We developed novel synthetic routes to heterocyclic ring systems by using transition metal-mediated or -catalyzed reactions. A Lewis acid-promoted addition of the propargyl Grignard reagent 2 to the Schiff base 1 followed by a silvermediated oxidative cyclization of the homopropargylamine 3 provided the aryl-substituted pyrrole 4. Combined with a chemoselective hydrogenation of the pyrrole ring, this method has been applied to the total synthesis of the biologically active fused indolizidine alkaloids ( ± )-harmicine and ( ± )-crispine A[1]. See Fig. 1.">

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Synthesis of Heterocyclic Ring Systems Using Organometallic Reagents Synthesis of Heterocyclic Ring Systems Using Organometallic Reagents

Synthesis of Heterocyclic Ring Systems Using Organometallic Reagents

  • 期刊名字:復(fù)旦學(xué)報(自然科學(xué)版)
  • 文件大?。?/li>
  • 論文作者:Sameer Agarwal,Jan Knll,Micha
  • 作者單位:Institut für Organische Chemie
  • 更新時間:2022-11-28
  • 下載次數(shù):
論文簡介

1Introduction We developed novel synthetic routes to heterocyclic ring systems by using transition metal-mediated or -catalyzed reactions. A Lewis acid-promoted addition of the propargyl Grignard reagent 2 to the Schiff base 1 followed by a silvermediated oxidative cyclization of the homopropargylamine 3 provided the aryl-substituted pyrrole 4. Combined with a chemoselective hydrogenation of the pyrrole ring, this method has been applied to the total synthesis of the biologically active fused indolizidine alkaloids ( ± )-harmicine and ( ± )-crispine A[1]. See Fig. 1.

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