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酮合成酶超家族内的进化关系反映了复杂的途径关联。

Evolutionary affiliations within the superfamily of ketosynthases reflect complex pathway associations.

作者信息

Moffitt Michelle C, Neilan Brett A

机构信息

School of Microbiology and Immunology, The University of New South Wales, Sydney NSW, 2052, Australia.

出版信息

J Mol Evol. 2003 Apr;56(4):446-57. doi: 10.1007/s00239-002-2415-0.

Abstract

Type I polyketide synthases are known to produce a wide range of medically and industrially important polyketides. The ketosynthase (KS) domain is required for the condensation of an extender unit onto the growing polyketide chain during polyketide biosynthesis. KSs represent a superfamily of complex biosynthetic pathway-associated enzymes found in prokaryotes, fungi, and plants. Although themselves functionally conserved, KSs are involved in the production of a structurally diverse range of metabolites. Degenerate oligonucleotide primers, designed for the amplification of KS domains, amplified KS domains from a range of organisms including cyanobacterial and dinoflagellates. KS domains detected in dinoflagellate cultures appear to have been amplified from the less than 3- micro m filtrate of the nonaxenic culture. Phylogenetic analysis of sequences obtained during this study enabled the specific identification of KS domains of hybrid or mixed polyketide synthase/peptide synthetase complexes, required for the condensation of an extender unit onto an amino acid starter unit. The primer sets described in this study were also used for the detection of novel KS domains directly from environmental samples. The ability to predict function based on primary molecular structure will be critical for future discovery and rational engineering of polyketides.

摘要

已知I型聚酮合酶可产生多种具有医学和工业重要性的聚酮化合物。在聚酮化合物生物合成过程中,酮缩合酶(KS)结构域是将延伸单元缩合到不断增长的聚酮链上所必需的。KS代表了一类在原核生物、真菌和植物中发现的与复杂生物合成途径相关的酶的超家族。尽管KS本身在功能上是保守的,但它们参与了结构多样的一系列代谢产物的合成。为扩增KS结构域设计的简并寡核苷酸引物,从包括蓝细菌和甲藻在内的一系列生物体中扩增出了KS结构域。在甲藻培养物中检测到的KS结构域似乎是从非无菌培养物的小于3微米的滤液中扩增出来的。对本研究中获得的序列进行系统发育分析,能够特异性鉴定杂交或混合聚酮合酶/肽合成酶复合物的KS结构域,这些复合物是将延伸单元缩合到氨基酸起始单元上所必需的。本研究中描述的引物组也用于直接从环境样品中检测新的KS结构域。基于一级分子结构预测功能的能力对于未来聚酮化合物的发现和合理工程设计至关重要。

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