Identification and Optimization of Kratom Strictosidine Pathway Enabled by Yeast Multiplex Engineering

Monoterpene indole alkaloids (MIAs) are a major class of plant natural products with important pharmaceutical activities, yet the biosynthetic pathway to their universal precursor, strictosidine, has been fully elucidated in only Catharanthus roseus. In kratom (Mitragyna speciosa), only the first and last steps of strictosidine biosynthesis were previously known. Here, we applied multiplex pathway engineering in yeast to accelerate the discovery, reconstruction, and optimization of the kratom strictosidine pathway. Iterative multiplex integration and screening identified 13 functional kratom genes and enabled rapid validation of functional pathway modules, thereby completing the kratom strictosidine pathway from geranyl pyrophosphate and tryptophan. We also identified a vacuolar secologanin transporter, MsNPF2.6, which increased strictosidine production by 62% in yeast. Pathway optimization through the incorporation of nepetalactol-producing enzymes from other plants further supported strictosidine production in yeast from fed geraniol and tryptophan. These results establish the strictosidine pathway in kratom and highlight multiplex engineering as a powerful platform for rapid plant pathway discovery and optimization.