FGTI-2734( —— )

Catalog No. M26215 CAS No. 1247018-19-4

FGTI-2734 can prevent membrane localization of KRAS, hence solving KRAS resistance problem and thwarting mutant KRAS patient-derived pancreatic tumors.

Purity : >98% (HPLC)

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Size	Price / USD	Stock	Quantity
1 mL x 10 mM in DMSO	131	In Stock
5MG	116	In Stock
10MG	188	In Stock
25MG	392	In Stock
50MG	575	In Stock
100MG	817	In Stock
200MG	Get Quote	In Stock
500MG	Get Quote	In Stock
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Biological Information

Product Name

FGTI-2734
Note

Research use only, not for human use.
Brief Description

FGTI-2734 can prevent membrane localization of KRAS, hence solving KRAS resistance problem and thwarting mutant KRAS patient-derived pancreatic tumors.
Description

FGTI-2734 can prevent membrane localization of KRAS, hence solving KRAS resistance problem and thwarting mutant KRAS patient-derived pancreatic tumors. FGTI-2734 is a RAS C-terminal mimetic dual farnesyl transferase (FT) and geranylgeranyl transferase-1 (GGT-1) inhibitor with IC50s of 250 nM and 520 nM for FT and GGT-1, respectively.(In Vitro):FGTI-2734 (3-30 μM; 72 hours) inhibits both protein prenylation of HDJ2, RAP1A, KRAS and NRAS. FGTI-2734 inhibits KRAS membrane localization in RAS-transformed murine NIH3T3 cells and in mutant KRAS human cancer cells. FGTI-2734 (1-30 μM; 72 hours) induces CASPASE-3 and PARP cleavage in MiaPaCa2, L3.6pl and Calu6 cells.(In Vivo):FGTI-2734 (100 mg/kg/daily for 18 to 25 days; i.p.) only inhibited tumor growth in mutant KRAS-dependent tumors but not in mutant KRAS-independent tumors.
In Vitro

FGTI-2734 (1-30 μM; 72 hours) induces CASPASE-3 and PARP cleavage in MiaPaCa2, L3.6pl and Calu6 cells. FGTI-2734 (3-30 μM; 72 hours) inhibits both protein prenylation of HDJ2, RAP1A, KRAS and NRAS. FGTI-2734 inhibits KRAS membrane localization in RAS-transformed murine NIH3T3 cells and in mutant KRAS human cancer cells. Apoptosis Analysis Cell Line:MiaPaCa2, L3.6pl and Calu6 cells Concentration:1, 3, 10, 30 μM Incubation Time:72 hours Result:Induced CASPASE-3 and PARP cleavage in MiaPaCa2, L3.6pl and Calu6 cells.Western Blot Analysis Cell Line:KRAS, HRAS, and NRAS-transformed NIH3T3 cells Concentration:3, 10, 30 μM Incubation Time:72 hours Result:Inhibited both protein prenylation of HDJ2, RAP1A, KRAS and NRAS.
In Vivo

FGTI-2734 (intraperitoneally; 100 mg/kg/daily for 18 to 25 days) only inhibits tumor growth in mutant KRAS-dependent tumors but not in mutant KRAS-independent tumors. Animal Model:Male SCID-bg mice following injection of MiaPaCa2, L3.6pl, Calu6, A549, H460 and DLD1 cancer cells.Dosage:100 mg/kg Administration:Intraperitoneally; daily; for 18 to 25 days Result:Inhibited tumor growth in mutant KRAS-dependent tumors.
Synonyms

——
Pathway

Metabolic Enzyme/Protease
Target

Transferase
Recptor

NMDA receptor
Research Area

——
Indication

——

Chemical Information

CAS Number

1247018-19-4
Formula Weight

510.63
Molecular Formula

C26H31FN6O2S
Purity

>98% (HPLC)
Solubility

In Vitro:?DMSO : 50 mg/mL (97.92 mM)
SMILES

Cn1cncc1CN(CCN(CC1CCCCC1)S(=O)(=O)c1ccccn1)c1ccc(cc1F)C#N
Chemical Name

——

Shipping & Storage Information

Storage

(-20℃)
Shipping

With Ice Pack
Stability

≥ 2 years

Reference

1.J Lehmann, et al. CGS 19755, a selective and competitive N-methyl-D-aspartate-type excitatory amino acid receptor antagonist. J Pharmacol Exp Ther. 1988 Jul;246(1):65-75.

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