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在阿维链霉菌ATCC31272的阿维菌素聚酮合酶中进行结构域交换后直接生产伊维菌素类药物。

Direct production of ivermectin-like drugs after domain exchange in the avermectin polyketide synthase of Streptomyces avermitilis ATCC31272.

作者信息

Gaisser Sabine, Kellenberger Laurenz, Kaja Andrew L, Weston Alison J, Lill Rachel E, Wirtz Gabriele, Kendrew Steven G, Low Lindsey, Sheridan Rose M, Wilkinson Barrie, Galloway Ian S, Stutzman-Engwall Kim, McArthur Hamish A, Staunton James, Leadlay Peter F

机构信息

Biotica Technology Limited, 181A Huntingdon Road, Cambridge, UK CB3 0DJ.

出版信息

Org Biomol Chem. 2003 Aug 21;1(16):2840-7. doi: 10.1039/b304022d.

Abstract

Ivermectin, a mixture of 22,23-dihydroavermectin B1a9 with minor amounts of 22,23-dihydroavermectin B1b 10, is one of the most successful veterinary antiparasitic drugs ever produced. In humans, ivermectin has been used for the treatment of African river blindness (onchocerciasis) resulting in an encouraging decrease in the prevalence of skin and eye diseases linked to this infection. The components of ivermectin are currently synthesized by chemical hydrogenation of a specific double bond at C22-C23 in the polyketide macrolides avermectins B1a 5 and B1b 6, broad-spectrum antiparasitic agents isolated from the soil bacterium Streptomyces avermitilis. We describe here the production of such compounds (22,23-dihydroavermectins B1a 9 and A1a 11) by direct fermentation of a recombinant strain of S. avermitilis containing an appropriately-engineered polyketide synthase (PKS). This suggests the feasibility of a direct biological route to this valuable drug.

摘要

伊维菌素是22,23-二氢阿维菌素B1a9与少量22,23-二氢阿维菌素B1b10的混合物,是有史以来最成功的兽用抗寄生虫药物之一。在人类中,伊维菌素已被用于治疗非洲河盲症(盘尾丝虫病),使得与这种感染相关的皮肤和眼部疾病患病率出现了令人鼓舞的下降。伊维菌素的成分目前是通过对聚酮类大环内酯阿维菌素B1a5和B1b6中C22 - C23处的特定双键进行化学氢化合成的,阿维菌素B1a5和B1b6是从土壤细菌阿维链霉菌中分离出的广谱抗寄生虫剂。我们在此描述了通过含有经过适当工程改造的聚酮合酶(PKS)的阿维链霉菌重组菌株的直接发酵来生产此类化合物(22,23-二氢阿维菌素B1a9和A1a11)。这表明了通过直接生物途径生产这种有价值药物的可行性。

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