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          目錄:MedChemExpress LLC>>生化試劑>> Retaspimycin Hydrochloride | MCE

          Retaspimycin Hydrochloride | MCE
          • Retaspimycin Hydrochloride | MCE
          參考價 950
          具體成交價以合同協(xié)議為準
          參考價 950
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          更新時間:2023-06-14 13:05:12瀏覽次數(shù):119評價

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          CAS 857402-63-2 純度 98.35%
          分子量 624.17 分子式 C??H??ClN?O?
          供貨周期 現(xiàn)貨 規(guī)格 1 mg
          貨號 HY-10210 應(yīng)用領(lǐng)域 醫(yī)療衛(wèi)生,化工,生物產(chǎn)業(yè),制藥
          Retaspimycin Hydrochloride | MCERetaspimycin Hydrochloride is a potent inhibitor of <b>Hsp90</b> with <b>EC<sub>50</sub></b>s of 119 nM for both Hsp90 and Grp9.

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          Retaspimycin Hydrochloride

          CAS No. : 857402-63-2

          產(chǎn)品活性:Retaspimycin Hydrochloride is a potent inhibitor of Hsp90 with EC50s of 119 nM for both Hsp90 and Grp9.

          研究領(lǐng)域:Cell Cycle/DNA Damage  |  Metabolic Enzyme/Protease

          作用靶點:HSP

          In Vitro: Retaspimycin (IPI-504) is a novel and highly soluble analog of 17AAG, an inhibitor of Hsp90. Retaspimycin can abrogate both the unfolded protein response element (UPRE) and ERSE-driven luciferase activity in non-treated U266 and MM.1s cells as well as in Tunicamycin (Tm)-treated cells. The IC50s for the inhibition of reporter gene activity by Retaspimycin are 196±56 nM in U266 and 472±177 nM in MM.1s for UPRE-luc activity and 213±140 nM for the ERSE-driven activity in MM.1s cells. Retaspimycin treatment leads to a dose-dependent decrease of p50ATF6 with EC50 of 237 nM, consistent with the reporter-gene assay. The level of sXBP1 is decreased in the presence of Retaspimycin with an apparent EC50 between 300 nM and 1 μM. Incubation of Retaspimycin (IPI-504) potently suppresses both Akt and MAPKs phosphorylation in both sensitive and Trastuzumab-resistant cells. Total levels of Akt decreased in all 4 cell lines (BT474, SKBR-3, HCC1569, and HCC1569) in a dose-dependent manner. However, levels of total MAPKs are not significantly altered with Retaspimycin treatment.

          In Vivo: Retaspimycin (IPI-504) and Trastuzumab independently induce tumor regression of Trastuzumab-sensitive BT474 cell-derived xenografts. Xenografts derived from BT474R cells continue to grow in the presence of Trastuzumab but are still sensitive to Retaspimycin. When used in combination, Retaspimycin and Trastuzumab add only marginal benefits to Retaspimycin monotherapy. Retaspimycin (100 mg/kg) as a single agent is more efficacious than Trastuzumab in inhibiting tumor growth in HCC1569 xenografts. The combination is not significantly superior to Retaspimycin used as a single agent.

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