Intramolecular ring-opening from a CO<sub>2</sub>-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed [aziridine + CO<sub>2</sub>] coupling

Debashis Adhikari; Aaron W. Miller; Mu-Hyun Baik; SonBinh T. Nguyen

首页> 外文期刊>Chemical science >Intramolecular ring-opening from a CO₂-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed [aziridine + CO₂] coupling

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Intramolecular ring-opening from a CO₂-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed [aziridine + CO₂] coupling

机译：源自CO _{2 的亲核试剂的分子内开环，作为由（salen）Cr催化的[氮丙啶+ CO _{2 ]偶联生成5-取代的恶唑烷酮的选择性起点}}

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The (salen)Cr-catalyzed [aziridine + CO₂] coupling to form oxazolidinone was found to exhibit excellent selectivity for the 5-substituted oxazolidinone product in the absence of any cocatalyst. Quantum mechanical calculations suggest that the preferential opening of the substituted C–N bond of the aziridine over the unsubstituted C–N bond is a key factor for this selectivity, a result that is supported by experiment with several phenyl-substituted aziridines. In the presence of external nucleophile such as dimethyl aminopyridine (DMAP), the reaction changes pathway and the ring-opening process is regulated by the steric demand of the nucleophile.

机译：发现在不存在任何助催化剂的情况下，（salen）Cr催化的[氮丙啶+ CO _{2 ]偶联形成恶唑烷酮对5-取代的恶唑烷酮产物具有优异的选择性。。量子力学计算表明，氮丙啶的取代C–N键优先于未取代的C–N键的开放是该选择性的关键因素，这一结果得到了多个苯基取代氮丙啶的实验的支持。在外部亲核试剂如二甲基氨基吡啶（DMAP）的存在下，反应会改变途径，开环过程受亲核试剂的空间需求所调节。}

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《Chemical science》 |2015年第2期|共8页
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Debashis Adhikari; Aaron W. Miller; Mu-Hyun Baik; SonBinh T. Nguyen;
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1. Intramolecular ring-opening from a CO2-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed [aziridine + CO2] coupling [J] . Adhikari Debashis, Miller Aaron W., Baik Mu-Hyun, Chemical science . 2015,第2期

机译：源自CO2的亲核试剂的分子内开环，作为由（salen）Cr催化的[氮丙啶+ CO2]偶联生成5-取代的恶唑烷酮的选择性起点
2. Intramolecular ring-opening from a CO₂-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed [aziridine + CO₂] coupling [J] . Debashis Adhikari, Aaron W. Miller, Mu-Hyun Baik, Chemical science . 2015,第2期

机译：源自CO _{2 的亲核试剂的分子内开环，作为由（salen）Cr催化的[氮丙啶+ CO _{2 ]偶联生成5-取代的恶唑烷酮的选择性起点}}
3. Intramolecular ring-opening from a CO2-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed [aziridine + CO2] coupling [J] . Debashis Adhikari, Aaron W. Miller, Mu-Hyun Baik, Chemical science . 2014,第2期

机译：从二氧化碳衍生的亲核试剂的分子内开环作为5-取代的恶唑烷酮的选择性起源，来自（盐）Cr催化的[氮杂辛+ CO2]偶联
4. Regio- and Stereo-Controlled Ring-Opening Cross-Coupling of Aziridines Enabled by Pd Catalysis [C] . Youhei Takeda 日本化学会春季年会講演予稿集 . 2018

机译：通过PD催化启用的亚齐齐齐齐的立体声和立体控制的开环交叉偶联
5. Ring-opening of aziridine-2-carboxamides by carbohydrate C1-O nucleophiles. Stereoselective preparation of O-linked glycopeptides. [D] . Ryan, Daniel. 2009

机译：碳水化合物C1-O亲核试剂打开氮丙啶-2-羧酰胺的开环。 O-连接糖肽的立体选择性制备。
6. Intramolecular ring-opening from a CO2-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed aziridine + CO2 coupling [O] . Debashis Adhikari, Aaron W. Miller, Mu-Hyun Baik, 2015

机译：源自CO2的亲核试剂的分子内开环作为由（salen）Cr催化的氮丙啶+ CO2偶联生成5-取代的恶唑烷酮的选择性起点
7. (Salen)chromium(III)/DMAP: An Efficient Catalyst System for the Selective Synthesis of 5-Substituted Oxazolidinones from Carbon Dioxide and Aziridines [O] . -1

机译：（Salen）铬（III）/ DMAP：一种有效的催化剂体系，用于选择性合成5-取代的二氧化碳和氮化吡啶的奥基唑烷酮

Intramolecular ring-opening from a CO2-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed [aziridine + CO2] coupling

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Intramolecular ring-opening from a CO₂-derived nucleophile as the origin of selectivity for 5-substituted oxazolidinone from the (salen)Cr-catalyzed [aziridine + CO₂] coupling