Ciclopirox (olamine)


CAS No. : 41621-49-2

(Synonyms: Ciclopirox (ethanolamine); HOE 296)

41621-49-2
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Cat. No. : HY-B0450A
M.Wt: 268.35
Formula: C14H24N2O3
Purity: >98 %
Solubility: DMSO : 25 mg/mL (ultrasonic;warming;heat to 60°C)
Introduction of 41621-49-2 :

Ciclopirox olamine (Ciclopirox ethanolamine) is a synthetic and orally active antifungal agent that can be used for superficial mycoses reseaech. Ciclopirox olamine has a very broad spectrum of activity and inhibits dermatophytes, yeasts, molds, and many Gram-positive and Gram-negative species pathogenic. Ciclopirox olamine also has anticancer and anti-inflammatory effect[1][2][3]. In Vitro:Ciclopirox (10 μM, 18 h) olamine inhibits HUVEC proliferation and angiogenesis[4].
Ciclopirox (0-10 μM, 20 h) olamine inhibits deoxyhypusine hydroxylation in HUVECs[4].
Ciclopirox (0-40 μM, 72 h) olamine shows anti-tumor activity in H1299 and 95D cells (decreases cell viability, with IC50s of 11.13 and 4.136 μM respectively), and inhibits cell migration and invasion[5].
Ciclopirox (0-40 μM, 48 h) olamine arrests both H1299 and 95D cells in G1 phase, decreases Cyclin D1 and CDK4 protein level in H1299 and 95D cells[5].
Ciclopirox (0-20 μM) olamine induces cell aerobic glycolysis, impairs mitochondrial functions and enhances the generation of ROS in H1299 and 95D cells[5].
Ciclopirox (0-40 μM, 48 h) olamine activates PERK-dependent ER stress in CRC cells (HCT-8, HCT-8/5-FU, and DLD-1 cells)[6].
In Vivo:Ciclopirox (20 mg/kg, i.p.) olamine reduces tumor size in mouse H1299 xenograft model, and reduces tumor cell proliferation (Ki67 staining) and increases apoptosis (Cleaved-Caspase 3 and Tunel staining)[5].
Ciclopirox (25 mg/kg, p.o., daily) olamine also inhibits tumor growth in human breast cancer MDA-MB231 xenografts in mice[6].

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