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05-374

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Anti-Cyclin A (human), clone BF683
Tipo de documento:

Certificado de análisis
Número de lote:

2477862

Referencia del producto:

05-374
Anti-Cyclin A (human), clone BF683 - DAM1518953
Tipo de documento:

Certificado de análisis
Número de lote:

DAM1518953

Referencia del producto:

05-374
Anti-Cyclin A, clone BF 683 - 22690
Tipo de documento:

Certificado de análisis
Número de lote:

22690

Referencia del producto:

05-374
Anti-Cyclin A, clone BF 683 - 14686
Tipo de documento:

Certificado de análisis
Número de lote:

14686

Referencia del producto:

05-374
Certificate of Analysis 05-59-0537_A34337
Tipo de documento:

Certificado de análisis
Número de lote:

A34337

Referencia del producto:

05-59-0537
Preclinical activity of ABT-869, a multitargeted receptor tyrosine kinase inhibitor.
ABT-869 is a structurally novel, receptor tyrosine kinase (RTK) inhibitor that is a potent inhibitor of members of the vascular endothelial growth factor (VEGF) and platelet-derived growth factor (PDGF) receptor families (e.g., KDR IC50 = 4 nmol/L) but has much less activity (IC50s greater than 1 micromol/L) against unrelated RTKs, soluble tyrosine kinases, or serine/threonine kinases. The inhibition profile of ABT-869 is evident in cellular assays of RTK phosphorylation (IC50 = 2, 4, and 7 nmol/L for PDGFR-beta, KDR, and CSF-1R, respectively) and VEGF-stimulated proliferation (IC50 = 0.2 nmol/L for human endothelial cells). ABT-869 is not a general antiproliferative agent because, in most cancer cells, greater than 1,000-fold higher concentrations of ABT-869 are required for inhibition of proliferation. However, ABT-869 exhibits potent antiproliferative and apoptotic effects on cancer cells whose proliferation is dependent on mutant kinases, such as FLT3. In vivo ABT-869 is effective orally in the mechanism-based murine models of VEGF-induced uterine edema (ED50 = 0.5 mg/kg) and corneal angiogenesis (greater than 50% inhibition, 15 mg/kg). In tumor growth studies, ABT-869 exhibits efficacy in human fibrosarcoma and breast, colon, and small cell lung carcinoma xenograft models (ED50 = 1.5-5 mg/kg, twice daily) and is also effective (greater than 50% inhibition) in orthotopic breast and glioma models. Reduction in tumor size and tumor regression was observed in epidermoid carcinoma and leukemia xenograft models, respectively. In combination, ABT-869 produced at least additive effects when given with cytotoxic therapies. Based on pharmacokinetic analysis from tumor growth studies, efficacy correlated more strongly with time over a threshold value (cellular KDR IC50 corrected for plasma protein binding = 0.08 microg/mL, greater than or=7 hours) than with plasma area under the curve or Cmax. These results support clinical assessment of ABT-869 as a therapeutic agent for cancer.
Tipo de documento:

Referencia

Referencia del producto:

Múltiplo
Nombre del producto:

Múltiplo
Certificate of Analysis 053474 U11106974W
Tipo de documento:

Certificado de análisis
Número de lote:

U11106974W

Referencia del producto:

053474
Certificate of Analysis 053474 U11052774W
Tipo de documento:

Certificado de análisis
Número de lote:

U11052774W

Referencia del producto:

053474
Certificate of Analysis 053474 U130117W74
Tipo de documento:

Certificado de análisis
Número de lote:

U130117W74

Referencia del producto:

053474
Certificate of Analysis 053474 U11132474W
Tipo de documento:

Certificado de análisis
Número de lote:

U11132474W

Referencia del producto:

053474