Akt抑制剂VIII, Akti-1/2

Name: Akt抑制剂VIII, Akti-1/2
Brand: MM

InSolution, ≥95%, Isozyme-Selective

别名:

InSolution Akt抑制剂VII，同工酶选择性，Akti-1/2

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经验公式（希尔记法）:

C₃₄H₂₉N₇O

分子量:

551.64

NACRES:

NA.77

UNSPSC Code:

12352200

主要文件

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产品名称

Akt抑制剂VIII, Akti-1/2, InSolution, ≥95%, Isozyme-Selective

assay

≥95% (HPLC)

form

liquid

manufacturer/tradename

Calbiochem^®

storage condition

OK to freeze
desiccated (hygroscopic)
protect from light

shipped in

wet ice

storage temp.

−70°C

Quality Level

100

Biochem/physiol Actions

主要靶标
Akt1, Akt2, Akt3

产物不与ATP竞争。

可逆性：是

细胞可渗透性：是

靶标IC₅₀：在体外激酶测定中，Akt1，Akt2和Akt3分别为58 nM，210 nM和2.12 µM

Disclaimer

毒性：刺激性（B）

General description

Akt1/Akt2活性的细胞可渗透，有效和选择性抑制剂（在体外激酶测定中，Akt1，Akt2和Akt3的IC₅₀分别为58 nM，210 nM和2.12 µM）。据报道抑制作用具有普列克底物蛋白同源物（PH）域依赖性。即使在50 µM的高浓度情况下，它也不会对缺乏PH结构域的Akt或其他紧密相关的AGC家族激酶，PKA，PKC和SGK表现出任何抑制作用。克服了Akt1/Akt2介导的肿瘤细胞对化学疗法的抗性并显示出在体外培养的细胞和体内小鼠中均能阻断Akt1/Akt2的基础和刺激的磷酸化/激活。

Other Notes

Barnett, S.F., et al. 2005.Biochem.J.385, 399.
DeFeo-Jones, D., et al. 2005.Mol.Cancer Ther.4, 271.
Zhao, Z., et al. 2005.Bioorg.Med. Chem. Lett.15, 905.
Lindsley, C.W., et al. 2005.Bioorg.Med. Chem. Lett.15, 761.

Packaging

用惰性气体包装

请参考特定浓度批号的标签。

Physical form

10 mM（1 mg/181 µl）Akt抑制剂VIII，同工酶选择性，Akti-1/2（目录号124018）在DMSO中的溶液。

Preparation Note

初次解冻后，分装冻存（-70°C）。

Legal Information

CALBIOCHEM is a registered trademark of Merck KGaA, Darmstadt, Germany

存储类别

10 - Combustible liquids

wgk

WGK 2

flash_point_f

188.6 °F - closed cup - (Dimethylsulfoxide)

flash_point_c

87 °C - closed cup - (Dimethylsulfoxide)

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Alternative signaling pathways from IGF1 or insulin to AKT activation and FOXO1 nuclear efflux in adult skeletal muscle fibers.

Sarah J Russell et al.

The Journal of biological chemistry, 295(45), 15292-15306 (2020-09-02)

Muscle atrophy is regulated by the balance between protein degradation and synthesis. FOXO1, a transcription factor, helps to determine this balance by activating pro-atrophic gene transcription when present in muscle fiber nuclei. Foxo1 nuclear efflux is promoted by AKT-mediated Foxo1

Impaired degradation of YAP1 and IL6ST by chaperone-mediated autophagy promotes proliferation and migration of normal and hepatocellular carcinoma cells.

Enrico Desideri et al.

Autophagy, 19(1), 152-162 (2022-04-19)

Impaired degradation of the transcriptional coactivator YAP1 and IL6ST (interleukin 6 cytokine family signal transducer), two proteins deregulated in liver cancer, has been shown to promote tumor growth. Here, we demonstrate that YAP1 and IL6ST are novel substrates of chaperone-mediated

Akt抑制剂VIII, Akti-1/2

InSolution, ≥95%, Isozyme-Selective

选择尺寸

关于此项目

主要文件

属性

产品名称

assay

form

manufacturer/tradename

storage condition

shipped in

storage temp.

Quality Level

相关类别

说明

Biochem/physiol Actions

Disclaimer

General description

Other Notes

Packaging

Physical form

Preparation Note

Legal Information

安全信息

存储类别

wgk

flash_point_f

flash_point_c

文件

分析证书(COA)

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