SAR125844

SAR125844 is a potent intravenously active and highly selective Met (c-Met) kinase inhibitor, displaying nanomolar activity against the wild-type kinase (IC50 value of 4.2 nmol/L) and H1094Y, Y1235D, M1250T, L1195V, and D1228H kinase domain mutants (IC50 values of 0.22, 1.7, 6.5, 65, and 81 nmol/L, respectively).

SAR125844化学構造

CAS No. 1116743-46-4

サイズ 価格(税別) 在庫状況
JPY 23100 国内在庫あり
JPY 69600 国内在庫あり

代表番号: 045-509-1970|電子メール:[email protected]
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製品安全説明書

現在のバッチを見る: S756401 DMSO] 11 mg/mL] false] Water] ˂1 mg/mL] false] Ethanol] ˂1 mg/mL] false 純度: 99.02%
99.02

SAR125844関連製品

シグナル伝達経路

c-Met阻害剤の選択性比較

生物活性

製品説明 SAR125844 is a potent intravenously active and highly selective Met (c-Met) kinase inhibitor, displaying nanomolar activity against the wild-type kinase (IC50 value of 4.2 nmol/L) and H1094Y, Y1235D, M1250T, L1195V, and D1228H kinase domain mutants (IC50 values of 0.22, 1.7, 6.5, 65, and 81 nmol/L, respectively).
Targets
MET H1094Y [2]
(Cell-free assay)
MET Y1235D [2]
(Cell-free assay)
WT MET [2]
(Cell-free assay)
MET M1250T [2]
(Cell-free assay)
TRKA/NTRK1 [2]
(Cell-free assay)
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0.22 nM 1.7 nM 4.2 nM 6.5 nM 39 nM
In Vitro
In vitro

SAR125844 is an ATP-competitive and reversible inhibitor. The biochemical selectivity of SAR125844 is documented in a panel of 275 human kinases and against tubulin. SAR125844 is moderately active on RON, a close structural homolog of MET, with IC50 value of approximately 740 nmol/L, suggesting that SAR125844 is highly (>100-fold) selective for the MET kinase over RON. Minimal inhibitory activity is identified on 5 additional kinases with IC50 values below 300 nmol/L, including TRKA/NTRK1 (39 nmol/L), TRKB/NTRK2 (280 nmol/L), PDGFRα-V561D (55 nmol/L), AXL (87 nmol/L), and MER (105 nmol/L). Biochemical activities on Aurora A and Aurora B are detected with IC50 values of 320 and 820 nmol/L, respectively, but these activities do not translate into cellular activity as demonstrated by the lack of antiproliferative activity in tumor cell lines without MET gene amplification. No activity on tubulin is detected up to 25 μmol/L of SAR125844. SAR125844 inhibits MET autophosphorylation in cell-based assays in the nanomolar range, and promotes low nanomolar proapoptotic and antiproliferative activities selectively in cell lines with MET gene amplification or pathway addiction[2].

細胞実験 細胞株 MKN-45, Hs 746T, and SNU-5 cells
濃度 --
反応時間 1 hour
実験の流れ

MKN-45, Hs 746T, and SNU-5 cells are seeded in poly d-lysine 96-well plates in complete medium. Plates are incubated with increasing SAR125844 concentrations for 1 hour, cell lysates are generated.

In Vivo
In Vivo

In PK studies in mice, the oral bioavailability of SAR125844 is low (∼2%), in line with its moderate Caco-2 permeability. In female SCID mice bearing xenograft tumors based on the MET-amplified Hs 746T human gastric tumor cell line, a single intravenous administration at 20 mg/kg is performed. plasma exposure of SAR125844 (area under the curve (AUC)) is 6190 h·ng/mL, the clearance moderate (CL = 3.1 L/h/kg), and the volume of distribution is large (Vss = 4.2 L/kg). A rapid and sustained uptake of SAR125844 in tumor tissue is observed, associated with a slower decrease of concentration from tumor tissue compared to the plasma concentration. The clearances of SAR125844 in mice, rats, and dogs are moderate. The plasma terminal elimination half-life (t1/2) is moderate (rats and dogs) to long (mice). The volume of distribution at steady state is moderate in dogs and large in rodents[1]. In two MET-amplified human gastric tumor xenograft models, SNU-5 and Hs 746T, intravenous treatment with SAR125844 leads to potent, dose- and time-dependent inhibition of the MET kinase and to significant impact on downstream PI3K/AKT and RAS/MAPK pathways. Daily or every-2-days intravenous treatment of SAR125844 promots a dose-dependent tumor regression in MET-amplified human gastric cancer models at tolerated doses without treatment-related body weight loss[2].

動物実験 動物モデル 8-10 weeks old SCID female mice
投与量 20 mg/kg
投与経路 i.v.
NCT Number Recruitment Conditions Sponsor/Collaborators Start Date Phases
NCT02435121 Completed
Neoplasm Malignant
Sanofi
November 2015 Phase 2
NCT01657214 Completed
Neoplasm Malignant
Sanofi
September 2012 Phase 1
NCT01391533 Completed
Malignant Solid Tumors
Sanofi
July 2011 Phase 1

化学情報

分子量 550.63 化学式

C25H23FN8O2S2

CAS No. 1116743-46-4 SDF --
Smiles C1COCCN1CCNC(=O)NC2=NC3=C(S2)C=C(C=C3)SC4=NN=C5N4N=C(C=C5)C6=CC=C(C=C6)F
保管 3 years -20°C powder

In vitro
Batch:

DMSO : 11 mg/mL ( (19.97 mM); 吸湿したDMSOは溶解度を減少させます。新しいDMSOをご使用ください。)

Water : ˂1 mg/mL

Ethanol : ˂1 mg/mL

モル濃度計算器

in vivo
Batch:

Add solvents to the product individually and in order.

投与溶液組成計算機

実験計算

モル濃度計算器

質量 濃度 体積 分子量

投与溶液組成計算機(クリア溶液)

ステップ1:実験データを入力してください。(実験操作によるロスを考慮し、動物数を1匹分多くして計算・調製することを推奨します)

mg/kg g μL

ステップ2:投与溶媒の組成を入力してください。(ロット毎に適した溶解組成が異なる場合があります。詳細については弊社までお問い合わせください)

% DMSO % % Tween 80 % ddH2O
%DMSO %

計算結果:

投与溶媒濃度: mg/ml;

DMSOストック溶液調製方法: mg 試薬を μL DMSOに溶解する(濃度 mg/mL, 注:濃度が当該ロットのDMSO溶解度を超える場合はご連絡ください。 )

投与溶媒調製方法:Take μL DMSOストック溶液に μL PEG300,を加え、完全溶解後μL Tween 80,を加えて完全溶解させた後 μL ddH2O,を加え完全に溶解させます。

投与溶媒調製方法:μL DMSOストック溶液に μL Corn oil,を加え、完全溶解。

注意:1.ストック溶液に沈殿、混濁などがないことをご確認ください;
2.順番通りに溶剤を加えてください。次のステップに進む前に溶液に沈殿、混濁などがないことを確認してから加えてください。ボルテックス、ソニケーション、水浴加熱など物理的な方法で溶解を早めることは可能です。

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