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2-(2,5-dimethoxy-phenyl)-5-hydroxy-benzofuran-3-carboxylic acid ethyl ester is a complex organic compound with the molecular formula C18H18O7. It is a derivative of benzofuran, a heterocyclic aromatic compound consisting of a benzene ring fused to a furan ring. The molecule features a 2,5-dimethoxyphenyl group attached to the benzofuran core, which contributes to its unique chemical properties. The hydroxyl group at the 5-position and the carboxylic acid group at the 3-position further modify its reactivity and solubility. The ethyl ester group at the carboxylic acid end enhances the compound's lipophilicity, making it more soluble in organic solvents. This chemical is primarily of interest in the field of organic chemistry and may have potential applications in pharmaceuticals or as a synthetic intermediate due to its structural diversity and functional groups.

60946-81-8

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60946-81-8 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 60946-81-8 includes 8 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 5 digits, 6,0,9,4 and 6 respectively; the second part has 2 digits, 8 and 1 respectively.
Calculate Digit Verification of CAS Registry Number 60946-81:
(7*6)+(6*0)+(5*9)+(4*4)+(3*6)+(2*8)+(1*1)=138
138 % 10 = 8
So 60946-81-8 is a valid CAS Registry Number.

60946-81-8Downstream Products

60946-81-8Relevant academic research and scientific papers

Identification of Novel Coumestan Derivatives as Polyketide Synthase 13 Inhibitors against Mycobacterium tuberculosis. Part II

Zhang, Wei,Lun, Shichun,Liu, Ling-Ling,Xiao, Shiqi,Duan, Guanfu,Gunosewoyo, Hendra,Yang, Fan,Tang, Jie,Bishai, William R.,Yu, Li-Fang

, p. 3575 - 3589 (2019)

Our group recently reported the identification of novel coumestan derivatives as Mycobacterium tuberculosis (Mtb) Pks13-thioesterase (TE) domain inhibitors, with mutations observed (D1644G and N1640K) in the generated coumestan-resistant Mtb colonies. Herein, we report a further structure-activity relationships exploration exploiting the available Pks13-TE X-ray co-crystal structure that resulted in the discovery of extremely potent coumestan analogues 48 and 50. These molecules possess excellent anti-tuberculosis activity against both the drug-susceptible (MIC = 0.0039 μg/mL) and drug-resistant Mtb strains (MIC = 0.0078 μg/mL). Moreover, the excellent in vitro activity is translated to the in vivo mouse serum inhibitory titration assay, with administration of coumestan 48 at 100 mg/kg showing an 8-fold higher activity than that of isoniazid or TAM16 given at 10 or 100 mg/kg, respectively. Preliminary ADME-Tox data for the coumestans were promising and, coupled with the practicality of synthesis, warrant further in vivo efficacy assessments of the coumestan derivatives.

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