紫杉醇
红豆杉
生物合成
基因
化学
代谢途径
酶
生物化学
功能(生物学)
生物
计算生物学
细胞生物学
遗传学
植物
癌症
作者
Chun‐Ting Liu,Ricardo De La Peña,Christian Tocol,Elizabeth S. Sattely
标识
DOI:10.1038/s41467-024-45574-8
摘要
Abstract Paclitaxel is an anticancer therapeutic produced by the yew tree. Over the last two decades, a significant bottleneck in the reconstitution of early paclitaxel biosynthesis has been the propensity of heterologously expressed pathway cytochromes P450, including taxadiene 5α-hydroxylase (T5αH), to form multiple products. Here, we structurally characterize four new products of T5αH, many of which appear to be over-oxidation of the primary mono-oxidized products. By tuning the promoter strength for T5αH expression in Nicotiana plants, we observe decreased levels of these proposed byproducts with a concomitant increase in the accumulation of taxadien-5α-ol, the paclitaxel precursor, by three-fold. This enables the reconstitution of a six step biosynthetic pathway, which we further show may function as a metabolic network. Our result demonstrates that six previously characterized Taxus genes can coordinatively produce key paclitaxel intermediates and serves as a crucial platform for the discovery of the remaining biosynthetic genes.
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