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Chemo-Enzymatic Synthesis of Chiral Epoxides Ethyl and Methyl (S)-3-(Oxiran-2-yl)propanoates from Renewable Levoglucosenone: An Access to Enantiopure (S)-Dairy Lactone

机译:化学-酶法合成手性环氧乙烷和(S)-3-(Oxiran-2-yl)丙酸甲酯从可再生的左旋葡糖酮中获得:对映纯(S)-乳状内酯

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摘要

Chiral epoxides—such as ethyl and methyl (S)-3-(oxiran-2-yl)propanoates ((>S)>-1a/>1b)—are valuable precursors in many chemical syntheses. Until recently, these compounds were synthesized from glutamic acid in four steps (deamination, reduction, tosylation and epoxide formation) in low to moderate overall yield (20%–50%). Moreover, this procedure requires some harmful reagents such as sodium nitrite ((eco)toxic) and borane (carcinogen). Herein, starting from levoglucosenone (>LGO), a biobased chiral compound obtained through the flash pyrolysis of acidified cellulose, we propose a safer and more sustainable chemo-enzymatic synthetic pathway involving lipase-mediated Baeyer-Villiger oxidation, palladium-catalyzed hydrogenation, tosylation and treatment with sodium ethoxide/methoxide as key steps. This route afforded ethyl and methyl (S)-3-(oxiran-2-yl)propanoates in 57% overall yield, respectively. To demonstrate the potentiality of this new synthetic pathway from >LGO, the synthesis of high value-added (S)-dairy lactone was undertaken from these epoxides and provided the target in 37% overall yield from >LGO.
机译:手性环氧化物-如(S)-3-(环氧乙烷-2-基)丙酸乙酯和丙酸酯((> S )> -1a / > 1b >)-在许多化学合成中都是有价值的前体。直到最近,这些化合物都是由谷氨酸分四个步骤(脱氨基,还原,甲苯磺酸和环氧化物形成)合成的,总产率低至中等(20%–50%)。而且,此程序需要一些有害的试剂,例如亚硝酸钠((生态)有毒)和硼烷(致癌物)。在此,从通过酸化纤维素的快速热解获得的生物基手性化合物左旋葡糖酮(> LGO )开始,我们提出了一种更安全,更可持续的化学酶合成途径,涉及脂肪酶介导的Baeyer-Villiger氧化,钯催化的氢化,甲苯磺酸化和乙醇钠/甲醇钠处理是关键步骤。该路线分别以57%的总收率提供(S)-3-(环氧乙烷-2-基)丙酸乙酯和丙酸甲酯。为了证明这种来自> LGO 的新合成途径的潜力,从这些环氧化物进行了高附加值(S)-乳制品内酯的合成,并提供了>总收率达到37%的目标LGO

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