MCE 國際站:Oxaliplatin
中文名:奧沙利鉑
CAS:61825-94-3
品牌:MedChemExpress (MCE)
存儲條件:4°C, protect from light
生物活性:Oxaliplatin 是一種DNA 合成 抑制劑,。 Oxaliplatin 引起 DNA 交聯(lián)損傷,阻止 DNA 復制和轉(zhuǎn)錄并誘導細胞凋亡,。奧沙利鉑可用于癌癥研究[1][2][3],。 IC50 和目標:IC50:DNA 合成[1]
體外:Oxaliplatin(24-72 小時;2-128 μM,;HCC,、HCCLM3 和 Hep3B 細胞)抑制細胞生長并誘導細胞凋亡[1]。
Oxaliplatin(10 μM,;15-240 分鐘,; CEM 細胞 ) 誘導原發(fā)性和繼發(fā)性 DNA 損傷,包括 DNA 交聯(lián) (ISC) 和 DNA-蛋白質(zhì)交聯(lián) (DPC)[2],。
奧沙利鉑(0.01 至 100 μM,; 24 小時)有效抑制膀胱癌細胞系 RT4 和 TCCSUP、卵巢癌細胞系 A2780,、結(jié)腸癌細胞系 HT-29,、膠質(zhì)母細胞瘤細胞系 U-373MG 和 U-87MG,以及黑色素瘤細胞系 SK-MEL-2 和 HT- 144 的 IC50 分別為 11 μM,、15 μM,、0.17 μM、0.97 μM,、2.95 μM,、17.6 μM、30.9 μM 和 7.85 μM[3],。
體內(nèi):奧沙利鉑(5-10 mg/kg,;腹腔注射;32 天,;裸鼠)抑制腫瘤生長[1],。
銷售產(chǎn)品:GNE-987 | L-DOPA | Adenine | Niraparib (tosylate) | Rosuvastatin (Calcium) | Caerulomycin A | Fagomine | Palmitic acid-13C16 | Canakinumab | BODIPY 576/589
研究領(lǐng)域:Cell Cycle/DNA Damage | Apoptosis
作用靶點:DNA/RNA Synthesis | Apoptosis
Trending products:Recombinant Proteins | Bioactive Screening Libraries | Natural Products | Fluorescent Dye | PROTAC | Isotope-Labeled Compounds | Oligonucleotides
參考文獻:
[1]. Raymond E, et al. Oxaliplatin: a review of preclinical and clinical studies. Ann Oncol. 1998 Oct;9(10):1053-71.
[2]. Mohammed MQ, et al. Oxaliplatin is active in vitro against human melanoma cell lines: comparison with NSC 119875 and NSC 241240. Anticancer Drugs. 2000 Nov;11(10):859-63.
[3]. Pendyala L, et al. In vitro cytotoxicity, protein binding, red blood cell partitioning, and biotransformation of oxaliplatin. Cancer Res. 1993 Dec 15;53(24):5970-6.
[4]. Wang Z, et al. Oxaliplatin induces apoptosis in hepatocellular carcinoma cells and inhibits tumor growth. Expert Opin Investig Drugs. 2009 Nov;18(11):1595-604
[5]. Mathé G, et al. Oxalato-platinum or 1-OHP, a third-generation platinum complex: an experimental and clinical appraisal and preliminary comparison with cis-platinum. Biomed Pharmacother. 1989;43(4):237-50.
[6]. Schellingerhout D, et al. Impairment of retrograde neuronal transport in oxaliplatin-induced neuropathy demonstrated by molecular imaging. PLoS One. 2012;7(9):e45776. doi: 10.1371/journal.pone.0045776. Epub 2012 Sep 20.
[7]. Park GY, et al. Phenanthriplatin, a monofunctional DNA-binding platinum anticancer drug candidate with unusual potency and cellular activity profile. Proc Natl Acad Sci U S A. 2012 Jul 24;109(30):11987-92.
[8]. Yi Yao, et al. Comparative proteomic analysis of colon cancer cells in response to oxaliplatin treatment. Biochim Biophys Acta. 2009 Oct;1794(10):1433-40.
[9]. Garrett MJ, et, al. Capecitabine, Oxaliplatin, and Bevacizumab (BCapOx) Regimen for Metastatic Colorectal Cancer. Hosp Pharm. 2017 May;52(5):341-347.
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