61350-00-3

中文名称 VU 0364770

英文名称 VU 0364770

CAS 61350-00-3

分子式 C12H9ClN2O

分子量 232.67

MOL 文件 61350-00-3.mol

更新日期 2024/04/27 11:50:37

61350-00-3 结构式

基本信息物理化学性质安全数据应用领域 VU 0364770价格(试剂级) 常见问题列表

基本信息

中文别名

N-(3-氯苯基)吡啶甲酰胺
N-(3-氯苯基)-2-吡啶甲酰胺

英文别名

VU 0364770
VU 0364770 100MG
VU 0364770 USP/EP/BP
VU0364770
VU-0364770
N-(3-Chlorophenyl)picolinamide
N-(3-chlorophenyl)pyridine-2-carboxamide
2-PyridinecarboxaMide, N-(3-chlorophenyl)-

所属类别

生物化工：GluR 拮抗剂

物理化学性质

熔点81-83 °C

沸点293.6±20.0 °C(Predicted)

密度1.341±0.06 g/cm3(Predicted)

储存条件Inert atmosphere,Store in freezer, under -20°C

溶解度DMF: 30 mg/ml; DMF:PBS (pH 7.2) (1:1): 0.5 mg/ml; DMSO: 25 mg/ml; Ethanol: 5 mg/ml

酸度系数(pKa)11.24±0.70(Predicted)

形态粉末

安全数据

危险性符号(GHS)

GHS07

警示词警告

危险性描述H302-H315-H319-H335

防范说明P261-P305+P351+P338

应用领域

用途1

N-(3-Chlorophenyl)-2-pyridinecarboxamide shows positive allosteric modulation at the mGlu4 receptors in combination with other antagonists resulting in treatment for the neurodegenerative Parkinson鈥檚 disease.

VU 0364770价格(试剂级)

报价日期	产品编号	产品名称	CAS号	包装	价格
2024/04/30	HY-100588	VU 0364770 VU0364770	61350-00-3	10mg	900元
2024/04/30	HY-100588	VU 0364770 VU0364770	61350-00-3	10mM * 1mLin DMSO	1024元
2024/04/30	HY-100588	VU 0364770 VU0364770	61350-00-3	25mg	1100元

常见问题列表

生物活性

VU0364770 是一种有效的选择性 mGlu4 正变构调节剂 (PAM)。VU0346770 对大鼠 mGlu4 和人 mGlu4 受体的 EC50 分别为 290 nM 和 1.1 μM。VU0364770 对 mGlu5 具有拮抗活性，EC50 为 17.9 μM，VU0364770 对 mGlu6 具有正变构调节活性，EC50 为 6.8 μM。VU0364770 还对 MAO 具有活性，作用于人 MAO-A 和 MAO-B 的 Ki 值分别为8.5 和 0.72 μM。

靶点

Rat mGlu ₄

290 nM (EC ₅₀ )

Human mGlu ₄

1.1 μM (EC ₅₀ )

mGlu ₆

6.8 μM (EC ₅₀ )

mGlu ₅

17.9 μM (EC ₅₀ )

体外研究

VU0364770 is a selective positive allosteric modulator of mGlu ₄ in recombinant systems. VU0364770 is a potent PAM of multiple signaling pathways that enhances the response of the rat and human mGlu ₄ receptors to the endogenous agonist glutamate. VU0364770 produces a concentration-dependent potentiation of the response to an EC ₂₀ concentration of glutamate with EC ₅₀ of 1.1±0.2 μM and increases the maximal response to glutamate from 100 to 227±17%. Because of concerns that this chemical scaffold might possess activity at MAO, full IC ₅₀ determinations is performed for VU0364770 at the MAO-A and MAO-B isoforms; these studies result in K _i s of 8.5 and 0.72 μM for human MAO-A and human MAO-B, respectively. When tested at a 10 μM concentration at each mGlu receptor, VU0364770 exhibits weak PAM activity (4.3-fold left shift of the glutamate CRC) at mGlu6 and antagonist activity (3.3-fold right shift of the glutamate CRC) at mGlu5 (compare to the 16.5-fold left shift of the glutamate concentration-response for mGlu ₄ at 10 μM). When further evaluated in a full concentration-response curve format, VU0364770 exhibits antagonist activity at mGlu ₅ with a potency of 17.9±5.5 μM and PAM activity at mGlu ₆ with a potency of 6.8±1.7 μM (compare with the potency of VU0364770 on the rat mGlu ₄ receptor of 290±80 nM).

体内研究

VU0364770 exhibits suitable pharmacokinetic properties for systemic dosing in animal models. After intravenous administration, VU0364770 is rapidly clears from the systemic circulation (165 ml/min/kg) and exhibits a volume of distribution of 2.92 L/kg. VU0364770 is a highly protein-bound ligand displaying free fractions of 2.7 and 1.8% in human and rat plasma, respectively. VU0364770 also shows an improved pharmacokinetic profile relative to previously reported mGlu ₄ PAMs with enhanced central penetration and a total brain-to-plasma ratio of more than 1 after systemic administration of a 10 mg/kg dose. VU0364770 produces a dose-dependent reversal of haloperidol-induced catalepsy. VU0364770 dose-dependently reverses haloperidol (0.75 mg/kg)-induced catalepsy in rats, significant at doses of 10 to 56.6 mg/kg, after subcutaneous dosing (F _6,69 =8.04; p<0.001).