OX4 Is an NADPH-Dependent Dehydrogenase Catalyzing an Extended Michael Addition Reaction To Form the Six-Membered Ring in the Antifungal HSAF.
Xue LiHao-Xin WangYue-Mao ShenYao-Yao LiLiangcheng DuPublished in: Biochemistry (2019)
The polycyclic tetramate macrolactam HSAF is an antifungal natural product isolated from Lysobacter enzymogenes. HSAF and its analogues have a distinct chemical structure and new mode of antifungal action. The mechanism by which the 5/5/6 tricycle of HSAF is formed from the polyene precursor is not totally clear. Here, we used purified OX4, a homologous enzyme of alcohol dehydrogenase/Zn-binding proteins, to show the enzymatic mechanism for six-membered ring formation. The results from the deuterium isotope incorporation demonstrated that OX4 selectively transfers the pro-R hydride of NADPH to C21 and one proton from water to C10 of 3-deOH alteramide C (1), resulting in 3-deOH HSAF (2) through a reductive cyclization of the polyene precursor by a mechanism consistent with an extended 1,6-Michael addition reaction. The regioselective incorporation of the NADPH hydride into C21 of 1 is also stereoselective, leading to the 21S configuration of 2. This work represents the first characterization of the activity and selectivity of the enzyme for six-membered ring formation in a group of distinct antifungal polycyclic tetramate macrolactams.