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靶向宏基因组学作为一种挖掘海洋天然产物多样性以发现和生产候选药物的工具。

Targeted metagenomics as a tool to tap into marine natural product diversity for the discovery and production of drug candidates.

作者信息

Trindade Marla, van Zyl Leonardo Joaquim, Navarro-Fernández José, Abd Elrazak Ahmed

机构信息

Institute for Microbial Biotechnology and Metagenomics, University of the Western Cape, Bellville South Africa.

Institute for Microbial Biotechnology and Metagenomics, University of the Western Cape, Bellville South Africa ; Centro Regional de Hemodonación, Servicio de Hematología y Oncología Médica, Universidad de Murcia, IMIB-Arrixaca, Murcia Spain.

出版信息

Front Microbiol. 2015 Aug 28;6:890. doi: 10.3389/fmicb.2015.00890. eCollection 2015.

Abstract

Microbial natural products exhibit immense structural diversity and complexity and have captured the attention of researchers for several decades. They have been explored for a wide spectrum of applications, most noteworthy being their prominent role in medicine, and their versatility expands to application as drugs for many diseases. Accessing unexplored environments harboring unique microorganisms is expected to yield novel bioactive metabolites with distinguishing functionalities, which can be supplied to the starved pharmaceutical market. For this purpose the oceans have turned out to be an attractive and productive field. Owing to the enormous biodiversity of marine microorganisms, as well as the growing evidence that many metabolites previously isolated from marine invertebrates and algae are actually produced by their associated bacteria, the interest in marine microorganisms has intensified. Since the majority of the microorganisms are uncultured, metagenomic tools are required to exploit the untapped biochemistry. However, after years of employing metagenomics for marine drug discovery, new drugs are vastly under-represented. While a plethora of natural product biosynthetic genes and clusters are reported, only a minor number of potential therapeutic compounds have resulted through functional metagenomic screening. This review explores specific obstacles that have led to the low success rate. In addition to the typical problems encountered with traditional functional metagenomic-based screens for novel biocatalysts, there are enormous limitations which are particular to drug-like metabolites. We also present how targeted and function-guided strategies, employing modern, and multi-disciplinary approaches have yielded some of the most exciting discoveries attributed to uncultured marine bacteria. These discoveries set the stage for progressing the production of drug candidates from uncultured bacteria for pre-clinical and clinical development.

摘要

微生物天然产物展现出巨大的结构多样性和复杂性,几十年来一直吸引着研究人员的关注。它们已被探索用于广泛的应用,其中最值得注意的是它们在医学中的突出作用,并且其多功能性扩展到作为多种疾病的药物应用。获取蕴藏独特微生物的未开发环境有望产生具有独特功能的新型生物活性代谢物,从而为匮乏的制药市场提供产品。为此,海洋已成为一个有吸引力且富有成效的领域。由于海洋微生物具有巨大的生物多样性,以及越来越多的证据表明许多先前从海洋无脊椎动物和藻类中分离出的代谢物实际上是由其相关细菌产生的,对海洋微生物的兴趣日益浓厚。由于大多数微生物尚未培养,因此需要宏基因组学工具来开发未开发的生物化学资源。然而,在将宏基因组学用于海洋药物发现多年之后,新药物的数量却严重不足。虽然报道了大量天然产物生物合成基因和基因簇,但通过功能宏基因组筛选仅产生了少数潜在的治疗性化合物。本综述探讨了导致成功率低的具体障碍。除了在基于传统功能宏基因组的新型生物催化剂筛选中遇到的典型问题外,类药物代谢物还存在巨大的局限性。我们还介绍了采用现代多学科方法的靶向和功能导向策略如何产生了一些归因于未培养海洋细菌的最令人兴奋的发现。这些发现为从未培养细菌生产候选药物用于临床前和临床开发奠定了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/40f8/4552006/15bc438530ea/fmicb-06-00890-g001.jpg

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