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化合物 Prexasertib dihydrochloride,Prexasertib dihydrochloride
  • 化合物 Prexasertib dihydrochloride,Prexasertib dihydrochloride

化合物 Prexasertib dihydrochloride|T4327|TargetMol

價(jià)格 398 578 1080
包裝 1mg 2mg 5mg
最小起訂量 1mg
發(fā)貨地 上海
更新日期 2024-09-30
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產(chǎn)品詳情

中文名稱:化合物 Prexasertib dihydrochloride英文名稱:Prexasertib dihydrochloride
CAS:1234015-54-3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: 99.82%產(chǎn)品類別: 抑制劑
貨號(hào): T4327
2024-09-30 化合物 Prexasertib dihydrochloride Prexasertib dihydrochloride 1mg/398RMB;2mg/578RMB;5mg/1080RMB 398 TargetMol 美國 Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice. 99.82% 抑制劑

Product Introduction

Bioactivity

名稱Prexasertib dihydrochloride
描述Prexasertib dihydrochloride (LY2606368) is an ATP-competitive CHK1 inhibitor (Ki: 0.9 nmol/L). in the cell-free assay, its IC50 values are 8 nM and 9 nM for CHK2 and RSK, respectively.
細(xì)胞實(shí)驗(yàn)HeLa cells were plated onto T25 flasks and allowed to recover for 24 hours.LY2606368 was then added to give final concentrations of 33 or 100 nmol/L.In some experiments,20 μMol/L Z-VAD-FMK was included during the drug treatment.Cells were treated for 12 hours,and during the last 2 hours,colchicine was added to 1 μg/mL.Fixation of nuclei for metaphase spreads was done following the method of Bayani and Squire.Chromosome spreads were done.A 12-μL volume of cell suspension in 3:1 methanol/acetic acid fixative was dropped from a height of 3 cm onto dry glass slides or coverslips.The slides were then heated for 45 seconds on a 43°C metal block,before being removed to allow drying to complete at room temperature.Coverslips were mounted on slides with Vectashield Hard Set mounting medium with DAPI.Slides were examined with a Leica DMR fluorescence microscope and images were captured using a SPOT RT3 Slider camera.
激酶實(shí)驗(yàn)The interaction of COTI-2 with 227 kinases is tested using the AMBIT BIOSCIENCES KINOMESCAN assay. In brief, streptavidin-coated magnetic beads are treated with biotinylated small molecule ligands for 30 min at 25°C to generate affinity resins for kinase assays. The liganded beads are blocked with excess biotin and washed with blocking buffer (1% BSA, 0.05% Tween 20, 1 mM DTT) to remove unbound ligand and to reduce non-specific binding. Binding reactions are assembled by combining phage lysates, liganded affinity beads, and COTI-2 in 1× binding buffer (20% SeaBlock, 0.17× PBS, 0.05% Tween 20, 6 mM DTT). All reactions are carried out in polystyrene 96-well plates that have been pre-treated with blocking buffer in a final volume of 0.1 mL.
動(dòng)物實(shí)驗(yàn)LY2606368 is formulated in a vehicle consisting of 20% Captisol.Female CD-1 nu-/nu- mice (26-28 g) are used for this study. Tumor growth is initiated by subcutaneous injection of 1×106 Calu-6 cells in a 1:1 mixture of serum-free growth medium and Matrigel in the rear flank of each subject animal. When tumor volumes reach approximately 150 mm3 in size, the animals are randomized by tumor size and body weight and placed into their respective treatment groups. The vehicle consisting of 20% Captisol pH4 or LY2606368 is administered by subcutaneous injection in a volume of 200 μL. Four, eight, 12, 24, and 48 hours after drug administration, blood for plasma drug exposure is extracted via cardiac puncture and assayed on a Sciex API 4000 LC/MS-MS system. The xenograft tissue is promptly removed and prepared. Lysates were analyzed by immunoblot analysis for protein phosphorylation levels.
體外活性LY2606368 induces DNA damage and increases in pH2A.X. In cells, LY2606368 causes the rapid appearance of TUNEL and pH2AX-positive double-stranded DNA breaks in the S-phase cell population. In a functional assay, LY2606368 effectively abrogates the G2–M checkpoint activated by doxorubicin in p53-deficient HeLa cells (EC50: 9 nM). LY2606368 was broadly antiproliferative in the most sensitive cell lines (IC50s<50 nM) with a minority of cell lines showing considerable resistance (IC50s >1,000 nM). LY2606368 requires CDK2 and CDC25A to cause DNA damage.
體內(nèi)活性In cancer xenografts, LY2606368 inhibits tumor growth by monotherapy and combined with other agents. In an orthotopic SKOV3 ovarian cancer model, LY2606368 inhibits the growth of primary tumors and markedly reduces the incidence of metastases and ascites accumulation. In an SW1990 orthotopic pancreatic cancer model, LY2606368 also causes a 92% inhibition of primary tumor growth and the elimination of metastases to the lymph node, spleen, and intestine.
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 : 4.38 mg/mL (10 mM), Sonication is recommended.
關(guān)鍵字Apoptosis | CDK2 | ARK5 | replication | RSK1 | inhibit | MELK | DNA | HeLa | Inhibitor | Prexasertib dihydrochloride | HT-29 | Prexasertib Dihydrochloride | double-stranded | BRSK2 | ATP-competitive | CDC25A | S296 | S516 | autophosphorylation | H2AX | LY 2606368 | LY-2606368 | SIK | Checkpoint Kinase (Chk) | Prexasertib
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關(guān)鍵字: Prexasertib HCl|||LY2606368 (dihydrochloride)|||LY2606368|TargetMol

公司簡介

TargetMol Chemicals Inc. 總部位于馬薩諸塞州波士頓,致力于為全球生化領(lǐng)域科學(xué)家的研究提供專業(yè)的產(chǎn)品和服務(wù)。TargetMol?品牌的客戶群分布于40多個(gè)國家和地區(qū),已發(fā)展成為全球知名的化合物庫和小分子化合物研究供應(yīng)商。 TargetMol?可提供160多種滿足不同需求的化合物庫,以及多種類型的生化試劑產(chǎn)品,包括12000多種抑制劑、16000多種天然產(chǎn)物和各類多肽、抗體、生命科學(xué)試劑盒等,此外,我們還建設(shè)有CADD(計(jì)算機(jī)輔助藥物設(shè)計(jì))研究中心、藥理實(shí)驗(yàn)室、藥化合成平臺(tái)三大技術(shù)中心,全方位滿足客戶的定制需求。 憑借我們優(yōu)質(zhì)的產(chǎn)品和服務(wù)、快速高效的全球供應(yīng)鏈和專業(yè)的技術(shù)支持,我們將有效幫助您縮短研發(fā)周期,取得更成功的結(jié)果。
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主營行業(yè) 天然產(chǎn)物,生化試劑,分子生物學(xué),分子砌塊,生物技術(shù)服務(wù) 經(jīng)營模式 貿(mào)易,工廠,試劑,定制,服務(wù)
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  • 公司成立:12年
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  • 企業(yè)類型:有限責(zé)任公司(自然人投資或控股)
  • 主營產(chǎn)品:小分子抑制劑、藥物篩選化合物庫、藥物篩選等
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