NVP-CLR457

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NVP-CLR457

本产品不向个人销售，仅用作科学研究，不用于任何人体实验及非科研性质的动物实验。

CAS NO:

1453082-52-4

包装与价格：

包装	价格(元)
100mg	电议
250mg	电议
500mg	电议

产品介绍

NVP-CLR457 (compound 40) 是一种口服有效的和平衡的泛 I 类PI3K抑制剂。NVP-CLR457 显示出明显的剂量依赖性 PK / PD / 疗效关系。NVP-CLR457 具有抗肿瘤活性。

生物活性

NVP-CLR457 (compound 40) is an orally active, potent and balanced pan-class IPI3Kinhibitor. NVP-CLR457 shows a clear dose-dependent PK/PD/efficacy relationship. NVP-CLR457 has antitumor activity^[1].

IC₅₀& Target

PI3Kα

12 ± 1.5 nM (IC₅₀)

PI3Kβ

8.3 ± 1.0 nM (IC₅₀)

PI3Kδ

8.3 ± 2.0 nM (IC₅₀)

PI3Kγ

230 ± 31 nM (IC₅₀)

体外研究
(In Vitro)

NVP-CLR457 (compound 40) shows the mTOR activity, with an IC₅₀of 2474 ± 722 nM, and inhibits RPS6 phosphorylation with an IC₅₀of 1633 ± 54 nM^[1].
NVP-CLR457 has no impact on the DDR response at concentrations of 1 and 5 μM^[1].
NVP-CLR457 has no effect on the rate of microtubule polymerization^[1].

Western Blot Analysis

Cell Line:	U87MG cells^[1]
Concentration:	0, 1. 4, 16, 63, 250, 1000 nM
Incubation Time:	24 h
Result:	Inhibited the readouts of class I PI3K activity in a dose-dependent manner, with IC₅₀and IC₉₀values of 100 and 507 nM determined for the inhibition of S473P-Akt, and had no significant change in the readouts of mTOR activity.

体内研究
(In Vivo)

NVP-CLR457 (compound 40) (athymic nude mice bearing xenotransplanted Rat1-myr-p110α tumors, 3-20 mg/kg, PO, daily for 8 days) shows a dose-dependent inhibition of tumor growth^[1].
NVP-CLR457 (Mice bearing xenograft HBRX2524 human primary breast tumor, 40 mg/kg, PO, daily for 15 days) inhibits the tumor growth throughout the study^[1].
NVP-CLR457 (male Sprague-Dawley rats, 1.0 mg/kg, IV; 3.0 mg/kg, PO; once) shows high level of oral exposure and bioavailability^[1].
Pharmacokinetic Parameters of NVP-CLR457 in male Sprague-Dawley rats^[1].

compound	40
CL (mL/min/kg)	22 ± 6
Vss (L/kg)	4.4 ± 0.2
t_1/2(h)	3.3 ± 0.2
AUC iv (nM*h)	1770 ± 443
oral F (%)	97 ± 20
HDM FA (%)	37

NVP-CLR457 (3 mg/kg (IV) and 10 mg/kg (PO) for female OF1 mice, 0.1 mg/kg (IV), 0.3 mg/kg (PO) for male beagle dogs, once) shows low clearance, moderate volume of distribution, and rapid absorption leading to moderate to long half-lives and high oral bioavailability^[1].
Pharmacokinetic Parameters of NVP-CLR457 in female OF1 mice and male beagle dogs^[1].

species	mouse	dog
PPB (%)	76	71
CL (mL/min/kg)	10	3 ± 0
Vss (L/kg)	2	1.5 ± 0.2
t_1/2(h)	2	11 ± 3
AUC iv (nM*h)	3580	11213 ± 1169
AUC po (nM*h)	1738	11034 ± 1531
oral F (%)	49	98 ± 14
C_max(nM)	422	1121 ± 128
T_max(h)	0.5	1.3 ± 0.6

NVP-CLR457 (0.3-100 mg/kg, PO, once) leads to under-proportional increases in exposure (both AUC and Cmax) and much longer Tmax values^[1].
Pharmacokinetic Parameters of NVP-CLR457 in male Sprague Dawley rats, male beagle dogs^[1].

species	rat			dog
dose (mg/kg)	3	30	100	0.3	3
AUC (nM*h)	1709 ± 362	913 ± 251	784 ± 342	12,970 ± 1828	11,213 ± 1169
C_max(nM)	213 ± 61	41 ± 6	22 ± 4	1121 ± 128	309 ± 40
T_max(h)	0.5-2	4–24	24	1-2	2-24

Animal Model:	Sprague Dawley rats (male)^[1]
Dosage:	1 mg/kg (IV), 3 mg/kg (PO)
Administration:	IV or PO, once (Pharmacokinetic Analysis)
Result:	Showed high level of oral exposure and bioavailability.

Animal Model:	Female OF1 mice, male beagle dogs^[1]
Dosage:	3 mg/kg (IV) and 10 mg/kg (PO) for mice, 0.1 mg/kg (IV), 0.3 mg/kg (PO) for dogs
Administration:	IV or PO, once (Pharmacokinetic Analysis)
Result:	Showed low clearance, moderate volume of distribution, and rapid absorption leading to moderate to long half-lives and high oral bioavailability.

Animal Model:	Male Sprague Dawley rats, male beagle dogs^[1]
Dosage:	0.3, 3, 30, 100 mg/kg
Administration:	PO, once (Pharmacokinetic Analysis)
Result:	Led to under-proportional increases in exposure (both AUC and Cmax) and much longer Tmax values when it formulated as a suspension of the crystalline material.

Animal Model:	Female athymic nude mice (bearing xenotransplanted Rat1-myr-p110α tumors)^[1]
Dosage:	3, 10, and 20 mg/kg
Administration:	PO, daily for 8 days
Result:	Observed dose-dependent exposure and PD responses, and showed a dose-dependent inhibition of tumor growth. The 3 mg/kg dose achieved 80% S473P-Akt inhibition only at the 1 h time point; the 10 mg/kg dose at the 1 and 4 h time points; and the 20 mg/kg at the 1, 4, and 10 h time points, with a high level of inhibition remaining at the 14 h time point (76%).

Animal Model:	Mice bearing xenograft HBRX2524 human primary breast tumor^[1]Dosage: 40 mg/kg
Dosage:	40 mg/kg
Administration:	PO, daily for 15 days
Result:	Inhibited the tumor growth throughout the study, and showed a significant level of regression the end of the 15 day treatment period.

分子量

455.39

Formula

C₁₈H₂₀F₃N₇O₄

CAS 号

1453082-52-4

运输条件

Room temperature in continental US; may vary elsewhere.

储存方式

Please store the product under the recommended conditions in the Certificate of Analysis.