Maly Dustin J, Leonetti Francesco, Backes Bradley J, Dauber Deborah S, Harris Jennifer L, Craik Charles S, Ellman Jonathan A
Department of Chemistry, University of California, Berkeley, California 94720, USA.
J Org Chem. 2002 Feb 8;67(3):910-5. doi: 10.1021/jo016140o.
A highly efficient solid-phase synthesis method for the preparation of fluorogenic protease substrates based upon the bifunctional leaving group 7-amino-4-carbamoylmethylcoumarin (ACC) is reported. Methods for the large-scale preparation of the novel fluorogenic leaving-group ACC are provided (Scheme 1). Detailed procedures are also provided for loading a diverse set of amino acids to support-bound ACC in good yields and with minimal racemization. Finally, procedures are included for the preparative synthesis of optimized ACC substrates for HIV-1 protease and plasmin.
报道了一种基于双功能离去基团7-氨基-4-氨甲酰甲基香豆素(ACC)制备荧光蛋白酶底物的高效固相合成方法。提供了大规模制备新型荧光离去基团ACC的方法(方案1)。还提供了详细的程序,用于以高收率和最小的消旋作用将多种氨基酸负载到载体结合的ACC上。最后,包括了用于制备HIV-1蛋白酶和纤溶酶的优化ACC底物的合成程序。
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