A New Synthesis Of Coenzymically Active Water-Soluble Macromolecular Nad And Nadp Derivatives

Based on an unexpected transformation of N (1)-(2-aminoethyl)-NAD(P) to N⁶-(2-aminoethy1)-NAD(P) under mild aqueous conditions (pH 6.0-6.5, 50°C) synthesis of uniform macromolecular derivatives of N⁶-alkylated NAD and N⁶-alkylated NADP was possible, with, in most cases, acceptable overall yields (6-37%). The usual steps of (a) the chemical reduction with Na₂S₂O₄,(b) the Dimroth rearrangement under harsh alkaline conditions and (c) the enzymatic or chemical oxidation were omitted. This represents a significant simplification of the procedure. A common procedure for the synthesis of macromolecular N⁶-(2-aminoethyl)-NAD(P) derivatives was pursued, coupling N⁶-(2-aminoethyl)-NAD(P) to several water-soluble copolymers containing maleic acid anhydride. PEG (M_r = 20000)-N⁶-(2-aminoethl)-NAD, polyvinylpyrrolidone (M_r,= 160000)-N⁶-(2-aminoethylNAD and dextran (M_r= 70000)-N⁶-(2-aminoethyl)-NAD were synthesized by covalently binding N⁶-(2-aminoethyl)-NAD to the corresponding carboxylated polymers by the carbodiimide method. PEG (M_r= 4000 and 20000-N⁶-(2-aminoethyl)-NADP was efficiently synthesized by covalent attachment of N⁶-(2-aminoethyl)-NADP to N-hydroxy-succinimide activated carboxylate PEG (M_r= 4000 and 20000), avoiding the carbodiimide method, which would lead simultaneously to 2′3′-cyclic NADP derivatives. Except for the macromolecular cofactor derivatives based on copolymers containing maleic acid anhydride, the total enzymatic reducibility of the macromolecular N-(2-aminoethyl)-NAD(P) derivatives was satisfactory (90-95%).