220736-25-4Relevant articles and documents
Short-step and scalable synthesis of (±)-cytoxazone
Asano, Masayoshi,Nagasawa, Chiaki,Suzuki, Masumi,Nishiyama, Shigeru,Sugai, Takeshi
, p. 145 - 148 (2005)
A five-step and scalable synthesis of racemic cytoxazone, a novel cytokine modulator, was accomplished in a total yield of 51% from p-methoxycinnamyl alcohol without any protective groups. The keystep was the new one-pot azidohydroxylation procedure by th
Chemoenzymatic synthesis of all four cytoxazone stereoisomers
Hamersak,Ljubovic,Mercep,Mesic,Sunjic
, p. 1989 - 1992 (2001)
Racemic cytoxazone (±-5) was synthesized starting from easily available glycidic ester (±)-1 by nucleophilic epoxide ring opening, followed by 2-oxazolidinone ring construction and calcium chloride/sodium borohydride reduction of the intermediary ester (±
Preparation method of (-) - Cytoxazone and (+) -4 - epi-Cytoxazone
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Paragraph 0090-0091; 0124-0126; 0131, (2021/11/14)
The preparation method of (-) - Cytoxazone and (+) -4 - epi-Cytoxazone takes D - p-hydroxyphenylglycine as a raw material, the intermediate 2 is obtained through methyl esterification reaction under catalysis of thionyl chloride, and then the amino is protected with Boc anhydride to obtain the intermediate 3. The compound 4 is obtained by using potassium carbonate as a base and reacting with methyl iodide under reflux conditions. The methyl ester was reduced with sodium borohydride/lithium chloride to give the primary alcohol compound 5. An intermediate IBX is then obtained with 6 primary alcohol, then reacted with acetone cyanohydrin SN2 to give intermediate 7, and the intermediate 8 is obtained by reacting with the methanol solution of hydrogen chloride to obtain two five-membered ring compound compounds 9 and 10, respectively, with sodium borohydride to obtain (-) - Cytoxazone and its isomers (+) -4 - epi-Cytoxtoxtoxtoxol, respectively.
Stereoselective synthesis of oxazolidin-2-ones via an asymmetric aldol/curtius reaction: Concise total synthesis of (?)-cytoxazone
Choi, Hosam,Choi, Joohee,Jang, Hanho,Lee, Kiyoun
, (2021/06/14)
Herein, we are reporting an efficient approach toward the synthesis of 4,5-disubstituted oxazolidin-2-one scaffolds. The developed approach is based on a combination of an asymmetric aldol and a modified Curtius protocol, which uses an effective intramolecular ring closure to rapidly access a range of oxazolidin-2-one building blocks. This strategy also permits a straightforward and concise asymmetric total synthesis of (?)-cytoxazone. Consisting of three steps, this is one of the shortest syntheses reported to date. Ultimately, this convenient platform would provide a promising method for the early phases of drug discovery.
New approach for the stereoselective synthesis of (+)-epi-cytoxazone
Miranda, Izabel L.,Sartori, Suélen K.,Diaz, Marisa A.N.,Diaz-Mu?oz, Gaspar
, p. 585 - 591 (2019/08/26)
The stereoselective total synthesis of (+)-epi-cytoxazone was performed satisfactorily in 8 steps, in 17percent overall yield, via a novel route from 2,3-O-(3-pentylidene)-(R)-glyceraldehyde. The bulky group alkene-ketal allowed intramolecular control of