HM30181

"目录号: HY-13646

Membrane Transporter/Ion Channel-

HM30181是一种有效的选择性的P-glycoprotein抑制剂。

P-glycoprotein

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生物活性

Description

HM30181 is a potent and selective inhibitor ofP-glycoprotein.

In Vitro

HM30181 is shown to be approximately equipotent with the reference Pgp inhibitor tariquidar in inhibiting rhodamine 123 efflux from CCRF-CEM T cells (IC50, tariquidar: 8.2±2.0 nM, HM30181: 13.1±2.3 nM)[1]. HM30181 shows a high selectivity for mP-gp and its potency is 20-50 times higher than that of tariquitar, another third generation P-gp inhibitor[2].

In Vivo

PET scans with the Pgp substrate (R)-[11C]verapamil in FVB wild-type mice pretreated i.v. with HM30181 (10 or 21 mg/kg) failes to show significant increases in (R)-[11C]verapamil brain uptake compared with vehicle treated animals[1]. HM30181 inhibits P-gp mainly in the intestinal endothelium, which can be beneficial because pan-inhibition of P-gp, particularly in the brain, could lead to detrimental adverse events. HM30181 increases the oral bioavailability of co-administered paclitaxel by more than 12 times in rats[2].

Clinical Trial

NCT00954304

Hanmi Pharmaceutical Company Limited

Healthy

June 2009

Phase 1

NCT00986843

Hanmi Pharmaceutical Company Limited

Advanced Solid Malignancies

June 2008

Phase 1

NCT00979563

Hanmi Pharmaceutical Company Limited

Advanced Solid Malignancies

July 2008

Phase 1

NCT01491204

Hanmi Pharmaceutical Company Limited

Advanced Solid Tumors

August 2006

Phase 1

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References

[1].Bauer F, et al. Interaction of HM30181 with P-glycoprotein at the murine blood-brain barrier assessed with positron emission tomography. Eur J Pharmacol. 2012 Dec 5;696(1-3):18-27.

[2].Kim TE, et al. Effects of HM30181, a P-glycoprotein inhibitor, on the pharmacokinetics and pharmacodynamics of loperamide in healthy volunteers. Br J Clin Pharmacol. 2014 Sep;78(3):556-64.

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