MJ33 lithium salt
| 规格 | 价格 | 货期 | 数量 |
|---|---|---|---|
| 5mg | ¥2762.00 | 10-15工作日发货 | |
| 10mg | ¥4225.00 | 10-15工作日发货 | |
| 25mg | ¥9208.00 | 10-15工作日发货 |
特色产品
- 用于免疫印迹和质谱分析等后续操作
- 适用于30 KDa-130 KDa大小的蛋白
- 可将信号灵敏度提高100倍
- 同时保持稳定的特异性和分辨率
- 提供更高的转录效率并抑制免疫激活
- 使用5-moUTP和Cy5-utp修饰
产品描述
MJ33 is an inhibitor of the acidic, calcium-independent (ai)PLA2 activity of Prdx6.
Peroxiredoxin-6 (Prdx6), a bifunctional enzyme, has both non-selenium glutathione peroxidase and phospholipase A2 (PLA2) activities. The PLA2 activity of Prdx6 is calcium-independent, functions optimally in acidic conditions, and facilitates the intracellular processing of surfactant lipids, such as dipalmitoylphosphatidylcholine.
In vitro: MJ33 was found to be specifically inhibit the aiPLA2 activity of the protein. Moreover, the Ca2+-independent PLA2 activity of phosphorylated rat Prdx6 could be abolished by the treatment of either MJ33 or surfactant protein A (SP-A), known inhibitors of aiPLA2 activity. Further supporting the results with intact cells, recombinant Prdx6 was phosphorylated in vitro by ERK and p38, but not by JNK. Phosphorylation in vitro led to a great increase in PLA2 activity that was Ca2+-independent and ould be inhibited by both MJ33 and by SP-A, which was similar to native lung enzyme [1].
In vivo: A previous study evaluated the effect of MJ33 on manifestations of acute lung injury. Results showed that MJ33 could inhibit reactive oxygen species generation by lungs when measured LPS treatment. LPS at either a low or high dose significantly increased lung infiltration with inflammatory cells, secretion of proinflammatory cytokines, expression of lung vascular cell adhesion molecule, lung permeability, tissue lipid peroxidation, tissue protein oxidation, and activation of NF-κB. MJ33, given either concurrently or 2 h subsequent to LPS, was able to significantly reduce all of these measured parameters [2].
Clinical trial: So far, no clinical study has been conducted.
References:
[1] Wu, Y. ,Feinstein, S.I.,Manevich, Y., et al. Mitogen-activated protein kinase-mediated phosphorylation of peroxiredoxin 6 regulates its phospholipase A2 activity. Biochem. 419(3), 669-679 (2009).
[2] Lee I, Dodia C, Chatterjee S, Feinstein SI, Fisher AB. Protection against LPS-induced acute lung injury by a mechanism-based inhibitor of NADPH oxidase (type 2). Am J Physiol Lung Cell Mol Physiol. 2014 Apr 1;306(7):L635-44.
产品性质
| 物理外观 | A crystalline solid |
| CAS号 | 1007476-63-2 |
| 分子式 | C22H43F3O6P·Li |
| 分子量 | 498.5 |
| 化学名称 | mono[1-[(hexadecyloxy)methyl]-2-(2,2,2-trifluoroethoxy)ethyl] monomethyl ester phosphoric acid, monolithium salt |
| 溶解度 | ≤2mg/ml in ethanol;0.25mg/ml in DMSO;0.5mg/ml in dimethyl formamide |
| SMILES | O=P(OC)([O-])OC(COCC(F)(F)F)COCCCCCCCCCCCCCCCC.[Li+] |
| 存储条件 | -20°C |
| 运输条件 | 蓝冰 |
生物相关数据
质量控制
操作说明
APExBIO 顾客使用本产品发表的 3 篇科研文献
- 1. Huiqing Wang, Yao Zhou, et al. "Ferrostatin-1 attenuates brain injury in animal model of subarachnoid hemorrhage via phospholipase A2 activity of PRDX6." Neuroreport. 2023 Aug 2;34(12):606-616. PMID: 37395228
- 2. Wen-ying Yang, Xiang Meng, et al. "PRDX6 Alleviates Lipopolysaccharide-induced Inflammation in Human Gingival Fibroblasts by Regulation of NRF2." Research Square. rs-1108989/v1.
- 3. Lu B, Chen XB, et al. "Identification of PRDX6 as a regulator of ferroptosis." Acta Pharmacol Sin. 2019 Apr 29. PMID:31036877



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