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18378-89-7

中文名稱 光輝霉素
英文名稱 MITHRAMYCIN A
CAS 18378-89-7
分子式 C52H76O24
分子量 1085.15
MOL 文件 18378-89-7.mol
更新日期 2024/12/17 09:24:28
18378-89-7 結(jié)構(gòu)式 18378-89-7 結(jié)構(gòu)式

基本信息

中文別名
金霉酸
光神霉素
光輝酶素
普卡霉素
光輝霉素
普卡酶素
光神霉素A
光輝霉素A
普芳拉星,金霉酸
光神霉素,光輝霉素A
英文別名
2371
pa144
a-2371
nsc24559
MITHRACIN
PLICAMYCIN
mitramycin
MITHRAMYCIN
aurelicacid
aurlelicacid
所屬類別
原料藥:抗生素類抗腫瘤藥

物理化學(xué)性質(zhì)

熔點(diǎn)180-183 °C
熔點(diǎn)180-183 °C
比旋光度D20 -51° (c = 0.4 in ethanol)
沸點(diǎn)761.72°C (rough estimate)
密度1.1576 (rough estimate)
折射率1.6500 (estimate)
儲存條件2-8°C
儲存條件2-8°C
溶解度可溶于DMSO(高達(dá)20mg/ml)或乙醇(高達(dá)10mg/ml)
酸度系數(shù)(pKa)4.54±0.60(Predicted)
形態(tài)粉末
顏色紅色至棕色
Merck13,7619
BRN5236667
穩(wěn)定性自購買之日起 1 年內(nèi)保持穩(wěn)定。 DMSO 或乙醇溶液可在 -20°C 下保存長達(dá) 1 個(gè)月。
EPA化學(xué)物質(zhì)信息Plicamycin (18378-89-7)

安全數(shù)據(jù)

危險(xiǎn)性符號(GHS)GHS hazard pictograms
GHS07
警示詞警告
危險(xiǎn)性描述H302
防范說明P301+P312+P330
危險(xiǎn)品標(biāo)志Xn,T+
危險(xiǎn)類別碼22-26/27/28
危險(xiǎn)品運(yùn)輸編號3249
WGK Germany3
WGK Germany3
RTECS號PZ2800000
危險(xiǎn)等級6.1(b)
包裝類別III
海關(guān)編碼29419090
毒害物質(zhì)數(shù)據(jù)18378-89-7(Hazardous Substances Data)
毒性LD50 in mice, rats (mg/kg): 2.14, 1.74 i.v. (Slavik, Carter)

應(yīng)用領(lǐng)域

用途1
抗癌抗生素,對多種動物腫瘤有較強(qiáng)的抑制作用,其作用機(jī)理是與DNA結(jié)合,抑制轉(zhuǎn)錄和蛋白合成,抑制RNA的合成,作用于細(xì)胞增殖各期。在MDR表現(xiàn)形中是Pgp的底物。 在流式細(xì)胞計(jì)中用于熒光染色DNA。適合于檢測DNA。

常見問題列表

生物活性
Plicamycin 是一種選擇性特 Sp1 轉(zhuǎn)錄因子抑制劑。Plicamycin 通過降低 Sp1 蛋白表達(dá)來抑制癌細(xì)胞生長。
靶點(diǎn)

Sp1 transcription factor

體外研究

Sp1 is a zinc-finger transcription factor that regulates multiple cellular functions and promotes tumor progression by controlling expression of genes involved in cell cycle, apoptosis and DNA damage. Sp1 binds to GC-rich motifs of promoters and interacts with components of the general transcriptional machinery and co-activator complexes of multiple signaling pathways. Plicamycin (Mith) decreases Sp1 protein by inducing proteasome-dependent degradation, thereby suppressing cervical cancer growth through a DR5/caspase-8/Bid signaling pathway. To assess the antiproliferative effects of Plicamycin on cervical cancer cells, two cervical cancer cell lines with different genetic backgrounds are grown with or without treatment with Plicamycin at different concentrations. Plicamycin inhibits HEp-2 and KB cell growth in a concentration-dependent manner after 48 h. Apoptotic cell death is qualitatively estimated by DAPI staining for nuclear condensation and fragmentation. Plicamycin leads to significant DNA fragmentation compared to untreated controls.

體內(nèi)研究

The antitumorigenic activity of Plicamycin (0.2 mg/kg/day) is determined in a xenograft model and observed reduction in tumor volume and weight. No significant mouse body weight loss is observed in Plicamycin-treatment groups, indicating that Plicamycin-associated toxicity is minimal. Plicamycin also increases TUNEL-positive cells in tumor xenografts. No notable intergroup differences are observed among organs, indicating no marked signs of systemic toxicity at the Plicamycin dose used in this study.

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