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1-benzyl-3-bromomethyl-1H-quinoxalin-2-one is a chemical with a specific purpose. Lookchem provides you with multiple data and supplier information of this chemical.

328249-83-8

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328249-83-8 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 328249-83-8 includes 9 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 6 digits, 3,2,8,2,4 and 9 respectively; the second part has 2 digits, 8 and 3 respectively.
Calculate Digit Verification of CAS Registry Number 328249-83:
(8*3)+(7*2)+(6*8)+(5*2)+(4*4)+(3*9)+(2*8)+(1*3)=158
158 % 10 = 8
So 328249-83-8 is a valid CAS Registry Number.

328249-83-8Downstream Products

328249-83-8Relevant academic research and scientific papers

Structure-activity studies of substituted quinoxalinones as multiple-drug-resistance antagonists

Lawrence,Copper,Smith

, p. 594 - 601 (2001)

A significant problem in the clinical treatment of cancer relates to the development of tumor resistance to many chemotherapeutic agents. Acquired drug resistance is often mediated through overexpression of membrane transport proteins that effectively efflux anticancer agents. Two of the best-studied transporters, P-glycoprotein (Pgp) and MRP1, have pharmacological properties that only partially overlap. In our search for improved drug-resistance antagonists, we have identified a family of substituted quinoxalines that selectively antagonizes Pgp over MRP1. Consequently, a focused library of congeners was designed and synthesized starting with a parent bromomethylquinoxalinone. This parent quinoxalinone was then condensed with a series of phenols to yield a family of substituted phenoxymethylquinoxalinones. These compounds were evaluated for their toxicity toward drug-sensitive MCF-7 breast carcinoma cells and for their abilities to antagonize Pgp and MRP1 in drug-resistant cell lines (NCI/ADR and MCF-7/VP, respectively). The results of this structure-activity study indicate that compounds with carbonyl substitutions of the phenoxy group (ester, amide, or ketone moieties) demonstrate excellent antagonism of Pgp while having relatively low toxicity toward drug-sensitive cells. Importantly, none of these compounds antagonized MRP1. Because of their transporter selectivity, we predict that substituted quinoxalinones may be more effective MDR modulators in vivo than are nonselective transporter antagonists.

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