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PIK-93

    
99.9%

PIK-93

源葉(MedMol)
S80818 一鍵復制產品信息
593960-11-3
C14H16ClN3O4S2
389.88
PIK93; PIK 93; PIK-93;N-[5-[4-Chloro-3-[(2-hydroxyethyl)sulfamoyl]phenyl]-4-methylthiazol-2-yl]acetamide
貨號 規格 價格 上海 北京 武漢 南京 購買數量
S80818-5mg
99.9% ¥540.00 6 - - -
S80818-10mg
99.9% ¥850.00 5 - - -
S80818-25mg
99.9% ¥1700.00 4 - - -
S80818-100mg
≥99% ¥4600.00 貨期:2-3天 - - -
產品介紹 參考文獻 質檢證書(COA) 摩爾濃度計算器 相關產品

產品介紹

PIK-93 is the first potent, synthetic PI4K inhibitor with IC50 of 19 nM; inhibits PI3Kα with IC50 of 39 nM.

產品描述: PIK-93 is the first potent, synthetic PI4K inhibitor with IC50 of 19 nM; inhibits PI3Kα with IC50 of 39 nM.
靶點: ATM/ATR;Carbonic Anhydrase;DNA-PK;HSV;mTOR;PI3K;PI4K;Virus Protease;ATM/ATR;DNA-PK;VirusProtease;PI3K;CarbonicAnhydrase;PI4K;mTOR;HSV
體外研究: PIK-93 inhibits PI3Kγ and PI4KIIIβ, with IC50 values of 16 nM and 19 nM, respectively. PIK-93 also inhibits other members of PI3Ks, including PI3Kα, β, and δ, with IC50 values of 39 nM, 0.59 μM, and 0.12 μM, respectively. PIK-93 shows no obvious inhibitory effect against a panel of other kinases, even at a concentration of 10 μM. In differentiated HL60 (dHL60) cells, PIK-93 (0.5 μM-1 μM) impairs consolidation and stability of the leading edge formed after treatment with uniform f-Met-Leu-Phe (fMLP). PIK-93 alters the localization, but not the amount, of the fMLP-dependent accumulation of total F-actin. In fMLP gradients, PIK-93 reduces the chemotactic index and triples the cells' turning frequency. In COS-7 cells, PIK-93 (250 nM) effectively abrogates the accumulation of CERT-PH domain and FL-Cer in Golgi. PIK-93 of the same concentration also significantly inhibits the conversion of [3H]serine-labeled endogenous ceramide to sphingomyelin. These facts indicate a key role of PI4KIIIβ in ceramide transport between the ER and Golgi, as well as in the regulation of spingomyelin synthesis. In T6.11 cells, PIK-93 (300 nM) reduces carbachol-induced translocation of TRPC6 to the plasma membrane and net Ca2+ entry. A recent report shows that PIK-93 has anti-enterovirus effects, as revealed by its inhibition of both poliovirus (PV) and hepatitis C virus (HCV) replication, with EC50 values of 0.14 μM and 1.9 μM, respectively.
體內研究: 0.5 μM-1 μM PIK-93作用于分化的HL60細胞,損害用f-Met-Leu-Phe處理而形成的聚集的穩定性。在COS-7細胞中,PIK-93(250 nM)有效地消除了高爾基體中CERT-PH結構域和FL-Cer的積累。在T6.11細胞中,300 nM PIK-93降低Carbachol誘導的TRPC6移位到質膜上和Ca2+進入。相同濃度PIK-93也明顯抑制[3H]絲氨酸標記的內源性神經酰胺轉變為神經鞘磷脂。這些說明了PI4KIIIβ在內質網和高爾基體中的神經酰胺轉移時具有重要作用,以及有效調節鞘磷脂的合成。一項研究顯示,PIK-93具有抗腸道病毒功能,抑制脊髓灰質炎病毒和丙型肝炎病毒復制,EC50分別為0.14 μM和1.9 μM。PIK-93有效抑制PI3Kγ和PI4KIIIβ,IC50分別為16 nM和19 nM。PIK-93也抑制其他PI3Ks成員,包括PI3Kα,β和δ,IC50分別為39 nM,0.59 μM和0.12 μM。而PIK-93對其他激酶幾乎沒有抑制效果,即使濃度為10 μM
細胞實驗: For actin staining, dHL60 cells are preincubated in suspension with PIK-93 or vehicle for 40 min, centrifuged for 5 min at 2000 rpm at room temperature in a J6-B centrifuge, resuspended in mHBSS containing the respective agent at the same concentration, allowed to stick to fibronectin-covered coverslips, and subjected to stimulation with a uniform concentration of 100 nM f-Met-Leu-Phe (fMLP) for 3 min. Cellsare fixed in 3.7% PFA and stained with 10 units/mL rhodamine-phalloidin for 15 min.(Only for Reference)
參考文獻: 1. Monet M, et al. J BiolChem, 2012, Epub ahead of print. 2. VanKeymeulen A, et al. Cell Biol. 2006, 174(3), 437-445. 3. Tóth B, et al. J BiolChem, 2006, 281(47), 36369-3637 4. Knight ZA, Cell, 2006, 125(4), 733-747. 5. Arita M, et al. J Virol, 2011, 85(5), 2364-2372.
溶解性: soluble  in  DMSO
保存條件: -20℃
配置溶液濃度參考:
1mg 5mg 10mg
1 mM 2.565 ml 12.824 ml 25.649 ml
5 mM 0.513 ml 2.565 ml 5.13 ml
10 mM 0.256 ml 1.282 ml 2.565 ml
50 mM 0.051 ml 0.256 ml 0.513 ml
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參考文獻

質檢證書(COA)

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摩爾濃度計算器

質量 (mg) = 濃度 (mM) x 體積 (mL) x 分子摩爾量 (g/mol)

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