達(dá)帕菲尼

Dabrafenib

	產(chǎn)品編號	CFN60005
	CAS編號	1195765-45-7
	分子式 = 分子量	C₂₃H₂₀F₃N₅O₂S₂ = 519.6
	產(chǎn)品價格	￥180/20mg(>=98%)
	物理屬性	Powder
	化合物類型	Alkaloids
	植物來源
ChemFaces的產(chǎn)品在影響因子大于5的優(yōu)秀和頂級科學(xué)期刊中被引用

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產(chǎn)品名稱	產(chǎn)品編號	CAS編號	包裝	QQ客服
達(dá)帕菲尼	CFN60005	1195765-45-7	1mg	QQ客服：3004468091
達(dá)帕菲尼	CFN60005	1195765-45-7	5mg	QQ客服：3004468091
達(dá)帕菲尼	CFN60005	1195765-45-7	10mg	QQ客服：3004468091
達(dá)帕菲尼	CFN60005	1195765-45-7	20mg	QQ客服：3004468091

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Description:

Dabrafenib (GSK2118436) is a mutant BRAFV600 specific inhibitor with IC50 of 0.7 nM in cell-free assays, with 7- and 9-fold less potency against B-Raf(wt) and c-Raf, respectively.

Targets:

BRAFV600 | c-Raf | PI3K | mTOR | MEK

In vivo:

Mol Cancer Ther,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.[Pubmed: 22389471]

Recent results from clinical trials with the BRAF inhibitors GSK2118436 (dabrafenib) and PLX4032 (vemurafenib) have shown encouraging response rates; however, the duration of response has been limited.
METHODS AND RESULTS:
To identify determinants of acquired resistance to GSK2118436 and strategies to overcome the resistance, we isolated GSK2118436 drug-resistant clones from the A375 BRAF(V600E) and the YUSIT1 BRAF(V600K) melanoma cell lines. These clones also showed reduced sensitivity to the allosteric mitogen-activated protein/extracellular signal-regulated kinase (MEK) inhibitor GSK1120212 (trametinib). Genetic characterization of these clones identified an in-frame deletion in MEK1 (MEK1(K59del)) or NRAS mutation (NRAS(Q61K) and/or NRAS(A146T)) with and without MEK1(P387S) in the BRAF(V600E) background and NRAS(Q61K) in the BRAF(V600K) background. Stable knockdown of NRAS with short hairpin RNA partially restored GSK2118436 sensitivity in mutant NRAS clones, whereas expression of NRAS(Q61K) or NRAS(A146T) in the A375 parental cells decreased sensitivity to GSK2118436. Similarly, expression of MEK1(K59del), but not MEK1(P387S), decreased sensitivity of A375 cells to GSK2118436. The combination of GSK2118436 and GSK1120212 effectively inhibited cell growth, decreased ERK phosphorylation, decreased cyclin D1 protein, and increased p27(kip1) protein in the resistant clones. Moreover, the combination of GSK2118436 or GSK1120212 with the phosphoinositide 3-kinase/mTOR inhibitor GSK2126458 enhanced cell growth inhibition and decreased S6 ribosomal protein phosphorylation in these clones.
CONCLUSIONS:
Our results show that NRAS and/or MEK mutations contribute to BRAF inhibitor resistance in vitro, and the combination of GSK2118436 and GSK1120212 overcomes this resistance. In addition, these resistant clones respond to the combination of GSK2126458 with GSK2118436 or GSK1120212. Clinical trials are ongoing or planned to test these combinations.

Molecular Cancer Therapeutics 8(Supplement 1):B88-B88.

A selective Raf kinase inhibitor induces cell death and tumor regression of human cancer cell lines encoding B-RafV600E mutation.[Reference: WebLink]

Activation of the Ras‐Raf‐MEK‐ERK pathway has been implicated in a large range of human cancers. Growth factor receptor stimulation by extracellular ligands activates Ras, which then sets in motion a signal transduction cascade through the Raf, MEK and ERK serine/threonine kinases. Mutation of the B‐Raf kinase constitutively activates MAPK signalling, thus bypassing the need for upstream stimuli. This has been genetically associated with several human cancers, especially occurrence of the B‐RafV600E mutant and its high prevalence in melanoma, colorectal carcinoma, ovarian cancer, papillary thyroid carcinoma, and cholangiocarcinoma. The ability to selectively and potently inhibit B‐Raf should provide a potential therapy for patients with mutant B‐Raf tumors, for which addictive dependency on this pathway is observed.
METHODS AND RESULTS:
We have identified a novel, potent, and selective Raf kinase inhibitor that is capable of inhibiting the kinase activity of wild‐type B‐Raf, B‐RafV600E and c‐Raf with IC50 values of 3.2, 0.8, and 5.0 nM, respectively. Kinase panel screening for over 270 kinases has indicated that this inhibitor is selective for Raf kinase, with ∼400 fold selectivity towards B‐Raf over 91% of the other kinases tested. Specific cellular inhibition of B‐RafV600E kinase by this inhibitor leads to decreased ERK phosphorylation and inhibition of cell proliferation by an initial arrest in the G1 phase of the cell cycle, followed by cell death. This inhibition is selective for cancer cells that specifically encode the mutation for B‐RafV600E.
CONCLUSIONS:
Oral compound administration inhibits the growth of B‐RafV600E mutant melanoma (A375P) and colon cancer (Colo205) human tumor xenografts, growing subcutaneously in immuno‐compromised mice. This cell‐specific B‐RafV600E inhibitor is currently being evaluated in a human Phase I clinical trial.

	1 mg	5 mg	10 mg	20 mg	25 mg
1 mM	1.9246 mL	9.6228 mL	19.2456 mL	38.4911 mL	48.1139 mL
5 mM	0.3849 mL	1.9246 mL	3.8491 mL	7.6982 mL	9.6228 mL
10 mM	0.1925 mL	0.9623 mL	1.9246 mL	3.8491 mL	4.8114 mL
50 mM	0.0385 mL	0.1925 mL	0.3849 mL	0.7698 mL	0.9623 mL
100 mM	0.0192 mL	0.0962 mL	0.1925 mL	0.3849 mL	0.4811 mL

產(chǎn)品名稱	產(chǎn)品編號	CAS編號	分子式 = 分子量	位單	聯(lián)系QQ
Clemomandshuricoside B; Clemomandshuricoside B	CFN95302	905294-48-6	C₂₂H₃₀O₁₃ = 502.2	10mg	QQ客服：3004468091
25-脫氫升麻醇 3-O-beta-D-木糖苷; 25-Anhydrocimigenol 3-O-beta-D-xyloside	CFN92522	181765-11-7	C₃₅H₅₄O₈ = 602.8	5mg	QQ客服：3004468088
6″-O-木糖黃豆黃苷; 6''-O-xylosyl-glycitin	CFN80151	231288-18-9	C₂₇H₃₀O₁₄ = 578.16	5mg	QQ客服：3004468087
傘花耳草苷; Corymboside	CFN95292	73543-87-0	C₂₆H₂₈O₁₄ = 564.5	10mg	QQ客服：3004468520

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Dabrafenib

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