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鉴定 pacidamycin 组肽核苷抗生素的生物合成基因簇。

Identification of the biosynthetic gene cluster for the pacidamycin group of peptidyl nucleoside antibiotics.

机构信息

Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Proc Natl Acad Sci U S A. 2010 Sep 28;107(39):16828-33. doi: 10.1073/pnas.1011557107. Epub 2010 Sep 8.

Abstract

Pacidamycins are a family of uridyl tetra/pentapeptide antibiotics that act on the translocase MraY to block bacterial cell wall assembly. To elucidate the biosynthetic logic of pacidamcyins, a putative gene cluster was identified by 454 shotgun genome sequencing of the producer Streptomyces coeruleorubidus NRRL 18370. The 31-kb gene cluster encodes 22 proteins (PacA-V), including highly dissociated nonribosomal peptide synthetase (NRPS) modules and a variety of tailoring enzymes. Gene deletions confirmed that two NRPSs, PacP and PacO, are required for the biosynthesis of pacidamycins. Heterologous expression and in vitro assays of PacL, PacO, and PacP established reversible formation of m-Tyr-AMP, l-Ala-AMP, and diaminopropionyl-AMP, respectively, consistent with the amino acids found in pacidamycin scaffolds. The unusual Ala(4)-Phe(5) dipeptidyl ureido linkage was formed during in vitro assays containing purified PacL, PacJ, PacN, and PacO. Both the genetic and enzymatic studies validate identification of the biosynthetic genes for this subclass of uridyl peptide antibiotics and provide the basis for future mechanistic study of their biosynthesis.

摘要

派卡霉素是一类尿苷四/五肽抗生素,通过作用于转位酶 MraY 来阻断细菌细胞壁的组装。为了阐明派卡霉素的生物合成逻辑,通过对其产生菌蓝色链霉菌 NRRL 18370 的 454 焦磷酸测序基因组测序,鉴定出了一个假定的基因簇。该 31kb 的基因簇编码 22 种蛋白(PacA-V),包括高度解离的非核糖体肽合成酶(NRPS)模块和各种修饰酶。基因缺失证实,两个 NRPS,PacP 和 PacO,是派卡霉素生物合成所必需的。PacL、PacO 和 PacP 的异源表达和体外实验建立了 m-Tyr-AMP、l-Ala-AMP 和二氨基丙酰基-AMP 的可逆形成,这与派卡霉素支架中发现的氨基酸一致。在含有纯化的 PacL、PacJ、PacN 和 PacO 的体外实验中形成了独特的 Ala(4)-Phe(5)二肽基脲键。遗传和酶学研究验证了该类尿苷肽抗生素生物合成基因的鉴定,并为其生物合成的进一步机制研究提供了基础。

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