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methyl 2-(3,5-dimethoxy-4-methylphenyl)acetate is a chemical with a specific purpose. Lookchem provides you with multiple data and supplier information of this chemical.

78707-40-1

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78707-40-1 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 78707-40-1 includes 8 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 5 digits, 7,8,7,0 and 7 respectively; the second part has 2 digits, 4 and 0 respectively.
Calculate Digit Verification of CAS Registry Number 78707-40:
(7*7)+(6*8)+(5*7)+(4*0)+(3*7)+(2*4)+(1*0)=161
161 % 10 = 1
So 78707-40-1 is a valid CAS Registry Number.

78707-40-1Relevant academic research and scientific papers

Total synthesis and cytotoxic activity of stellatin

Saeed, Aamer,Ashraf, Zaman,Rafique, Hummera

experimental part, p. 97 - 104 (2011/04/12)

Stellatin (3,4-dihydro-8-hydroxy-7-hydroxymethyl-6-methoxyisocoumarin) (8), an extrolite of fungal genera Emericella and Aspergillus, was synthesized. Thus, Vilsmeier-Haack formylation of methyl ester of 3,5-dimethoxy-4- methylphenylacetic acid (1) to aff

Total synthesis of chlorofusin, its seven chromophore diastereomers, and key partial structures

Clark, Ryan C.,Sang, Yeul Lee,Boger, Dale L.

supporting information; experimental part, p. 12355 - 12369 (2009/02/05)

Chlorofusin is a recently isolated, naturally occurring inhibitor of p53-MDM2 complex formation whose structure is composed of a densely functionalized azaphilone-derived chromophore linked through the terminal amine of ornithine to a nine residue cyclic peptide. Herein we report the full details of the total synthesis of chlorofusin, resulting in the assignment of the absolute stereochemistry and reassignment of the relative stereochemistry of the complex chromophore. Condensation of each enantiomer of an azaphilone chromophore precursor with the Nδ-amine of a protected ornithine-threonine dipeptide, followed by a one-step oxidation/spirocyclization of the most reactive olefin provided all eight diastereomers of the fully elaborated chromophore-dipeptide conjugate. Comparison of the spectroscopic properties for these eight compounds and those of simpler models with that reported for the natural product allowed the full assignment of the (4R,8S,9R)-stereochemistry of the chlorofusin chromophore. The natural, but stereochemically reassigned, diastereomer of the dipeptide conjugate was incorporated in a convergent total synthesis of chlorofusin confirming the stereochemical reassignment and establishing its absolute stereochemistry. Similarly and enlisting the late stage convergent point in the total synthesis, the remaining seven diastereomers of the chromophore-dipeptide conjugates were individually incorporated into the nine-residue cyclic peptide of chlorofusin (4 steps each) providing all seven remaining possible chromophore diastereomers of the natural product.

Total synthesis, stereochemical reassignment, and absolute configuration of chlorofusin

Sang, Yeul Lee,Clark, Ryan C.,Boger, Dale L.

, p. 9860 - 9861 (2008/03/12)

Chlorofusin is a recently isolated, naturally occurring inhibitor of p53-MDM2 complex formation whose structure is composed of a densely functionalized azaphilone-derived chromophore linked through the terminal amine of ornithine to a nine-residue cyclic peptide. Herein we report full details of the total synthesis of chlorofusin, resulting in the assignment of the absolute stereochemistry and reassignment of the relative stereochemistry of the complex chromophore. Condensation of each enantiomer of an azaphilone chromophore precursor with the Nδ-amine of a protected ornithine-threonine dipeptide, followed by a one-step oxidative spirocyclization of the most reactive olefin provided all eight diastereomers of the fully elaborated chromophore-dipeptide conjugate. Comparison of the spectroscopic properties for these eight compounds with simpler models and with that reported for the natural product allowed the full assignment of the (4R,8S,9R)-stereochemistry of the chlorofusin chromophore. The desired, but stereochemically reassigned, diastereomer of the dipeptide conjugate was incorporated in a convergent total synthesis of chlorofusin confirming both the relative stereochemical reassignment and the establishment of its absolute stereochemistry. In addition to natural chlorofusin, the (4R,8R,9R)-diastereomer proposed by Williams as well as the (4R,8S,9S) and (4R,8R,9S)-diastereomers of chlorofusin were also prepared as key analogues of the natural product, and the noncorrelation of their spectral data with that reported for natural chlorofusin further supports the new structural assignment and maintains the diagnostic spectroscopic distinctions observed with the eight diastereomers of the chromophore ornithine-threonine dipeptide conjugates. The reassignment of the relative stereochemistry for the chlorofusin chromophore is still, but less obviously, consistent with the experimental NOEs observed by Williams in the original structural assignment work, and the assignment of its absolute configuration is opposite that recently disclosed by Yao. Copyright

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