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The Architecture of Metabolism Maximizes Biosynthetic Diversity in the Largest Class of Fungi

机译:新陈代谢结构最大限度地提高了最大一类真菌的生物合成多样性

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摘要

Ecological diversity in fungi is largely defined by metabolic traits, including the ability to produce secondary or "specialized" metabolites (SMs) that mediate interactions with other organisms. Fungal SM pathways are frequently encoded in biosynthetic gene clusters (BGCs), which facilitate the identification and characterization of metabolic pathways. Variation in BGC composition reflects the diversity of their SM products. Recent studies have documented surprising diversity of BGC repertoires among isolates of the same fungal species, yet little is known about how this population-level variation is inherited across macroevolutionary timescales. Here, we applied a novel linkage-based algorithm to reveal previously unexplored dimensions of diversity in BGC composition, distribution, and repertoire across 101 species of Dothideomycetes, which are considered the most phylogenetically diverse class of fungi and known to produce many SMs. We predicted both complementary and overlapping sets of clustered genes compared with existing methods and identified novel gene pairs that associate with known secondary metabolite genes. We found that variation among sets of BGCs in individual genomes is due to nonoverlapping BGC combinations and that several BGCs have biased ecological distributions, consistent with niche-specific selection. We observed that total BGC diversity scales linearly with increasing repertoire size, suggesting that secondary metabolites have little structural redundancy in individual fungi. We project that there is substantial unsampled BGC diversity across specific families of Dothideomycetes, which will provide a roadmap for future sampling efforts. Our approach and findings lend new insight into how BGC diversity is generated and maintained across an entire fungal taxonomic class.
机译:真菌的生态多样性主要由代谢性状决定,包括产生介导与其他生物体相互作用的次级或“特化”代谢物(SMs)的能力。真菌SM通路通常编码在生物合成基因簇(BGCs)中,这有助于代谢通路的鉴定和表征。BGC 成分的变化反映了其 SM 产品的多样性。最近的研究记录了相同真菌物种的分离株中BGC库的惊人多样性,但对这种种群水平的变异如何在宏观进化时间尺度上遗传知之甚少。在这里,我们应用了一种基于连锁的新型算法来揭示 101 种点霉菌的 BGC 组成、分布和库中以前未探索的多样性维度,这些真菌被认为是系统发育多样性最强的一类真菌,已知会产生许多 SM。与现有方法相比,我们预测了互补和重叠的簇状基因集,并确定了与已知次级代谢物基因相关的新基因对。我们发现,单个基因组中BGCs组之间的变异是由于BGC组合不重叠,并且一些BGCs具有偏倚的生态分布,与生态位特异性选择一致。我们观察到,总BGC多样性随着库大小的增加呈线性比例,这表明次生代谢物在单个真菌中几乎没有结构冗余。我们预计,在特定的点霉菌家族中,存在大量的未采样BGC多样性,这将为未来的采样工作提供路线图。我们的方法和发现为BGC多样性如何在整个真菌分类类别中产生和维持提供了新的见解。

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