Dabrafenib
Référence M1988-5mg
Conditionnement : 5mg
Marque : AbMole Bioscience
All AbMole products are for research use only, cannot be used for human consumption.
GSK2118436
Quality Control & Documentation
Biological Activity
Dabrafenib (GSK2118436A) is a potent ATP-competitive inhibitor of B-Raf, B-Raf V600E and c-Raf with IC50 of 3.2 nM, 0.8 nM and 5.0 nM, respectively. Dabrafenib is selective for Raf kinase, with 400 fold selectivity towards B-Raf over 91% of the other kinases tested. Dabrafenib (orally administrated) inhibits the growth of B-RafV600E mutant melanoma (A375P) and colon cancer (Colo205) human tumor xenografts, growing subcutaneously in immuno-compromised mice. GSK2118436 treatment results in no detectable negative impact on existing systemic immunity or the de novo generation of tumor-specific T cells. Dabrafenib (GSK2118436A) is currently in phase III clinical trial in patients with melanoma.
Product Citations
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Arch Pathol Lab Med. 2024 May 16.
Genetic Landscape and Its Prognostic Impact in Children With Langerhans Cell Histiocytosis
Dabrafenib purchased from AbMole -
Int J Mol Sci. 2021 Nov 4;22(21):11951.
BRAF and MEK Inhibitors Affect Dendritic-Cell Maturation and T-Cell Stimulation
Dabrafenib purchased from AbMole -
Int J Mol Sci. 2018 Jan 18;19(1) pii: E289.
BRAF and MEK Inhibitors Influence the Function of Reprogrammed T Cells: Consequences for Adoptive T-Cell Therapy
Dabrafenib purchased from AbMole -
Cell Rep. 2016 Jun 28;16(1):263-77.
BRAF(V600E) Kinase Domain Duplication Identified in Therapy-Refractory Melanoma Patient-Derived Xenografts.
Dabrafenib purchased from AbMole -
Journal of Cell Science. 2016 Jun 1;129(11):2261-72.
PAX5 interacts with RIP2 to promote NF-κB activation and drug-resistance in B-lymphoproliferative disorders.
Dabrafenib purchased from AbMole -
EMBO Mol Med. 2015 Jun 23;1104-18.
Intra- and inter-tumor heterogeneity in a vemurafenib-resistant melanoma patient and derived xenografts.
Dabrafenib purchased from AbMole -
Cell Rep. 2014 Nov 20;1375-86.
Parallel in vivo and in vitro melanoma RNAi dropout screens reveal synthetic lethality between hypoxia and DNA damage response inhibition.
Dabrafenib purchased from AbMole
Customer Product Validations & Biological Datas
Source | Int J Mol Sci (2018). Figure 5. GSK2118436A (AbMole BioScience, Houston, TX, USA) | |
Method | vitro experiments | |
Cell Lines | CAR-T cells | |
Concentrations | 1 μM | |
Incubation Time | 16 h | |
Results | CAR-T cells in the conditions without inhibitor, with DMSO solvent control, with Vem alone, Tram alone, Dabra alone, and the combination Dabra + Tram |
Source | Int J Mol Sci (2018). Figure 4. GSK2118436A (AbMole BioScience, Houston, TX, USA) | |
Method | vitro experiments | |
Cell Lines | CAR-T cells | |
Concentrations | 1 μM | |
Incubation Time | 16 h | |
Results | The presence of Vem alone, Tram alone,Cobi alone, Vem + Cobi, and Dabra + Tram, but not of Dabra alone seemed to reduce these quantities to approximately 50%. |
Source | Int J Mol Sci (2018). Figure 3. GSK2118436A (AbMole BioScience, Houston, TX, USA) | |
Method | vitro experiments | |
Cell Lines | CAR-T cells | |
Concentrations | 1 μM | |
Incubation Time | 16 h | |
Results | "The condition with Vem + Cobi was similarly inhibited as Vem alone, while the Dabra + Tram condition was significantly less inhibited" |
Source | Int J Mol Sci (2018). Figure 2. GSK2118436A (AbMole BioScience, Houston, TX, USA) | |
Method | vitro experiments | |
Cell Lines | CAR-T cells | |
Concentrations | 1 μM | |
Incubation Time | 16 h | |
Results | Dabra alone had a significantly weaker effect on CD25-upregulation than Vem alone, and the combination Dabra + Tram resulted in the mildest effects on CD25 upregulation |
Source | Journal of Cell Science (2016) . Figure 3. Dabrafenib (M1988, Abmole, Houston, TX) | |
Method | Cell apoptosis assay and western blot | |
Cell Lines | IM9 and RPMI8226 cells expressing PAX5 | |
Concentrations | 10 μM | |
Incubation Time | 30 h | |
Results | Similarly, the selective RIP2 inhibitor SB 203580, but not the RIP1 inhibitor Necrostatin-1 (Degterev et al., 2013) nor the RIP3 inhibitor Dabrafenib (Li et al., 2014), was able to significantly increase Bortezomib-induced apoptosis in IM9 andPAX5-expressing RPMI8226 cells (Fig. 3D). Furthermore, only SB 203580 decreased Bortezomib-induced activation of RIP2 and NF-κB in IM9 cells (Fig. 3F). |
Source | Cell Report (2016). Figure 7.dabrafenib (GSK2118436, Abmole) | |
Method | Tumour volume and Immunoblotting | |
Cell Lines | ||
Concentrations | 30 mg/kg | |
Incubation Time | 25~30 days | |
Results | BRAFV600E/DK is Responsible for Resistance to BRAFi.Both PDXs were treated either with the BRAF inhibitor dabrafenib, to which they were completely resistant (Figures 7G and 7H). Indeed, AKT signaling was much more active in the M048R2.X2 PDX (Figure 7I), explaining its only partial sensitivity to LY3009120. |
Source | Cell Report (2016). Figure 3.dabrafenib (GSK2118436, Abmole) | |
Method | Immunoblotting and qPCR | |
Cell Lines | ||
Concentrations | 30 mg/kg | |
Incubation Time | 25~30 days | |
Results | These results demonstrate concordance between drug responses in patients and their corresponding PDXs, and they illustrate that the therapy response can be either stable or dynamic. |
Source | Cell Report (2014) . Figure 7.Dabrafenib (Abmole) | |
Method | In Vivo Experiments | |
Cell Lines | M026R.X1 tumors | |
Concentrations | 30mg/kg | |
Incubation Time | 33 days | |
Results | Synthetic lethality by hypoxia induction and Chek1/2 inhibition in vivo was observed for the PDX derived from a melanoma patient who had acquired resistance to BRAF inhibition. |
Source | EMBO Molecular Medicine (2015) . Figure 4.Dabrafenib (GSK2118436, Abmole) | |
Method | Mice--Derived Xenografts | |
Cell Lines | A375 cells infected with pQXCIPGFP, MEK1WT, and MEK1T55delinsRT | |
Concentrations | 30 mg/kg daily by oral gavage | |
Incubation Time | 12 days | |
Results | Altogether, these data confirm that MEK1T55delinsRT confers resistance to BRAF inhibition in vivo and induces local invasion. |
Source | EMBO Molecular Medicine (2015) . Figure 4.Dabrafenib (GSK2118436, Abmole) | |
Method | CellTiter-Blue Cell Viability Assay (G8081, Promega) | |
Cell Lines | A375-GFP, 888Mel-MEK1T55delinsRT,SK-MEL-28 | |
Concentrations | 0, 0.25, 0.5, 1, 2.5, 5 µ M | |
Incubation Time | 5 days | |
Results | MEK1T55delinsRT-expressing cells were also more resistant to low levels of the ERK inhibitor SCH772984 than control populations (Fig 4F and G). |
Protocol (for reference only)
Cell Experiment | |
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Cell lines | A375-GFP, 888Mel-MEK1T55delinsRT,SK-MEL-28 |
Preparation method | Dose–response curves were performed as follows: 3,000–6,000 cells were plated per well in a 96-well plate. For each condition, triplicates were plated. The next day, drug was added to the wells. At day 5 of the assay, medium-containing drug was removed and survival was measured by CellTiter-Blue Cell Viability Assay (G8081, Promega). |
Concentrations | 0, 0.25, 0.5, 1, 2.5, 5 µ M |
Incubation time | 5 Days |
Animal Experiment | |
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Animal models | A375 cells infected with pQXCIPGFP, MEK1WT, and MEK1T55delinsRT Mice--Derived Xenografts |
Formulation | Dabrafenib powder was first dissolved in DMSO and consequently, before injection, dissolved in 0.5% hydroxypropylmethylcellulose (Sigma-Aldrich), 0.2% Tween-80 in pH 8.0 distilled H2O. |
Dosages | 30 mg/kg daily (6 days per week) |
Administration | oral gavage |
Chemical Information
Molecular Weight | 519.56 |
Formula | C23H20F3N5O2S2 |
CAS Number | 1195765-45-7 |
Solubility (25°C) | DMSO 30 mg/mL |
Storage | Powder -20°C 3 years ; 4°C 2 years In solvent -80°C 6 months ; -20°C 1 month |
References
[1] Greger JG, et al. Mol Cancer Ther. Combinations of BRAF, MEK, and PI3K/mTOR inhibitors overcome acquired resistance to the BRAF inhibitor GSK2118436 dabrafenib, mediated by NRAS or MEK mutations.
[2] Hong DS, et al. Clin Cancer Res. BRAF(V600) inhibitor GSK2118436 targeted inhibition of mutant BRAF in cancer patients does not impair overall immune competency.