High-yield production of FK228 and new derivatives in a Burkholderia chassis

底盘 伯克氏菌属 产量(工程) 生产(经济) 化学 生物 工程类 遗传学 细菌 经济 物理 结构工程 热力学 宏观经济学
作者
Kai Gong,Maoqin Wang,Qiong Duan,Gang Li,Daojing Yong,Cailing Ren,Yue Li,Qi‐Jun Zhang,Zongjie Wang,Tao Sun,Huanyun Zhang,Qiang Tu,Changsheng Wu,Jun Fu,Aiying Li,Chaoyi Song,Youming Zhang,Rui-Juan Li
出处
期刊:Metabolic Engineering [Elsevier]
卷期号:75: 131-142 被引量:5
标识
DOI:10.1016/j.ymben.2022.12.002
摘要

FK228 (romidepsin) is the only natural histone deacetylases (HDACs) inhibitor approved by FDA to treat cutaneous and peripheral T-cell lymphoma. However, the limited supply and severe cardiotoxicity of FK228 underscore the importance to develop an effective synthetic biology platform for the manufacturing and fine-tuning of this drug lead. In this work, we constructed a Burkholderia chassis for the high-yield production of FK228-family (unnatural) natural products. By virtue of the optimized Burkholderia-specific recombineering system, the biosynthetic gene cluster (BGC) encoding the FK228-like skeleton thailandepsins (tdp) in Burkholderia thailandensis E264 was replaced with an attB integration site to afford the basal chassis KOGC1. The tdp BGC directly captured from E264 was hybridized with the FK228-encoding BGC (dep) using the versatile Red/ET technology. The hybrid BGC (tdp-dep) was integrated into the attB site of KOGC1, resulting in the heterologous expression of FK228. Remarkably, the titer reached 581 mg/L, which is 30-fold higher than that of native producer Chromobacterium violaceum No. 968. This success encouraged us to further engineer the NRPS modules 4 or 6 of hybrid tdp-dep BGC by domain units swapping strategy, and eight new FK228 derivatives (1-8) varying in the composition of amino acids were generated. Especially, the titers of 2 and 3 in KOGC1 were up to 985 mg/L and 453 mg/L, respectively. 2 and 3 displayed stronger cytotoxic activity than FK228. All in all, this work established a robust platform to produce FK228 and its new derivatives in sufficient quantities for anticancer drug development.
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