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基于系统发育的菌株优先级排序在药物发现中的风险:以一个案例研究为例。

On the Risks of Phylogeny-Based Strain Prioritization for Drug Discovery: as a Case Study.

机构信息

InBioS-Centre for Protein Engineering, Institut de Chimie B6a, University of Liège, B-4000 Liège, Belgium.

Hedera-22, Boulevard du Rectorat 27b, B-4000 Liège, Belgium.

出版信息

Biomolecules. 2020 Jul 10;10(7):1027. doi: 10.3390/biom10071027.

DOI:10.3390/biom10071027
PMID:32664387
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7408125/
Abstract

Strain prioritization for drug discovery aims at excluding redundant strains of a collection in order to limit the repetitive identification of the same molecules. In this work, we wanted to estimate what can be unexploited in terms of the amount, diversity, and novelty of compounds if the search is focused on only one single representative strain of a species, taking as a model. For this purpose, we selected 18 strains taxonomically clustered with the archetype strain MM109. Genome mining of all isolated from the same cave revealed that 54% of the 42 biosynthetic gene clusters (BGCs) are strain specific, and five BGCs are not present in the reference strain MM109. In addition, even when a BGC is conserved in all strains such as the / cluster involved in bagremycin and ferroverdin production, the compounds produced highly differ between the strains and previously unreported compounds are not produced by the archetype MM109. Moreover, metabolomic pattern analysis uncovered important profile heterogeneity, confirming that identical BGC predisposition between two strains does not automatically imply chemical uniformity. In conclusion, trying to avoid strain redundancy based on phylogeny and genome mining information alone can compromise the discovery of new natural products and might prevent the exploitation of the best naturally engineered producers of specific molecules.

摘要

为了在药物发现中进行菌株优先级排序,目的是排除一个集合中冗余的菌株,以限制对相同分子的重复鉴定。在这项工作中,我们想评估一下,如果将搜索仅集中在一个物种的单一代表菌株上,那么在化合物的数量、多样性和新颖性方面会有多少未被利用,我们以 作为模型。为此,我们选择了 18 株与原型菌株 MM109 聚类的菌株。从同一洞穴中分离出的所有 18 株菌的基因组挖掘显示,42 个生物合成基因簇(BGCs)中有 54%是菌株特异性的,而在参考菌株 MM109 中不存在 5 个 BGCs。此外,即使一个 BGC 如涉及 bagremycin 和 ferroverdin 生产的 / 簇在所有菌株中都保守,菌株之间产生的化合物也有很大差异,并且原型 MM109 不产生以前未报道的化合物。此外,代谢组学模式分析揭示了重要的特征异质性,证实了两个菌株之间相同 BGC 的倾向性并不自动意味着化学均匀性。总之,仅基于系统发育和基因组挖掘信息来避免菌株冗余可能会影响新天然产物的发现,并可能阻止对特定分子的最佳天然工程化生产者的利用。

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