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10mM in DMSO for sensitive chromatographic and analytical workflows requiring minimal baseline interference.
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Cited in 0 peer-reviewed publications across chromatography, organic synthesis, and cross-coupling reactions.
SOS1-IN-14 is a potent, selective and orally active SOS1 inhibitor with an IC 50 value of 3.9 nM. SOS1-IN-14 can be absorbed in the intestine via a P-glycoprotein-mediated efflux mechanism. SOS1-IN-14 can be used to research KRAS-mutated cancers. SOS1-IN-14 has better potent tumor suppression than BI-3406
In Vitro
SOS1-IN-14 (compound 13c) exhibits cellular SOS1 inhibition with an IC 50 of 21 nM. SOS1-IN-14 has certain inhibition for CYP2D6, CYP2C9, CYP2C8 and CYP3A4 with IC 50 s of 2.5 μM, 6.5 μM, 43.3 μM and 54.3 μM, respectively, indicating that it has a certain risk of drug-drug interaction. MCE has not independently confirmed the accuracy of these methods. They are for reference only.
In Vivo
SOS1-IN-14 (50 mg/kg; p.o.; qd) exhibits 83.0% tumor suppression in Mia-paca-2 pancreas xenograft mice tumor models . SOS1-IN-14 shows a favorable pharmacokinetic profile with a bioavailability of 86.8% in beagles . Pharmacokinetic Parameters of SOS1-IN-14 (compound 13c) in ICR mice, Sprague-Dawley rats and Beagle dogs . ICR Mice Sprague–Dawley Rats Beagle Dogs Administration p.o., 50 mg/kg i.v., 2 mg/kg p.o., 10 mg/kg i.v., 2 mg/kg p.o., 20 mg/kg T max (h) 0.5 0.08 3 0.08 2 T 1/2 (h) 4.61 1.17 2.32 3.83 6.68 C max (μg/mL) 2670 1261 265 568 1840 AUC 0-24 (ng/mL·h) 32300 970 1683 2962 25725 CL (mL/min/kg) / 2068 / 11.3 / V ss (L/kg) / 2126 / 3.88 / F (%) / / 34.5 / 86.8 K el (h -1 ) 0.265 / / / / MRT (h) 4.67 / / / / MCE has not independently confirmed the accuracy of these methods. They are for reference only. Animal Model: BALB/c nude mice (KRAS G12C variant Mia-paca-2 xenograft models) Dosage: 50 mg/kg Administration: p.o.; q.d., for 21 days Result: Exhibited 83.0% tumor suppression. Showed better potent tumor suppression than BI-3406 .
IC50& Target:IC 50 : 3.9 nM (SOS1)
| Peso molecular | 550.57 |
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