An Enzyme Module System for the Synthesis of dTDP-activated Deoxysugars from dTMP and Sucrose

A flexible enzyme module system is presented that allows preparative access to important dTDP-activated deoxyhexoses from dTMP and sucrose. The strategic combination of the recombinant enzymes dTMP-kinase and sucrose synthase (SuSy), and the enzymes RmlB (4,6-dehydratase), RmlC (3,5-epimerase) and RmlD (4-ketoreductase) from the biosynthetic pathway of dTDP-β-L-rhamnose was optimized. The SuSy module (dTMP-kinase, SuSy, ±RmlB) yielded the precursor dTDP-α-D-glucose (2) or the biosynthetic intermediate dTDP-6-deoxy-4-keto-α-D-glucose (3) on a 0.2–0.6 g scale with overall yields of 62 % and 72 %, respectively. A two-step strategy in which the SuSy module was followed by the deoxysugar module (RmlC and RmlD) resulted in the synthesis of dTDP-β-L-rhamnose (4; 24.1 μmol, overall yield: 35.9 %). Substitution of RmlC by DnmU from the dTDP-β-L-daunosamine pathway of Streptomyces peucetius in this module demonstrated that DnmU acts in vitro as a 3,5-epimerase with 3 as substrate to yield 4 (32.2 μmol, overall yield: 44.7 %). Chemical reduction of 3 with NaBH4 gave a mixture of the C-4 epimers dTDP-α-D-quinovose (6) and dTDP-α-D-fucose (7) in a ratio of 2:1. In summary, the modular character of the presented enzyme system provides valuable compounds for the biochemical characterization of deoxysugar pathways playing a major role in microbial producers of antibiotic and antitumour agents.