产品介绍:
基本信息
分子式 | C43H68ClNO11 |
分子量 | 810.47 |
存储条件 | Freezer -20℃ |
产品描述 Pimecrolimus是一种抑免蛋白配体, 可以特异地与胞质受体macrophilin-12结合;是钙调蛋白抑制剂。
靶点(IC50 & Targe) Others,
体外研究 Pimecrolimus通过抑制磷酸酶功能阻断T淋巴细胞激活途径。[1] Pimecrolimus阻止细胞因子和促炎性介质从肥大细胞中释放。Pimecrolimus与macrophilin-12结合,形成pimecrolimus-macrophilin复合物,然后与胞质酶钙调磷酸酶结合。Pimecrolimus-macrophilin复合物通过抑制钙调磷酸酶的作用,阻止活化的T细胞中核因子的细胞质成分去磷酸化。Pimecrolimus不仅抑制肥大细胞中细胞因子的转录和合成,也会通过抑制Fc∈-RI介导的脱粒和分泌而抑制预成形的介质5-羟色胺和β-氨基己糖苷酶的释放。Pimecrolimus治疗引起与macrolactam靶点通路和炎症相关基因的mRNA表达的强烈下调。[2]
体内研究 在小鼠体内,Pimecrolimus口服后与环孢霉素A一样有效,皮下注射后比环孢霉素A略有效。在过敏性接触皮炎小鼠体内,与环孢霉素A和他克莫司相比,Pimecrolimus不间断地抑制次级炎症反应,但是不损害初次免疫反应。[2] 在过敏性接触皮炎(ACD)猪模型中,Pimecrolimus与强效皮质类固醇氯倍他索-17-丙酸盐同样有效。在低镁无毛大鼠,一个模拟急性过敏性皮炎信号的模型中,Pimecrolimus也能有效降低皮肤炎症和瘙痒。在 (1)局部移植物抗宿主反应,(2)用绵羊红细胞形成抗体,和(3)肾移植的大鼠体内,与他克莫司相比,Pimecrolimus仅显示出低电势以减弱全身免疫应答反应。[3]
激酶实验 细胞实验 Cell lines: melanocytes Concentrations: 1, 10, 100, 1,000 nM Incubation Time: 3 days Method: The proliferation rate of melanocytes was determined using a colorimetric MTT assay. Melanocytes were plated in 96-well microplates, and each well was pretreated with 100 µl of different concentrations (1, 10, 100, 1,000 nM) of pimecrolimus for 3 days. Then, 50 µL of 5 mg/mL 3-(4, 5-dimethylthiazol-2-yl)-2, 5-diphenyltetrazolium bromide (MTT) solution was added to each well. The resulting formazan was dissolved with 150 µL dimethylsulfoxide. The absorbance of the samples was measured at a wavelength of 490 nm. (Only for Reference)
动物实验 参考文献 [1] Nghiem P, et al. Am Acad Dermatol, 2002, 46(2), 228-241. [2] Gupta AK, et al. J Eur Acad Dermatol Venereol, 2003, 17(5), 493-503. [3] Stuetz A, et al. Semin Cutan Med Surg, 2001, 20(4), 233-241. [4] Xu P, et al. Korean J Physiol Pharmacol. 2017, 21(3):287-292.
安全信息
图形或危害标志 | |
提示语 | Warning |
危险说明 | H302 H410 |
防范说明 | P264 P270 P273 P301+P312 P330 P391 P501 |
UN号码 | 3077 |
危险分类 | 9 |
包装等级 | III |