Literature DB >> 21175203

Biosynthesis of the allylmalonyl-CoA extender unit for the FK506 polyketide synthase proceeds through a dedicated polyketide synthase and facilitates the mutasynthesis of analogues.

SangJoon Mo1, Dong Hwan Kim, Jong Hyun Lee, Je Won Park, Devi B Basnet, Yeon Hee Ban, Young Ji Yoo, Shu-wei Chen, Sung Ryeol Park, Eun Ae Choi, Eunji Kim, Ying-Yu Jin, Sung-Kwon Lee, Ju Yeol Park, Yuan Liu, Mi Ok Lee, Keum Soon Lee, Sang Jun Kim, Dooil Kim, Byoung Chul Park, Sang-gi Lee, Ho Jeong Kwon, Joo-Won Suh, Bradley S Moore, Si-Kyu Lim, Yeo Joon Yoon.   

Abstract

The allyl moiety of the immunosuppressive agent FK506 is structurally unique among polyketides and critical for its potent biological activity. Here, we detail the biosynthetic pathway to allylmalonyl-coenzyme A (CoA), from which the FK506 allyl group is derived, based on a comprehensive chemical, biochemical, and genetic interrogation of three FK506 gene clusters. A discrete polyketide synthase (PKS) with noncanonical domain architecture presumably in coordination with the fatty acid synthase pathway of the host catalyzes a multistep enzymatic reaction to allylmalonyl-CoA via trans-2-pentenyl-acyl carrier protein. Characterization of this discrete pathway facilitated the engineered biosynthesis of novel allyl group-modified FK506 analogues, 36-fluoro-FK520 and 36-methyl-FK506, the latter of which exhibits improved neurite outgrowth activity. This unique feature of FK506 biosynthesis, in which a dedicated PKS provides an atypical extender unit for the main modular PKS, illuminates a new strategy for the combinatorial biosynthesis of designer macrolide scaffolds as well as FK506 analogues.

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Year:  2010        PMID: 21175203      PMCID: PMC3030623          DOI: 10.1021/ja108399b

Source DB:  PubMed          Journal:  J Am Chem Soc        ISSN: 0002-7863            Impact factor:   15.419


  29 in total

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4.  FK-506, a novel immunosuppressant isolated from a Streptomyces. II. Immunosuppressive effect of FK-506 in vitro.

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10.  Liquid chromatography-mass spectrometry characterization of FK506 biosynthetic intermediates in Streptomyces clavuligerus KCTC 10561BP.

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  52 in total

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