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宏基因组数据揭示了生物群落中I型聚酮合酶的分布。

Metagenomic Data Reveal Type I Polyketide Synthase Distributions Across Biomes.

作者信息

Singh Hans W, Creamer Kaitlin E, Chase Alexander B, Klau Leesa J, Podell Sheila, Jensen Paul R

出版信息

bioRxiv. 2023 Jan 11:2023.01.09.523365. doi: 10.1101/2023.01.09.523365.

DOI:10.1101/2023.01.09.523365
PMID:36711755
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9882069/
Abstract

UNLABELLED

Microbial polyketide synthase (PKS) genes encode the biosynthesis of many biomedically important natural products, yet only a small fraction of nature's polyketide biosynthetic potential has been realized. Much of this potential originates from type I PKSs (T1PKSs), which can be delineated into different classes and subclasses based on domain organization and structural features of the compounds encoded. Notably, phylogenetic relationships among PKS ketosynthase (KS) domains provide a method to classify the larger and more complex genes in which they occur. Increased access to large metagenomic datasets from diverse habitats provides opportunities to assess T1PKS biosynthetic diversity and distributions through the analysis of KS domain sequences. Here, we used the webtool NaPDoS2 to detect and classify over 35,000 type I KS domains from 137 metagenomic data sets reported from eight diverse biomes. We found biome-specific separation with soils enriched in modular -AT and hybrid -AT KSs relative to other biomes and marine sediments enriched in KSs associated with PUFA and enediyne biosynthesis. By extracting full-length KS domains, we linked the phylum Actinobacteria to soil-specific enediyne and -AT clades and identified enediyne and monomodular KSs in phyla from which the associated compound classes have not been reported. These sequences were phylogenetically distinct from those associated with experimentally characterized PKSs suggesting novel structures or enzyme functions remain to be discovered. Lastly, we employed our metagenome-extracted KS domains to evaluate commonly used type I KS PCR primers and identified modifications that could increase the KS sequence diversity recovered from amplicon libraries.

IMPORTANCE

Polyketides are a crucial source of medicines, agrichemicals, and other commercial products. Advances in our understanding of polyketide biosynthesis coupled with the accumulation of metagenomic sequence data provide new opportunities to assess polyketide biosynthetic potential across biomes. Here, we used the webtool NaPDoS2 to assess type I PKS diversity and distributions by detecting and classifying KS domains across 137 metagenomes. We show that biomes are differentially enriched in KS domain classes, providing a roadmap for future biodiscovery strategies. Further, KS phylogenies reveal both biome-specific clades that do not include biochemically characterized PKSs, highlighting the biosynthetic potential of poorly explored environments. The large metagenome-derived KS dataset allowed us to identify regions of commonly used type I KS PCR primers that could be modified to capture a larger extent of KS diversity. These results facilitate both the search for novel polyketides and our understanding of the biogeographical distribution of PKSs across earth's major biomes.

摘要

未标记

微生物聚酮合酶(PKS)基因编码许多具有重要医学价值的天然产物的生物合成,但自然界聚酮生物合成潜力中只有一小部分得以实现。这种潜力很大一部分源于I型聚酮合酶(T1PKSs),根据所编码化合物的结构域组织和结构特征,T1PKSs可分为不同的类别和亚类。值得注意的是,聚酮合酶酮基合成酶(KS)结构域之间的系统发育关系提供了一种对包含这些结构域的更大、更复杂基因进行分类的方法。从不同生境获取大量宏基因组数据集的机会增加,使得通过分析KS结构域序列来评估T1PKS生物合成多样性和分布成为可能。在这里,我们使用网络工具NaPDoS2从8个不同生物群落报告的137个宏基因组数据集中检测和分类了超过35,000个I型KS结构域。我们发现不同生物群落之间存在特异性分离,相对于其他生物群落,土壤中富含模块化 -AT和杂交 -AT KSs,而海洋沉积物中富含与多不饱和脂肪酸(PUFA)和烯二炔生物合成相关的KSs。通过提取全长KS结构域,我们将放线菌门与土壤特异性烯二炔和 -AT进化枝联系起来,并在尚未报道相关化合物类别的门中鉴定出烯二炔和单模块KSs。这些序列在系统发育上与那些与实验表征的PKSs相关的序列不同,表明仍有待发现新的结构或酶功能。最后,我们利用从宏基因组中提取的KS结构域来评估常用的I型KS聚合酶链反应(PCR)引物,并确定了可以增加从扩增子文库中回收的KS序列多样性的修饰。

重要性

聚酮化合物是药物、农用化学品和其他商业产品的重要来源。我们对聚酮生物合成理解的进展以及宏基因组序列数据的积累为评估跨生物群落的聚酮生物合成潜力提供了新机会。在这里,我们使用网络工具NaPDoS2通过检测和分类137个宏基因组中的KS结构域来评估I型PKS的多样性和分布。我们表明不同生物群落中KS结构域类别存在差异富集,为未来的生物发现策略提供了路线图。此外,KS系统发育揭示了不包括经过生物化学表征的PKSs的生物群落特异性进化枝,突出了未充分探索环境的生物合成潜力。大量来自宏基因组的KS数据集使我们能够识别常用的I型KS PCR引物中可以修改以捕获更大范围KS多样性的区域。这些结果有助于寻找新型聚酮化合物,并增进我们对PKSs在地球主要生物群落中生物地理分布的理解。

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