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组蛋白去乙酰化酶 mGluR Amino Acids and Amino Acid Derivatives
/ (S)-4CPG

(S)-4CPG {[allProObj[0].p_purity_real_show]}

货号:A462285 同义名: (S)-4-Carboxyphenylglycine

(S)-4CPG is a selective competitive group I mGlu antagonist.

(S)-4CPG 化学结构 CAS号:134052-73-6
(S)-4CPG 化学结构
CAS号:134052-73-6
(S)-4CPG 3D分子结构
CAS号:134052-73-6
(S)-4CPG 化学结构 CAS号:134052-73-6
(S)-4CPG 3D分子结构 CAS号:134052-73-6
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(S)-4CPG 纯度/质量文件 产品仅供科研

货号:A462285 标准纯度: {[allProObj[0].p_purity_real_show]}
批次查询: 批次纯度:

全球学术期刊中引用的产品

更多 >
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-B, IC50: 7.5 nM

HD1-A, IC50: 16 nM

 		+++

HD2, IC50: 10 nM

 		99%+
MC1568 ++

HD1-B (Maize), IC50: 3.4 μM

HD1-A (Maize), IC50: 100 nM

 		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

 		++++

HDAC3, IC50: 9.1 nM

 		+++

HDAC4, IC50: 13.2 nM

 		+++

HDAC5, IC50: 11.4 nM

 		+

HDAC7, IC50: 373 nM

 		++

HDAC8, IC50: 79.8 nM

 		++

HDAC9, IC50: 67.2 nM

 		EGFR,HER2 99%+
M344 ++

HDAC, IC50: 100 nM

 		99%+
Splitomicin +

Sir2p, IC50: 60 μM

 		99%
Panobinostat ++++

HDAC (Reh cells), IC50: 20 nM

HDAC (MOLT-4 cells), IC50: 5 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

 		++++

HDAC3, IC50: 1.8 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

 		99%
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

 		+

HDAC3, IC50: 1.7 μM

 		+

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

 		97%
Domatinostat +

HDAC1, IC50: 1.20 μM

 		+

HDAC10, IC50: 21 μM

 		+

HDAC11, IC50: 9.7 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

 		++

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。

(S)-4CPG 生物活性

描述 (S) -4CPG acts as competitive antagonists for mGluR1 with pA2 values of 4.46[1]. Early (S)-4CPG treatment significantly attenuated the development of mechanical allodynia (90 and 270 nmol) and cold hyperalgesia (270 nmol). However, late treatment with (S)-4CPG did not reduce the nociceptive behaviours in either behavioural task[2]. The decrease in the seizure threshold for pentylenetetrazole during diazepam withdrawal was significantly suppressed by intracerebroventricular (i.c.v.) pretreatment with the group 1 mGlu receptor antagonist, (S)-4-carboxyphenylglycine ((S)-4CPG: 56 and 100 nmol)[3]. i.t. treatment with MK-801 significantly reduced nociceptive scores in the formalin test and also produced a significant suppression of formalin-induced increases in [3H]-PDBu binding in laminae I-II, III-VI and X of the lumbar spinal cord. In contrast, i.t. treatment with (S)-4CPG failed to significantly affect either nociceptive behaviours in the formalin test or formalin-induced increases in [3H]-PDBu binding in laminae I-II and III-VI of the lumbar spinal cord. On the other hand, i.t. treatment with either MK-801 or (S)-4CPG produced a significant reduction in mechanical and cold hypersensitivity, as well as [3H]-PDBu binding in laminae I-II and III-VI of the lumbar spinal cord, after CCI(chronic constriction injury)[4].

(S)-4CPG 参考文献

[1]Hayashi Y, Sekiyama N, Nakanishi S, Jane DE, Sunter DC, Birse EF, Udvarhelyi PM, Watkins JC. Analysis of agonist and antagonist activities of phenylglycine derivatives for different cloned metabotropic glutamate receptor subtypes. J Neurosci. 1994 May;14(5 Pt 2):3370-7

[2]Fisher K, Fundytus ME, Cahill CM, Coderre TJ. Intrathecal administration of the mGluR compound, (S)-4CPG, attenuates hyperalgesia and allodynia associated with sciatic nerve constriction injury in rats. Pain. 1998 Jul;77(1):59-66

[3]Suzuki T, Shimizu N, Tsuda M, Soma M, Misawa M. Role of metabotropic glutamate receptors in the hypersusceptibility to pentylenetetrazole-induced seizure during diazepam withdrawal. Eur J Pharmacol. 1999 Mar 19;369(2):163-8

[4]Yashpal K, Fisher K, Chabot JG, Coderre TJ. Differential effects of NMDA and group I mGluR antagonists on both nociception and spinal cord protein kinase C translocation in the formalin test and a model of neuropathic pain in rats. Pain. 2001 Oct;94(1):17-29

(S)-4CPG 实验方案

计算器
存储液制备 1mg 5mg 10mg

1 mM

5 mM

10 mM

5.12mL

1.02mL

0.51mL

25.62mL

5.12mL

2.56mL

51.24mL

10.25mL

5.12mL

(S)-4CPG 技术信息

CAS号134052-73-6
分子式C9H9NO4
分子量 195.17
SMILES Code O=C(O)[C@@H](N)C1=CC=C(C(O)=O)C=C1
MDL No. MFCD00216831
别名 (S)-4-Carboxyphenylglycine
运输蓝冰
InChI Key VTMJKPGFERYGJF-ZETCQYMHSA-N
Pubchem ID 5311459
存储条件

In solvent -20°C:3-6个月-80°C:12个月

Pure form Keep in dark place, inert atmosphere, 2-8°C

Tags: (S)-4CPG | 134052-73-6 | (S)-4-Carboxyphenylglycine | mGluR | mGluR Agonist | GPCR/G Protein | Neuronal Signaling | mGluR | 仅供科研使用 | AmBeed-信号通路专用抑制剂 | (S)-4CPG 纯度/质量文件 | (S)-4CPG 亚型比较 | (S)-4CPG 生物活性 | (S)-4CPG 参考文献 | (S)-4CPG 实验方案 | (S)-4CPG 技术信息

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