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/ 组蛋白去乙酰化酶 / LMK-235

LMK-235 {[allProObj[0].p_purity_real_show]}

货号:A135784

LMK-235是一种强效且选择性的HDAC4/5抑制剂,对HDAC5HDAC4HDAC6HDAC1HDAC2HDAC11HDAC8IC50值分别为4.22 nM、11.9 nM、55.7 nM、320 nM、881 nM、852 nM和1278 nM,用于癌症研究。

LMK-235 化学结构 CAS号:1418033-25-6
LMK-235 化学结构
CAS号:1418033-25-6
LMK-235 3D分子结构
CAS号:1418033-25-6
LMK-235 化学结构 CAS号:1418033-25-6
LMK-235 3D分子结构 CAS号:1418033-25-6
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LMK-235 纯度/质量文件 产品仅供科研

货号:A135784 标准纯度: {[allProObj[0].p_purity_real_show]}
批次查询: 批次纯度:

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产品名称 HD1 HD2 HDAC HDAC1 HDAC10 HDAC11 HDAC2 HDAC3 HDAC4 HDAC5 HDAC6 HDAC7 HDAC8 HDAC9 其他靶点 纯度
Givinostat HCl monohydrate ++++

HD1-A, IC50: 16 nM

HD1-B, IC50: 7.5 nM

 		+++

HD2, IC50: 10 nM

 		99%+
MC1568 ++

HD1-A (Maize), IC50: 100 nM

HD1-B (Maize), IC50: 3.4 μM

 		96%
Trichostatin A ++++

HDAC, IC50: ~1.8 nM

 		99%+
Scriptaid 99%+
Valproic acid sodium Autophagy 97%
AR-42 +++

HDAC, IC50: 30 nM

 		99%+
Dacinostat +++

HDAC, IC50: 32 nM

 		98+%
CUDC-101 ++++

HDAC, IC50: 4.4 nM

 		++++

HDAC1, IC50: 4.5 nM

 		+++

HDAC10, IC50: 26.1 nM

 		+++

HDAC2, IC50: 12.6 nM

 		++++

HDAC3, IC50: 9.1 nM

 		+++

HDAC4, IC50: 13.2 nM

 		+++

HDAC5, IC50: 11.4 nM

 		++++

HDAC6, IC50: 5.1 nM

 		+

HDAC7, IC50: 373 nM

 		++

HDAC8, IC50: 79.8 nM

 		++

HDAC9, IC50: 67.2 nM

 		HER2,EGFR 99%+
M344 ++

HDAC, IC50: 100 nM

 		99%+
Splitomicin +

Sir2p, IC50: 60 μM

 		95%
Panobinostat ++++

HDAC (MOLT-4 cells), IC50: 5 nM

HDAC (Reh cells), IC50: 20 nM

 		98%
Sodium 4-Phenylbutyrate 98%
Vorinostat +++

HDAC, IC50: ~10 nM

 		98%
Curcumin NF-κB,Nrf2 98%
Belinostat +++

HDAC, IC50: 27 nM

 		98%
RG-2833 ++

HDAC1, Ki: 32 nM

 		++

HDAC3, Ki: 5 nM

 		98%
Valproic acid +

HDAC1, IC50: 0.4 mM

 		98%
BG45 +

HDAC1, IC50: 2 μM

 		+

HDAC2, IC50: 2.2 μM

 		+

HDAC3, IC50: 289 nM

 		99%+
Entinostat +

HDAC1, IC50: 0.51 μM

 		+

HDAC3, IC50: 1.7 μM

 		98%
Resminostat +++

HDAC1, IC50: 42.5 nM

 		++

HDAC3, IC50: 50.1 nM

 		++

HDAC6, IC50: 71.8 nM

 		98+%
Romidepsin +++

HDAC1, IC50: 36 nM

 		+++

HDAC2, IC50: 47 nM

 		99%+
Parthenolide NF-κB,p53 97% HPLC
Tacedinaline +

HDAC1, IC50: 0.9 μM

 		+

HDAC2, IC50: 0.9 μM

 		+

HDAC3, IC50: 1.2 μM

 		98%
Mocetinostat ++

HDAC1, IC50: 0.15 μM

 		+

HDAC11, IC50: 0.59 μM

 		+

HDAC2, IC50: 0.29 μM

 		+

HDAC3, IC50: 1.66 μM

 		98%
WT-161 ++++

HDAC1, IC50: 8.35 nM

 		+++

HDAC2, IC50: 15.4 nM

 		++++

HDAC6, IC50: 0.4 nM

 		99%+
Fimepinostat ++++

HDAC1, IC50: 1.7 nM

 		++++

HDAC10, IC50: 2.8 nM

 		++++

HDAC11, IC50: 5.4 nM

 		++++

HDAC2, IC50: 5.0 nM

 		++++

HDAC3, IC50: 1.8 nM

 		+++

HDAC6, IC50: 27 nM

 		99%+
Tucidinostat ++

HDAC1, IC50: 95 nM

 		++

HDAC10, IC50: 78 nM

 		++

HDAC2, IC50: 160 nM

 		++

HDAC3, IC50: 67 nM

 		99%+
Santacruzamate A ++++

HDAC2, IC50: 119 pM

 		99%+
(E,E)-RGFP966 ++

HDAC3, IC50: 80 nM

 		99%+
LMK-235 +++

HDAC4, IC50: 11.9 nM

 		++++

HDAC5, IC50: 4.2 nM

 		99%+
Tasquinimod 99%+
CAY10603 ++++

HDAC6, IC50: 2 pM

 		98%
Tubastatin A +++

HDAC6, IC50: 15 nM

 		98%
Tubacin ++++

HDAC6, IC50: 4 nM

 		99%+
ACY-738 ++++

HDAC6, IC50: 1.7 nM

 		99%+
Nexturastat A ++++

HDAC6, IC50: 5 nM

 		99%+
BRD73954 +++

HDAC6, IC50: 36 nM

 		++

HDAC8, IC50: 120 nM

 		98%
Tubastatin A HCl +++

HDAC6, IC50: 15 nM

 		+

HDAC8, IC50: 854 nM

 		98%
PCI-34051 +++

HDAC8, IC50: 10 nM

 		99%+
Ricolinostat ++

HDAC1, IC50: 58 nM

 		++

HDAC2, IC50: 48 nM

 		++

HDAC3, IC50: 51 nM

 		++++

HDAC6, IC50: 4.7 nM

 		++

HDAC8, IC50: 100 nM

 		99%+
Droxinostat +

HDAC3, IC50: 16.9 μM

 		+

HDAC6, IC50: 2.47 μM

 		+

HDAC8, IC50: 1.46 μM

 		99%+
Abexinostat ++++

HDAC1, Ki: 7 nM

 		+++

HDAC10, IC50: 24 nM

 		+++

HDAC2, Ki: 19 nM

 		++++

HDAC3/SMRT, Ki: 8.2 nM

 		+++

HDAC6, Ki: 17 nM

 		+

HDAC8, IC50: 280 nM

 		98%+
Citarinostat +++

HDAC1, IC50: 35 nM

 		+++

HDAC2, IC50: 45 nM

 		+++

HDAC3, IC50: 46 nM

 		++++

HDAC6, IC50: 2.6 nM

 		++

HDAC8, IC50: 137 nM

 		99%+
HPOB +

HDAC1, IC50: 2.9 μM

 		+

HDAC10, IC50: 3.0 μM

 		+

HDAC2, IC50: 4.4 μM

 		+

HDAC3, IC50: 1.7 μM

 		++

HDAC6, IC50: 56 nM

 		+

HDAC8, IC50: 2.8 μM

 		97%
Quisinostat 2HCl ++++

HDAC1, IC50: 0.11 nM

 		++++

HDAC10, IC50: 0.46 nM

 		++++

HDAC11, IC50: 0.37 nM

 		++++

HDAC2, IC50: 0.33 nM

 		++++

HDAC3, IC50: 4.86 nM

 		++++

HDAC4, IC50: 0.64 nM

 		++++

HDAC5, IC50: 3.69 nM

 		++++

HDAC8, IC50: 4.26 nM

 		99+%
Domatinostat +

HDAC1, IC50: 1.20 μM

 		+

HDAC10, IC50: 21 μM

 		+

HDAC11, IC50: 9.7 μM

 		+

HDAC2, IC50: 1.12 μM

 		+

HDAC3, IC50: 0.57 μM

 		+

HDAC5, IC50: 11.3 μM

 		+

HDAC9, IC50: 50 μM

 		99%+
TMP269 ++

HDAC4, IC50: 157 nM

 		++

HDAC5, IC50: 97 nM

 		+++

HDAC7, IC50: 43 nM

 		+++

HDAC9, IC50: 23 nM

 		99%+
Pracinostat ++

HDAC1, IC50: 49 nM

 		+++

HDAC10, IC50: 40 nM

 		++

HDAC11, IC50: 93 nM

 		++

HDAC2, IC50: 96 nM

 		+++

HDAC3, IC50: 43 nM

 		++

HDAC4, IC50: 56 nM

 		+++

HDAC5, IC50: 47 nM

 		+

HDAC6, IC50: 1.008 μM

 		++

HDAC7, IC50: 137 nM

 		++

HDAC8, IC50: 140 nM

 		++

HDAC9, IC50: 70 nM

 		99%+
TMP195 ++

HDAC4, Ki: 59 nM

 		++

HDAC5, Ki: 60 nM

 		+++

HDAC7, Ki: 26 nM

 		+++

HDAC9, Ki: 15 nM

 		99%+
1. 鼠标悬停在“+”上可以显示相关IC50的具体数值。"+"越多,抑制作用越强。2. "✔"表示该化合物对相应的亚型有抑制作用,但抑制强度暂时没有相关数据。

LMK-235 生物活性

靶点

  • HDAC4

    HDAC4, IC50:11.9 nM

  • HDAC5

    HDAC5, IC50:4.2 nM
描述 LMK235 a potent hydroxamate-based HDAC inhibitor with IC50 values of 320, 881, 11.9, 4.22, 55.7, 1278 and 852nM for HDAC1, 2, 4, 5, 6, 8 and 11, respectively. LMK235 inhibited HDAC activity of sensitive/Cisplatin-resistent MDA-MB-231, Cal27 and Kyse510 cells with IC50 values of 0.46μM/0.41μM, 0.36μM/0.36μM and 1μM /0.35μM, respectively, and exhibited cell growth inhibitory effect on sensitive/Cisplatin-resistent MDA-MB-231, Cal27 and Kyse510 cells with IC50 values of 1.37μM/1.68μM, 1.03μM/1.81μM and 2.96μM and 2.48μM, respectively. Compared with vorinostat, LMK235 showed similar effects on inhibition of cellular HDACs, but enhanced cytotoxic effects against the human cancer cell lines A2780, Cal27, Kyse510, and MDA-MB231. LMK-235 also showed nanomolar inhibition of HDAC4 and HDAC5, whereas vorinostat and TSA inhibit HDAC4 and HDAC5 in the higher micromolar range[2].
作用机制 LMK235 is a hydroxamate-based HDAC inhibitor which can chelate the catalytic zinc ion of HDAC. The alkoxyamide connecting unit linker region contributes to the selectivity of it.[2]

LMK-235 细胞研究

细胞系 浓度 检测类型 检测时间 活动说明 数据源
human A2780 cells Cytotoxicity assay 72 h Cytotoxicity against cisplatin resistant human A2780 cells after 72 hrs by MTT assay, IC50=0.32 μM 23252603
human A2780 cells Cytotoxicity assay 72 h Cytotoxicity against human A2780 cells after 72 hrs by MTT assay, IC50=0.49 μM 23252603
human A2780 cells Cytotoxicity assay 18 h Inhibition of HDAC in human A2780 cells after 18 hrs by fluorescence assay, IC50=0.65 μM 23252603
human HepG2 cells Cytotoxicity assay 48 h Cytotoxicity against human HepG2 cells after 48 hrs, IC60=1.26 μM 24904967

LMK-235 动物研究

Dose Mice: 1 mg/kg, 3 mg/kg[2] (i.p.), 5 mg/kg - 30 mg/kg[3] (right lateral ventricle through a 25 μl Hamilton syringe)
Administration i.p.

LMK-235 参考文献

[1]Marek L, Hamacher A, et al. Histone deacetylase (HDAC) inhibitors with a novel connecting unit linker region reveal a selectivity profile for HDAC4 and HDAC5 with improved activity against chemoresistant cancer cells. J Med Chem. 2013 Jan 24;56(2):427-36.

[2]Marek L, Hamacher A, Hansen FK, Kuna K, Gohlke H, Kassack MU, Kurz T. Histone deacetylase (HDAC) inhibitors with a novel connecting unit linker region reveal a selectivity profile for HDAC4 and HDAC5 with improved activity against chemoresistant cancer cells. J Med Chem. 2013 Jan 24;56(2):427-36. doi: 10.1021/jm301254q. Epub 2013 Jan 8. PMID: 23252603.

LMK-235 实验方案

计算器
存储液制备 1mg 5mg 10mg

1 mM

5 mM

10 mM

3.40mL

0.68mL

0.34mL

16.99mL

3.40mL

1.70mL

33.97mL

6.79mL

3.40mL

LMK-235 技术信息

CAS号1418033-25-6
分子式C15H22N2O4
分子量 294.346
别名
运输蓝冰
存储条件

液体 -20°C:3-6个月-80°C:12个月

粉末 Sealed in dry,2-8°C
溶解度

DMSO: 30 mg/mL(101.92 mM),注意:DMSO长时间开封后,会吸水并导致溶解能力下降,请避免使用长期开封的DMSO
动物实验配方

5%DMSO+30%PEG300+5%TW80+water 13 mg/mL

Tags: LMK-235 | 1418033-25-6 | LMK235 | LMK 235 | HDAC4/5 Inhibitor | Cell Cycle/DNA Damage | Epigenetics | HDAC | 仅供科研使用 | AmBeed-信号通路专用抑制剂 | LMK-235 纯度/质量文件 | LMK-235 亚型比较 | LMK-235 生物活性 | LMK-235 细胞研究 | LMK-235 动物研究 | LMK-235 参考文献 | LMK-235 实验方案 | LMK-235 技术信息

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