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他拉唑帕利,Talazoparib

他拉唑帕利|T6253

價(jià)格 253 357 588
包裝 1mg 2mg 5mg
最小起訂量 1mg
發(fā)貨地 上海
更新日期 2024-12-02
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產(chǎn)品詳情

中文名稱:他拉唑帕利英文名稱:Talazoparib
CAS:1207456-01-6品牌: TargetMol
產(chǎn)地: 美國保存條件: Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice.
純度規(guī)格: 99.85%產(chǎn)品類別: 抑制劑
貨號(hào): T6253
2024-12-02 他拉唑帕利 Talazoparib 1mg/253RMB;2mg/357RMB;5mg/588RMB 253 TargetMol 美國 Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice. 99.85% 抑制劑

Product Introduction

Bioactivity

名稱Talazoparib
描述Talazoparib (LT-673) is a PARP inhibitor that inhibits PARP 1 and PARP 2 (Ki=1.2/0.87 nM) and is orally active. Talazoparib has anti-tumorigenic activity and induces tumor cell death by blocking PARP enzyme activity and by trapping PARP at DNA damage sites.
細(xì)胞實(shí)驗(yàn)Colony formation assays were conducted as described previously. In brief, cells were seeded into 6-well plates at a concentration of 500 to 2,000 cells per well. After 24 hours, media was replaced with fresh media containing PARP1/2 inhibitor. This procedure was repeated twice weekly for 14 days, at which point colonies were fixed with TCA and stained with sulforhodamine B. Colonies were counted and surviving fractions calculated by normalizing colony counts to colony numbers in vehicle-treated wells. Survival curves were plotted using a four-parameter logistic regression curve fit [2].
激酶實(shí)驗(yàn)The ability of a test compound to inhibit PARP1 enzyme activity was assessed using the PARP Assay Kit following the manufacturer's instruction. IC50 values were calculated using GraphPad Prism5 software. For PARP inhibitor Ki determination, enzyme assays were conducted in 96-well FlashPlate with 0.5 U PARP1 enzyme, 0.25× activated DNA, 0.2 μCi [3H] NAD, and 5 μmol/L cold NAD in a final volume of 50 μL reaction buffer containing 10% glycerol (v/v), 25 mmol/L HEPES, 12.5 mmol/L MgCl2, 50 mmol/L KCl, 1 mmol/L dithiothreitol (DTT), and 0.01% NP-40 (v/v), pH 7.6. Reactions were initiated by adding NAD to the PARP reaction mixture with or without inhibitors and incubated for 1 minute at room temperature. Fifty microliter of ice-cold 20% trichloroacetic acid (TCA) was then added to each well to stop the reaction. The plate was sealed and shaken for a further 120 minutes at room temperature, followed by centrifugation. Radioactive signal bound to the FlashPlate was determined using TopCount. PARP1 Km was determined using Michaelis–Menten equation from various substrate concentrations (1–100 μmol/L NAD). Compound Ki was calculated from enzyme inhibition curve according to the formula: Ki = IC50/[1+(substrate)/Km]. Km for PARP2 enzyme and compound Ki were determined with the same assay protocol except 30 ng PARP2, 0.25× activated DNA, 0.2 μCi [3H] NAD, and 20 μmol/L cold NAD were used in the reaction for 30 minutes at room temperature [2].
動(dòng)物實(shí)驗(yàn)Female athymic nu/nu mice (8–10-week old) were used for all in vivo xenograft studies. Mice were quarantined for at least 1 week before experimental manipulation. Exponentially growing cells (LNcap and MDA-MB-468) or in vivo passaged tumor fragments (MX-1) were implanted subcutaneously at the right flank of nude mice. When tumors reached an average volume of approximately 150 mm^3, mice were randomized into various treatment groups (6–8 mice/group) in each study. Mice were visually observed daily and tumors were measured twice weekly by calliper to determine tumor volume using the formula [length/2] × [width^2]. Group median tumor volume (mm^3) was graphed over time to monitor tumor growth. In single-agent studies, olaparib (100 mg/kg), BMN 673 (various doses as indicated), or vehicle (10% DMAc, 6% Solutol, and 84% PBS) was administered by oral gavage (per os), once daily or BMN 673 (0.165 mg/kg) twice daily for 28 consecutive days. Mice were continuously monitored for 10 more days after last day of dosing. In cisplatin combination study, BMN 673, olaparib, or vehicle was administered per os once daily for 8 days starting on day 1. Cisplatin at a dosage of 6 mg/kg or its vehicle (saline) was administered intraperitoneally as a single injection on day 3, 30 minutes after PARP inhibitor was administered. Combination with carboplatin was conducted in a similar way in MX-1 model in which BMN 673 was administered per os once daily for either 8 days or 5 days and carboplatin was injected intraperitoneally at single dose of 35 mg/kg, 30 minutes after BMN 673 on day 3 [2].
體外活性方法:12 種 OCCC 細(xì)胞系用 Talazoparib (0-100 nM) 處理 14 天,使用 colony formation assays 檢測(cè)化合物敏感性。 結(jié)果:除 KOC-7c 外,所有 HR 缺陷細(xì)胞系對(duì) Talazoparib 均顯示出具有敏感性的劑量反應(yīng)曲線。而所有 HR 活性細(xì)胞系 (OVTOKO除外) 均顯示具有耐藥性的劑量響應(yīng)曲線。[1] 方法:人結(jié)腸癌細(xì)胞 LoVo 用 Talazoparib (10-40 nM) 和 temozolomide (0-400 μM) 處理 5 天,使用 CellTiterGlo assay 檢測(cè)細(xì)胞活力。 結(jié)果:?jiǎn)蝿?Talazoparib 暴露導(dǎo)致約 15% 的細(xì)胞生長(zhǎng)抑制。將 temozolomide 與 Talazoparib 組合可顯著增強(qiáng) temozolomide 的細(xì)胞毒性。[2]
體內(nèi)活性方法:為測(cè)試體內(nèi)抗腫瘤活性,將 Talazoparib (0.166-0.33 mg/kg) 口服給藥給攜帶人乳腺癌腫瘤 MX-1 的 athymic nu/nu 小鼠,每天一次或每天兩次,持續(xù)四周。 結(jié)果:Talazoparib 在小鼠異種移植物模型中以 0.165 mg/kg 劑量每天兩次給藥比 0.33 mg/kg 劑量每天一次給藥更有效。在 MX-1 模型中,不僅用 0.165 mg/kg/dose 2X/天方案治療的所有 6 只小鼠都達(dá)到了完全反應(yīng),而且直到研究結(jié)束,即給藥停止 8 周后,沒有一只小鼠出現(xiàn)腫瘤再生長(zhǎng)。[2]
存儲(chǔ)條件Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice.
溶解度DMSO : 36 mg/mL (94.6 mM)
H2O : < 1 mg/mL (insoluble or slightly soluble)
Ethanol : < 1 mg/mL (insoluble or slightly soluble)
10% DMSO+90% Saline : 0.1 mg/mL (0.26 mM), Please add co-solvents sequentially, clarifying the solution as much as possible before adding the next one. Dissolve by heating and/or sonication if necessary. Working solution is recommended to be prepared and used immediately.
關(guān)鍵字inhibit | Talazoparib | BRCA1/2 | MX-1 | PARP-mediated | poly ADP ribose polymerase | LT 673 | BMN673 | breast cancer | Inhibitor | PARylation | LT673 | anticancer | BMN 673 | PARP
相關(guān)產(chǎn)品VPC-70063 | Rucaparib | Niraparib | XAV-939 | Olaparib | 3-Aminobenzamide | Benzamide | OUL35 | 3-Methoxybenzamide | Picolinamide | 4'-Methoxychalcone | EB-47
相關(guān)庫抑制劑庫 | 抗癌上市藥物庫 | 經(jīng)典已知活性庫 | 抗癌活性化合物庫 | 已知活性化合物庫 | EMA 上市藥物庫 | 抗衰老化合物庫 | FDA 上市藥物庫 | 抗癌臨床化合物庫 | 抗癌藥物庫
關(guān)鍵字: 他拉唑帕利|||LT-673|||BMN-673|TargetMol

公司簡(jiǎn)介

上海陶術(shù)生物科技有限公司為美國Target Molecule Corp. ( Target Mol ) 在上海建立的全資子公司。我們與美國波士頓、德國慕尼黑的同事一起,為北美、歐洲和亞洲從事藥物研發(fā)和生物學(xué)研究的科學(xué)家提供優(yōu)質(zhì)的產(chǎn)品和專業(yè)的服務(wù)。公司下設(shè)篩選事業(yè)部,化學(xué)事業(yè)部,生物事業(yè)部和新材料部。 從虛擬篩選到實(shí)體化合物分子供應(yīng);從商業(yè)化產(chǎn)品銷售到個(gè)性化定制合成;從對(duì)明確靶點(diǎn)的分子篩選到對(duì)明確分子的多靶點(diǎn)篩選,從高通量篩選到化學(xué)結(jié)構(gòu)優(yōu)化,我們都可以滿足您的科研用品及技術(shù)服務(wù)的需求。 經(jīng)過在中國市場(chǎng)五年的精心耕耘,我們已成為篩選化合物領(lǐng)域優(yōu)秀的供應(yīng)商,為超過五百家學(xué)校和各類企業(yè)提供了品質(zhì)卓越的小分子化合物和藥物篩
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