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methyl 3'-{[(2,4-dimethoxybenzyl)amino]carbonyl}-4-hydroxy[1,1'-biphenyl]-3-carboxylate is a chemical with a specific purpose. Lookchem provides you with multiple data and supplier information of this chemical.

809278-93-1

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809278-93-1 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 809278-93-1 includes 9 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 6 digits, 8,0,9,2,7 and 8 respectively; the second part has 2 digits, 9 and 3 respectively.
Calculate Digit Verification of CAS Registry Number 809278-93:
(8*8)+(7*0)+(6*9)+(5*2)+(4*7)+(3*8)+(2*9)+(1*3)=201
201 % 10 = 1
So 809278-93-1 is a valid CAS Registry Number.

809278-93-1Downstream Products

809278-93-1Relevant academic research and scientific papers

Rational design of diflunisal analogues with reduced affinity for human serum albumin

Mao,Hajduk,Craig,Bell,Borre,Fesik

, p. 10429 - 10435 (2001)

Many lead compounds bind to serum albumin and exhibit markedly reduced efficacy in vivo as compared to their potency in vitro. To aid in the design of compounds with reduced albumin binding, we performed nuclear magnetic resonance (NMR) structural and binding studies on the complex between domain III of human serum albumin (HSA-III) and diflunisal, a cyclooxygenase inhibitor with antiinflammatory activity. The structural studies indicate that the aromatic rings of diflunisal are involved in extensive and specific interactions with hydrophobic residues that comprise the binding pocket in subdomain IIIA. The carboxylic acid of diflunisal forms electrostatic interactions with the protein similar to those observed in the X-ray structure of HSA complexed to myristic acid. In addition to the structural studies, NMR-derived binding constants were obtained for diflunisal and closely related analogues to develop a structure-affinity relationship for binding to subdomain IIIA. On the basis of the structural and binding data, compounds were synthesized that exhibit more than a 100-fold reduction in binding to domain III of HSA, and nearly a 10-fold reduction in affinity for full length albumin. Significantly, several of these compounds maintain activity against cyclooxygenase-2. These results suggest a rational strategy for designing out albumin binding in potential drug molecules by using structure-based design in conjunction with NMR-based screening.

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