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Ceranib-2

رقم الكتالوجGC15981

Ceranib-2 هو مثبط قوي وغير دهني للسيراميداز الذي يثبط نشاط سيراميداز الخلوي مع IC 50 من 28 ميكرومتر في خلايا SKOV3يحفز Ceranib-2 تراكم أنواع متعددة من السيراميد ، ويقلل من مستويات السفينجوزين والسفينجوزين -1 الفوسفات (S1P) ، ويحفز موت الخلايا المبرمجنشاط مضاد للسرطان

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Ceranib-2 التركيب الكيميائي

Cas No.: 1402830-75-4

الحجم السعر المخزون الكميّة
5mg
59٫00
متوفر
10mg
109٫00
متوفر
25mg
228٫00
متوفر
50mg
376٫00
متوفر

Tel:(909) 407-4943 Email: sales@glpbio.com

مراجعات العميل

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Sample solution is provided at 25 µL, 10mM.

Description Chemical Properties Product Documents Related Products

IC50: 28 μM

Ceranib-2 is an inhibitor of cellular ceramidase activity.

Ceramidase catalyzes the hydrolysis of the N-acyl linkage between the fatty acid and sphingosine base in ceramide to produce sphingosine and a free fatty acid. Ceramidase plays a key role in regulating cell fate and its inhibition in both malignant and non-cancerous cells results in apoptosis.

In vitro: In a previous study, a more potent analogue (Ceranib-2) of novel ceramidase inhibitor (Ceranib-1) was identified by screening a small molecule library. In a cell-based assay, both Ceranib-1 and Ceranib-2 were able to inhibit cellular ceramidase activity, decrease levels of sphingosine and S1P, inhibit the proliferation of cells alone and, induce the accumulation of multiple ceramide species, and induce cell-cycle arrest and death in combination with paclitaxel [1].

In vivo: In a previous study, Ceranib-2 was given by i.p. injection on 5 days per week. Resutls showed that the average normalized size of tumors in each treatment group increased over time. However, by day 11 Ceranib-2-treated groups had significantly lower tumor volumes. By day 21, the average normalized tumor volumes for the control, 20 mg/kg and 50 mg/kg Ceranib-2 groups were 1,400, 940, and 710, respectively. In addition, the administration of Ceranib-2 did not alter the total body weight of the mice [1].

Clinical trial: So far, no clinical study has been conducted.

Reference:
[1] Draper, J. M.,Xia, Z.,Smith, R.A., et al. Discovery and evaluation of inhibitors of human ceramidase. Molecular Cancer Therapeutics 1-27 (2011).

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