solo para uso en investigación
Alvespimycin (17-DMAG) Hydrochloride HSP Inhibidor
Cat. No.: S1142
Estructura química
Peso molecular: 653.21
Control de calidad (Quality Control)
Cultivo celular, tratamiento y concentración de trabajo
(Cell Culture, Treatment & Working Concentration)
| Líneas celulares | Tipo de ensayo | Concentración | Tiempo de incubación | Formulación | Descripción de la actividad | PMID |
|---|---|---|---|---|---|---|
| MDA-MB-231 | Function assay | Inhibition of Hsp90 in human MDA-MB-231 cells assessed as her2 degradation, IC50=0.0045μM. | 18929486 | |||
| A2058 | Cytotoxicity assay | Cytotoxicity against human A2058 cells by MTT assay, IC50=0.0021μM. | 18929486 | |||
| AGS | Cytotoxicity assay | Cytotoxicity against human AGS cells by MTT assay, IC50=16μM. | 18359631 | |||
| HeLa | Cytotoxicity assay | Cytotoxicity against human HeLa cells by MTT assay, IC50=2.06μM. | 18359631 | |||
| HeLa | Function assay | Inhibition of TNF-alpha-induced NF-kappaB activation in human HeLa cells, IC50=0.15μM. | 18359631 | |||
| AGS | Function assay | Inhibition of hypoxia-induced HIF1 activation in human AGS cells by reporter gene assay, IC50=0.0036μM. | 18359631 | |||
| NCI-H526 | Function assay | 1 uM | 96 hrs | Inhibition of HSP90-mediated proliferation of human NCI-H526 cells at 1 uM after 96 hrs by sulforhodamine B assay | 17603540 | |
| NCI-H526 | Function assay | 1 uM | 24 hrs | Binding affinity to HSP90 in human NCI-H526 cells at 1 uM after 24 hrs by fluorescence polarization assay | 17603540 | |
| AGS | Function assay | 24 hrs | Viability of human AGS cells under normoxic conditions after 24 hrs by MTT assay, IC50=16μM. | 17583950 | ||
| Hep3B | Function assay | 16 hrs | Inhibition of HIF1 activation in human Hep3B cells assessed as inhibition of hypoxia-induced luciferase expression after 16 hrs by reporter assay, IC50=0.061μM. | 17583950 | ||
| AGS | Function assay | 16 hrs | Inhibition of HIF1 activation in human AGS cells assessed as inhibition of hypoxia-induced luciferase expression after 16 hrs by reporter assay, IC50=0.036μM. | 17583950 | ||
| SKOV3 | Function assay | Degradation of Her2 in SKOV3 cells, EC50=0.046μM. | 16854066 | |||
| SKOV3 | Function assay | Upregulation of Hsp70 in SKOV3 cells, EC50=0.014μM. | 16854066 | |||
| SKBR3 | Function assay | Degradation of Her2 in SKBR3 cells, EC50=0.008μM. | 16854066 | |||
| SKBR3 | Function assay | Upregulation of Hsp70 in SKBR3 cells, EC50=0.004μM. | 16854066 | |||
| SKBr3 | Cytotoxicity assay | Cytotoxicity against SKBr3 cells, IC50=0.024μM. | 16165354 | |||
| MDA-MB-231 | Cytotoxicity assay | Cytotoxicity against human MDA-MB-231 cells by MTT assay, IC50=0.0058μM. | 18929486 | |||
| A2058 | Function assay | Inhibition of Hsp90 in human A2058 cells, EC50=0.0079μM. | 18929486 | |||
| MDA-MB-231 | Function assay | Inhibition of Hsp90 in human MDA-MB-231 cells assessed as Akt degradation, IC50=0.0176μM. | 18929486 | |||
| A2058 | Function assay | Inhibition of Hsp90 in human A2058 cells assessed as Akt degradation, IC50=0.0243μM. | 18929486 | |||
| HuH7 | Antiviral assay | 3 days | Antiviral activity against Hepatitis C virus genotype 1b Con1 infected in human HuH7 cells assessed as GAPDH RNA or 18S rRNA level after 3 days by qRT-PCR analysis, EC50=0.0012μM. | 18936191 | ||
| HuH7 | Antiviral assay | 3 days | Antiviral activity against Hepatitis C virus genotype 1b Con1 infected in human HuH7 cells assessed as GAPDH RNA or 18S rRNA level after 3 days selected with 40 nM HCV-796 and 800 nM boceprevir by qRT-PCR analysis, EC50=0.0031μM. | 18936191 | ||
| SKBR3 | Function assay | Binding affinity to Hsp90 in human SKBR3 cells, IC50=0.024μM. | 19017562 | |||
| Hep3B | Function assay | 30 mins | Inhibition of hypoxia-induced HIF1alpha protein accumulation in human Hep3B cells treated for 30 mins measured after 12 hrs by Western blot analysis, IC50=0.0572μM. | 19072214 | ||
| Hep3B | Function assay | 16 hrs | Inhibition of hypoxia-induced VEGF protein secretion in human Hep3B cells after 16 hrs by ELISA, IC50=0.0795μM. | 19072214 | ||
| HCT116 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human HCT116 cells after 72 hrs, IC50=0.057μM. | 19231864 | ||
| SKBR3 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human SKBR3 cells after 72 hrs, IC50=0.058μM. | 19231864 | ||
| MCF7 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human MCF7 cells after 72 hrs, IC50=0.071μM. | 19231864 | ||
| SKOV3 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human SKOV3 cells after 72 hrs, IC50=0.122μM. | 19231864 | ||
| SKBR3 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human SKBR3 cells after 72 hrs in presence of NQO1 inhibitor dicoumarol, IC50=0.23μM. | 19231864 | ||
| MCF7 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human MCF7 cells after 72 hrs in presence of NQO1 inhibitor dicoumarol, IC50=0.862μM. | 19231864 | ||
| NCI-H596 | Cytotoxicity assay | 72 hrs | Cytotoxicity against NQ01-deficient human NCI-H596 cells after 72 hrs, IC50=1.1μM. | 19231864 | ||
| MDA468 | Cytotoxicity assay | 72 hrs | Cytotoxicity against NQ01-deficient human MDA468 cells after 72 hrs, IC50=1.6μM. | 19231864 | ||
| SKBR3 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human SKBR3 cells after 72 hrs by celltiter-glo assay, IC50=0.024μM. | 19405528 | ||
| A549 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human A549 cells after 72 hrs by celltiter-glo assay, IC50=0.068μM. | 19405528 | ||
| SKOV3 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human SKOV3 cells after 72 hrs by celltiter-glo assay, IC50=0.22μM. | 19405528 | ||
| MCF7 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human MCF7 cells after 72 hrs by celltiter-glo assay, IC50=0.23μM. | 19405528 | ||
| CCRF-CEM | Cytotoxicity assay | 72 hrs | Cytotoxicity against human CCRF-CEM cells after 72 hrs by celltiter-96 aqueous one solution assay, IC50=0.54μM. | 19405528 | ||
| CCRF-CEM | Cytotoxicity assay | 72 hrs | Cytotoxicity against human paclitaxel-resistant CCRF-CEM cells after 72 hrs by celltiter-96 aqueous one solution assay, IC50=2.5μM. | 19405528 | ||
| Hep3B | Function assay | 30 mins | Inhibition of hypoxia-induced HIF1alpha protein accumulation in human Hep3B cells treated for 30 mins measured after 12 hrs by Western blot analysis, IC50=0.057μM. | 20469887 | ||
| Hep3B | Function assay | 16 hrs | Inhibition of hypoxia-induced VEGF protein secretion in human Hep3B cells after 16 hrs by ELISA, IC50=0.079μM. | 20469887 | ||
| HCT116 | Cytotoxicity assay | Cytotoxicity against human HCT116 cells by Alamar blue assay, IC50=0.05μM. | 20662534 | |||
| NCI-H1299 | Function assay | 24 hrs | Inhibition of human HSP90 in human NCI-H1299 cells assessed as Akt degradation after 24 hrs by luminex assay, IC50=0.1μM. | 21438541 | ||
| LN229-Lux | Function assay | 2.5 to 10 uM | 1 hr | Inhibition of luciferase activity in human LN229-Lux cells at 2.5 to 10 uM incubated for 1 hr under normoxia followed by 24 hrs under hypoxia by reporter gene assay | 22746274 | |
| MCF7 | Antiproliferative assay | 48 hrs | Antiproliferative activity against human MCF7 cells assessed as inhibition of cell viability after 48 hrs by MTT assay, IC50=0.39μM. | 24582477 | ||
| HCT116 | Antiproliferative assay | 48 hrs | Antiproliferative activity against human HCT116 cells assessed as inhibition of cell viability after 48 hrs by MTT assay, IC50=0.78μM. | 24582477 | ||
| SKBR3 | Antiproliferative assay | 48 hrs | Antiproliferative activity against human SKBR3 cells assessed as inhibition of cell viability after 48 hrs by MTT assay, IC50=1.34μM. | 24582477 | ||
| A231 | Antiproliferative assay | 48 hrs | Antiproliferative activity against human A231 cells after 48 hrs by MTT assay, IC50=0.17μM. | 24763261 | ||
| MCF7 | Antiproliferative assay | 48 hrs | Antiproliferative activity against human MCF7 cells after 48 hrs by MTT assay, IC50=0.8μM. | 24763261 | ||
| HCT116 | Antiproliferative assay | 48 hrs | Antiproliferative activity against human HCT116 cells after 48 hrs by MTT assay, IC50=1.21μM. | 24763261 | ||
| SKBR3 | Antiproliferative assay | 48 hrs | Antiproliferative activity against human SKBR3 cells after 48 hrs by MTT assay, IC50=3.11μM. | 24763261 | ||
| NCI-H1299 | Function assay | 12 hrs | Reduction in oxygen consumption rate in human NCI-H1299 cells incubated for 12 hrs | 25383915 | ||
| PC9 | Cytotoxicity assay | 72 hrs | Cytotoxicity against HGF-induced erlotinib-resistant human PC9 cells assessed as inhibition of cell growth after 72 hrs by MTT assay, IC50=0.01μM. | 26844689 | ||
| Ma1 | Cytotoxicity assay | 72 hrs | Cytotoxicity against HGF-induced erlotinib-resistant human Ma1 cells assessed as inhibition of cell growth after 72 hrs by MTT assay, IC50=0.01μM. | 26844689 | ||
| SKBR3 | Function assay | Inhibition of Hsp90 in human SKBR3 cells, IC50=0.024μM. | 26844689 | |||
| HeLa | Function assay | 10 uM | 6 hrs | Inhibition of HSP90 in human HeLa cells assessed as induction of chk1 degradation at 10 uM after 6 hrs by Western blot method | 28816449 | |
| HeLa | Function assay | 10 uM | 6 hrs | Inhibition of HSP90 in human HeLa cells assessed as induction of Akt degradation at 10 uM after 6 hrs by Western blot method | 28816449 | |
| HeLa | Function assay | 10 uM | 6 hrs | Inhibition of HSP90 in human HeLa cells assessed as induction of HSP70 protein expression at 10 uM after 6 hrs by Western blot method | 28816449 | |
| PC3 | Function assay | 10 uM | 6 hrs | Inhibition of HSP90 in human PC3 cells assessed as induction of chk1 degradation at 10 uM after 6 hrs by Western blot method | 28816449 | |
| PC3 | Function assay | 10 uM | 6 hrs | Inhibition of HSP90 in human PC3 cells assessed as induction of Akt degradation at 10 uM after 6 hrs by Western blot method | 28816449 | |
| PC3 | Function assay | 10 uM | 6 hrs | Inhibition of HSP90 in human PC3 cells assessed as induction of HSP70 protein expression at 10 uM after 6 hrs by Western blot method | 28816449 | |
| Haga clic para ver más datos experimentales de líneas celulares | ||||||
Información química, almacenamiento y estabilidad (Chemical Information, Storage & Stability)
| Peso molecular | 653.21 | Fórmula | C32H48N4O8•HCl |
Almacenamiento (Desde la fecha de recepción) | |
|---|---|---|---|---|---|
| Nº CAS | 467214-21-7 | Descargar SDF | Almacenamiento de soluciones madre |
|
|
| Sinónimos | NSC 707545,BMS 826476 HCl,KOS 1022 | Smiles | CC1CC(C(C(C=C(C(C(C=CC=C(C(=O)NC2=CC(=O)C(=C(C1)C2=O)NCCN(C)C)C)OC)OC(=O)N)C)C)O)OC.Cl | ||
Solubilidad (Solubility)
|
In vitro |
DMSO
: 100 mg/mL
(153.09 mM)
Water : Insoluble Ethanol : Insoluble |
Calculadora de Molaridad
|
In vivo |
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Calculadora de formulación in vivo (Solución clara)
Paso 1: Introduzca la información a continuación (Recomendado: Un animal adicional para tener en cuenta la pérdida durante el experimento)
Paso 2: Introduzca la formulación in vivo (Esto es solo la calculadora, no la formulación. Por favor, contáctenos primero si no hay una formulación in vivo en la sección de Solubilidad.)
Resultados del cálculo:
Concentración de trabajo: mg/ml;
Método para preparar el líquido maestro de DMSO: mg fármaco predissuelto en μL DMSO ( Concentración del líquido maestro mg/mL, Por favor, contáctenos primero si la concentración excede la solubilidad del DMSO del lote del fármaco. )
Método para preparar la formulación in vivo: Tomar μL DMSO líquido maestro, luego añadirμL PEG300, mezclar y clarificar, luego añadirμL Tween 80, mezclar y clarificar, luego añadir μL ddH2O, mezclar y clarificar.
Método para preparar la formulación in vivo: Tomar μL DMSO líquido maestro, luego añadir μL Aceite de maíz, mezclar y clarificar.
Nota: 1. Por favor, asegúrese de que el líquido esté claro antes de añadir el siguiente disolvente.
2. Asegúrese de añadir el (los) disolvente(s) en orden. Debe asegurarse de que la solución obtenida, en la adición anterior, sea una solución clara antes de proceder a añadir el siguiente disolvente. Se pueden utilizar métodos físicos como el vórtice, el ultrasonido o el baño de agua caliente para ayudar a la disolución.
Mecanismo de acción (Mechanism of Action)
| Características |
A synthetic derivative Geldanamycin, with lower hepatotoxicity than parent antibiotic & higher potency and bioavailability than the similar derivative 17-AAG.
|
|---|---|
| Targets/IC50/Ki |
HSP90
(Cell-free assay) 62 nM
|
| In vitro |
El 17-DMAG muestra una potencia ~2 veces mayor contra la Hsp90 humana que el 17-AAG, con una IC50 de 62 nM frente a 119 nM. En células SKBR3 y SKOV3 que sobreexpresan la proteína cliente de Hsp90 Her2, el 17-DMAG causa una regulación a la baja de Her2 con EC50 de 8 nM y 46 nM, respectivamente, así como la inducción de Hsp70 con EC50 de 4 nM y 14 nM, respectivamente, lo que lleva a una citotoxicidad significativa con GI50 de 29 nM y 32 nM, respectivamente, consistente con la inhibición de Hsp90. El 17-DMAG en combinación con vorinostat induce sinérgicamente la apoptosis de las células de LCM cultivadas, así como de las células de LCM primarias, con mayor potencia que cualquiera de los agentes por separado, al atenuar marcadamente los niveles de ciclina D1 y CDK4, así como de c-Myc, c-RAF y Akt. A diferencia del 17-AAG, que solo es activo para IKKβ en las células de leucemia linfocítica crónica (LLC), el tratamiento con 17-DMAG conduce eficazmente al agotamiento de la proteína cliente de Hsp90, lo que resulta en una disminución de la unión al ADN de NF-κB p50/p65, una disminución de la transcripción del gen diana de NF-κB y la apoptosis dependiente de caspasas. Al dirigirse a la familia NF-κB, el 17-DMAG media selectivamente la citotoxicidad dependiente de la dosis y el tiempo contra las células de LLC, pero no contra las células T normales o las células NK importantes para la vigilancia inmunitaria. |
| Ensayo de quinasa |
Ensayo de unión competitiva basado en polarización de fluorescencia (FP)
|
|
Este ensayo utiliza un análogo de geldanamicina marcado con difluoruro de boro dipirrometeno (BODIPY-AG) como sonda y mide la polarización de fluorescencia tras la unión de la sonda a una proteína. La proteína Hsp90 humana nativa (isoformas α + β) se aísla de células HeLa. La solución de BODIPY-AG se prepara fresca en tampón de ensayo FP (20 mM HEPES-KOH, pH 7,3, 1,0 mM EDTA, 100 mM KCl, 5,0 mM MgCl2, 0,01% NP-40, 0,1 mg/mL de γ-globulina bovina (BGG) fresca, 1,0 mM de DTT fresco y un inhibidor de proteasa de una solución madre en DMSO. Las curvas de competencia se obtienen mezclando 10 μL de cada una de las soluciones que contienen BODIPY-AG y Hsp90, y una dilución en serie de 17-DMAG recién preparada en tampón de ensayo FP a partir de una solución madre en DMSO. Las concentraciones finales son 10 nM BODIPY-AG, 40 o 60 nM Hsp90, concentración variable de 17-DMAG (0,10 nM-10 μM) y ≤0,25% de DMSO en una microplaca de 384 pocillos. Después de 3 horas de incubación a 30 °C, la anisotropía de fluorescencia (γEx = 485 nm, γEm = 535 nm) se mide en un lector de placas multietiqueta EnVision 2100. El valor de IC50 de 17-DMAG se obtiene de las curvas de competencia.
|
|
| In vivo |
El tratamiento con 17-DMAG a 5 mg/kg o 25 mg/kg tres veces por semana reduce significativamente el crecimiento tumoral de los xenoinjertos TMK-1, al reducir significativamente el área vascular y el número de células tumorales proliferantes en las secciones. De acuerdo con la inhibición de la señalización de FAK in vivo, el tratamiento con 17-DMAG a 25 mg/kg tres veces por semana suprime significativamente el crecimiento tumoral y la metástasis de los xenoinjertos ME180 y SiHa en ratones. La administración de 17-DMAG a 10 mg/kg durante 16 días disminuye significativamente el recuento de glóbulos blancos y prolonga la supervivencia en un modelo de ratón de trasplante TCL1-SCID. |
Referencias |
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Aplicaciones (Applications)
| Métodos | Biomarcadores | Imágenes | PMID |
|---|---|---|---|
| Western blot | HSP90 / HSP70 p-Akt / Survivin / MMP2 PARP / Cleaved caspase-3 / Cleaved caspase-8 / Cleaved caspase-9 / PUMA p-ALK / ALK / p-Akt / Akt / p-ERK / ERK α-Tax / α-IKKα / α-IKKβ/ α-NEMO / α-TBK1 / α-p65 / α-p50 |
|
28915605 |
| Growth inhibition assay | Cell proliferation |
|
28915605 |
Información del ensayo clínico (Clinical Trial Information)
(datos de https://clinicaltrials.gov, actualizado el 2024-05-22)
| Número NCT | Reclutamiento | Condiciones | Patrocinador/Colaboradores | Fecha de inicio | Fases |
|---|---|---|---|---|---|
| NCT00780000 | Terminated | Breast Cancer |
Bristol-Myers Squibb |
April 2008 | Phase 2 |
| NCT00248521 | Unknown status | Unspecified Adult Solid Tumor Protocol Specific |
Institute of Cancer Research United Kingdom|National Cancer Institute (NCI) |
October 2005 | Phase 1 |
Los productos son solo para uso de investigación. No para uso humano. No vendemos a pacientes.
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