

DMSO:60 mg/mL (241.24 mM); Ethanol:12.4 mg/mL (49.86 mM);

细胞实验

NCI-H460 cells, MCF-7 cells, U-2 OS cells, or HMEC were plated at 2,000 cells per well in opaque-walled 96-well plates for the viability assay and 800 cells per well in 96-well Cytostar-T scintillating microplates for the proliferation assay. Cells were incubated for 1 day (NCI-H460) or 2 days (MCF-7, U-2 OS, and HMEC) prior to exposure to DNA-damaging agents and deacetylase inhibitors. All experiments were performed in triplicate. For viability assays, cells were treated with the indicated compounds for 48 h. Cell viability was then determined using the Cell Titer-Glo luminescent assay, which measures total ATP levels as an index of cell number. Luminescence was measured on a Luminoskan Ascent. For the proliferation assay, 0.5 μCi/ml of [14C]thymidine was added to the medium immediately after the genotoxins and deacetylase inhibitors. Plates were counted at 48 h (HMEC) or 72 h (NCI-H460, MCF-7, and U-2 OS cells) in a Microbeta liquid scintillation counter. Thymidine incorporated by the cells was detected by proximity to the scintillant in the base of the Cytostar-T tissue culture plate [1].

动物实验

Mice were injected with RSV (RSV) 30mg/kg (4ml/kg) or equivalent volume of DMSO (Vehicle) (4ml/kg) intraperitoneally 18 hours pre-sepsis. This dose of RSV in mice was as per documented literature. In one group of mice, RSV pre-treated mice received EX-527 (10 mg/kg intraperitoneally; 4ml/kg, Vehicle: DMSO) within 10 minutes of cecal ligation and puncture [5].

参考文献

1.Kabra N, et al. SirT1 is an inhibitor of proliferation and tumor formation in colon cancer. J Biol Chem. 2009 Jul 3;284(27):18210-7.
2.Solomon JM, et al. Inhibition of SIRT1 catalytic activity increases p53 acetylation but does not alter cell survival following DNA damage. Mol Cell Biol. 2006 Jan;26(1):28-38.
3.Huang J, et al. The SIRT1 inhibitor EX-527 suppresses mTOR activation and alleviates acute lung injury in mice with endotoxiemia. Innate Immun. 2017 Nov;23(8):678-686.
4.mith MR, et al. A potent and selective Sirtuin 1 inhibitor alleviates pathology in multiple animal and cell models of Huntington's disease. Hum Mol Genet. 2014 Jun 1;23(11):2995-3007.
5.Wang X, et al. Resveratrol attenuates microvascular inflammation in sepsis via SIRT-1-Induced modulation of adhesion molecules in ob/ob mice. Obesity (Silver Spring). 2015 Jun;23(6):1209-17.
6.Luo Y, Lu S, Gao Y, et al. Araloside C attenuates atherosclerosis by modulating macrophage polarization via Sirt1-mediated autophagy[J]. Aging (Albany NY). 2020, 12(2): 1704.
7.Chen W, Lin B, Xie S, et al. Naringenin protects RPE cells from NaIO3-induced oxidative damage in vivo and in vitro through up-regulation of SIRT1[J]. Phytomedicine. 2020: 153375.

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