BMS-536924

Modify Date: 2024-01-08 14:39:14

BMS-536924 Structure
BMS-536924 structure
Common Name BMS-536924
CAS Number 468740-43-4 Molecular Weight 479.959
Density 1.4±0.1 g/cm3 Boiling Point N/A
Molecular Formula C25H26ClN5O3 Melting Point N/A
MSDS N/A Flash Point N/A

 Use of BMS-536924


BMS-536924 is an ATP-competitive IGF-1R/IR inhibitor with IC50 of 100 nM/73 nM.IC50 value: 100 nM (IGF-1R); 73 nM (IR) [1]Target: IGF-1R; IRin vitro: BMS-536924 also inhibits FAK and Lck with IC50 of 150 nM and 341 nM, respectively. BMS-536924 inhibits cellular proliferation and disrupts Akt and MAPK phosphorylation [1]. BMS-536924 inhibits IGF-I-stimulated IGF-1R signaling in MCF10A cells and blocks constitutive IGF-1R activity in CD8-IGF-1R-MCF10A. Preincubation of MCF10A cells with 1 μM BMS-536924 completely blocks the ability of IGF-I to stimulate IGF-1R phosphorylation. IGF-I stimulation results in increased phosphorylation of ERK1/2, GSK3β, and Akt. BMS-536924 inhibits this ligand-induced phosphorylation. Treatment of the CD8-IGF-1R-MCF10A cells with BMS-536924 results in a dose-dependent inhibition of phosphorylation with partial inhibition at 0.01 μM and 0.1 μM, but complete receptor inhibition at a concentration of 1 μM. Maximal inhibition of phosphorylated IGF-1R is observed as early as 10 minutes following incubation. BMS-536924 retains its ability to inhibit IGF-1R phosphorylation for up to 48 hours. Addition of BMS-536924 time-dependently inhibits Akt phosphorylation starting at 1 hour. By 48 hours, Akt activation is completely blocked [2]. in vivo: Oral administration of BMS-536924 at 100-300 mpk strongly inhibits IGR-1R Sal tumor model. Efficacy is also observed in the nonengineered Colo205 human colon carcinoma mode. Oral administration of 3 on a once a day schedule (100-300 mpk) or a twice a day schedule (50, 100 mpk) demonstrates antitumor activity in this tumor model. Oral glucose tolerance test (OGTT) shows 100 mpk (b.i.d.) causes a significant elevation in glucose levels after glucose challenge. The pharmacokinetic parameters of BMS-536924, administered orally in poly(ethylene glycol) 400 and water (80:20 v/v), are determined in mouse, rat, dog, and monkey. Good bioavailability is evident in all species. Significant nonlinear pharmacokinetics is observed in rodents at increasing p.o. dose [1]. Oral administration of 70 mg/kg BMS-536924 significantly inhibits tumor growth (TGBC-1TKB cells) inoculated in nude mice. BMS-536924 up regulates apoptosis in xenografts tumors. The treatment doesn't have adverse effects on the body weight of mice or the glucose levels at the time of death, suggesting tolerable toxicity [3].

 Names

Name (S)-4-[2-(3-Chloro-phenyl)-2-hydroxy-ethylamino]-3-(4-methyl-6-morpholin-4-yl-1H-benzoimidazol-2-yl)-1H-pyridin-2-one
Synonym More Synonyms

 BMS-536924 Biological Activity

Description BMS-536924 is an ATP-competitive IGF-1R/IR inhibitor with IC50 of 100 nM/73 nM.IC50 value: 100 nM (IGF-1R); 73 nM (IR) [1]Target: IGF-1R; IRin vitro: BMS-536924 also inhibits FAK and Lck with IC50 of 150 nM and 341 nM, respectively. BMS-536924 inhibits cellular proliferation and disrupts Akt and MAPK phosphorylation [1]. BMS-536924 inhibits IGF-I-stimulated IGF-1R signaling in MCF10A cells and blocks constitutive IGF-1R activity in CD8-IGF-1R-MCF10A. Preincubation of MCF10A cells with 1 μM BMS-536924 completely blocks the ability of IGF-I to stimulate IGF-1R phosphorylation. IGF-I stimulation results in increased phosphorylation of ERK1/2, GSK3β, and Akt. BMS-536924 inhibits this ligand-induced phosphorylation. Treatment of the CD8-IGF-1R-MCF10A cells with BMS-536924 results in a dose-dependent inhibition of phosphorylation with partial inhibition at 0.01 μM and 0.1 μM, but complete receptor inhibition at a concentration of 1 μM. Maximal inhibition of phosphorylated IGF-1R is observed as early as 10 minutes following incubation. BMS-536924 retains its ability to inhibit IGF-1R phosphorylation for up to 48 hours. Addition of BMS-536924 time-dependently inhibits Akt phosphorylation starting at 1 hour. By 48 hours, Akt activation is completely blocked [2]. in vivo: Oral administration of BMS-536924 at 100-300 mpk strongly inhibits IGR-1R Sal tumor model. Efficacy is also observed in the nonengineered Colo205 human colon carcinoma mode. Oral administration of 3 on a once a day schedule (100-300 mpk) or a twice a day schedule (50, 100 mpk) demonstrates antitumor activity in this tumor model. Oral glucose tolerance test (OGTT) shows 100 mpk (b.i.d.) causes a significant elevation in glucose levels after glucose challenge. The pharmacokinetic parameters of BMS-536924, administered orally in poly(ethylene glycol) 400 and water (80:20 v/v), are determined in mouse, rat, dog, and monkey. Good bioavailability is evident in all species. Significant nonlinear pharmacokinetics is observed in rodents at increasing p.o. dose [1]. Oral administration of 70 mg/kg BMS-536924 significantly inhibits tumor growth (TGBC-1TKB cells) inoculated in nude mice. BMS-536924 up regulates apoptosis in xenografts tumors. The treatment doesn't have adverse effects on the body weight of mice or the glucose levels at the time of death, suggesting tolerable toxicity [3].
Related Catalog
References

[1]. Wittman M, et al. Discovery of a (1H-benzoimidazol-2-yl)-1H-pyridin-2-one (BMS-536924) inhibitor of insulin-like growth factor I receptor kinase with in vivo antitumor activity. J Med Chem. 2005 Sep 8;48(18):5639-43.

[2]. Litzenburger BC, et al. BMS-536924 reverses IGF-IR-induced transformation of mammary epithelial cells and causes growth inhibition and polarization of MCF7 cells. Clin Cancer Res. 2009 Jan 1;15(1):226-37.

[3]. Ohashi H, et al. Insulin-like growth factor receptor expression is associated with aggressive phenotypes and has therapeutic activity in biliary tract cancers. Cancer Sci. 2012 Feb;103(2):252-61.

 Chemical & Physical Properties

Density 1.4±0.1 g/cm3
Molecular Formula C25H26ClN5O3
Molecular Weight 479.959
Exact Mass 479.172424
PSA 106.27000
LogP 2.61
Index of Refraction 1.717
Storage condition -20℃

 Synthetic Route

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BMS-536924 Structure

BMS-536924

CAS#:468740-43-4

Literature: Wittman, Mark; Carboni, Joan; Attar, Ricardo; Balasubramanian, Balu; Balimane, Praveen; Brassil, Patrick; Beaulieu, Francis; Chang, Chiehying; Clarke, Wendy; Dell, Janet; Eummer, Jeffrey; Frennesson, David; Gottardis, Marco; Greer, Ann; Hansel, Steven; Hurlburt, Warren; Jacobson, Bruce; Krishnananthan, Subramaniam; Lee, Francis Y.; Li, Aixin; Lin, Tai-An; Liu, Peiying; Ouellet, Carl; Sang, Xiaopeng; Saulnier, Mark G.; Stoffan, Karen; Sun, Yax; Velaparthi, Upender; Wong, Henry; Yang, Zheng; Zimmermann, Kurt; Zoeckler, Mary; Vyas, Dolatrai Journal of Medicinal Chemistry, 2005 , vol. 48, # 18 p. 5639 - 5643

~%

BMS-536924 Structure

BMS-536924

CAS#:468740-43-4

Literature: Wittman, Mark; Carboni, Joan; Attar, Ricardo; Balasubramanian, Balu; Balimane, Praveen; Brassil, Patrick; Beaulieu, Francis; Chang, Chiehying; Clarke, Wendy; Dell, Janet; Eummer, Jeffrey; Frennesson, David; Gottardis, Marco; Greer, Ann; Hansel, Steven; Hurlburt, Warren; Jacobson, Bruce; Krishnananthan, Subramaniam; Lee, Francis Y.; Li, Aixin; Lin, Tai-An; Liu, Peiying; Ouellet, Carl; Sang, Xiaopeng; Saulnier, Mark G.; Stoffan, Karen; Sun, Yax; Velaparthi, Upender; Wong, Henry; Yang, Zheng; Zimmermann, Kurt; Zoeckler, Mary; Vyas, Dolatrai Journal of Medicinal Chemistry, 2005 , vol. 48, # 18 p. 5639 - 5643

~%

BMS-536924 Structure

BMS-536924

CAS#:468740-43-4

Literature: Wittman, Mark; Carboni, Joan; Attar, Ricardo; Balasubramanian, Balu; Balimane, Praveen; Brassil, Patrick; Beaulieu, Francis; Chang, Chiehying; Clarke, Wendy; Dell, Janet; Eummer, Jeffrey; Frennesson, David; Gottardis, Marco; Greer, Ann; Hansel, Steven; Hurlburt, Warren; Jacobson, Bruce; Krishnananthan, Subramaniam; Lee, Francis Y.; Li, Aixin; Lin, Tai-An; Liu, Peiying; Ouellet, Carl; Sang, Xiaopeng; Saulnier, Mark G.; Stoffan, Karen; Sun, Yax; Velaparthi, Upender; Wong, Henry; Yang, Zheng; Zimmermann, Kurt; Zoeckler, Mary; Vyas, Dolatrai Journal of Medicinal Chemistry, 2005 , vol. 48, # 18 p. 5639 - 5643

~%

BMS-536924 Structure

BMS-536924

CAS#:468740-43-4

Literature: Wittman, Mark; Carboni, Joan; Attar, Ricardo; Balasubramanian, Balu; Balimane, Praveen; Brassil, Patrick; Beaulieu, Francis; Chang, Chiehying; Clarke, Wendy; Dell, Janet; Eummer, Jeffrey; Frennesson, David; Gottardis, Marco; Greer, Ann; Hansel, Steven; Hurlburt, Warren; Jacobson, Bruce; Krishnananthan, Subramaniam; Lee, Francis Y.; Li, Aixin; Lin, Tai-An; Liu, Peiying; Ouellet, Carl; Sang, Xiaopeng; Saulnier, Mark G.; Stoffan, Karen; Sun, Yax; Velaparthi, Upender; Wong, Henry; Yang, Zheng; Zimmermann, Kurt; Zoeckler, Mary; Vyas, Dolatrai Journal of Medicinal Chemistry, 2005 , vol. 48, # 18 p. 5639 - 5643

 Synonyms

CDK inhibitor
4-{[(2S)-2-(3-chlorophenyl)-2-hydroxyethyl]amino}-3-[4-methyl-6-(morpholin-4-yl)-1H-benzimidazol-2-yl]pyridin-2(1H)-one
4-{[(2S)-2-(3-Chlorophenyl)-2-hydroxyethyl]amino}-3-[4-methyl-6-(4-morpholinyl)-1H-benzimidazol-2-yl]-2(1H)-pyridinone
CHEMBL401930
4-[[(2S)-2-(3-CHLOROPHENYL)-2-HYDROXYETHYL]AMINO]-3-[7-METHYL-5-(4-MORPHOLINYL)-1H-BENZIMIDAZOL-2-YL]-2(1H)-PYRIDINONE
2(1H)-Pyridinone, 4-[[(2S)-2-(3-chlorophenyl)-2-hydroxyethyl]amino]-3-[4-methyl-6-(4-morpholinyl)-1H-benzimidazol-2-yl]-
INSULIN-LIKE GROWTH FACTOR-1 RECEPTOR INHIBITOR
BMS-536924
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