| Literature DB >> 33764297 |
Lisa Mahler1,2, Sarah P Niehs3, Karin Martin1, Thomas Weber1, Kirstin Scherlach3, Christian Hertweck2,3, Martin Roth1, Miriam A Rosenbaum1,2.
Abstract
Antibiotics from few culturable microorganisms have saved millions of lives since the 20th century. But with resistance formation, these compounds become increasingly ineffective, while the majority of microbial and with that chemical compound diversity remains inaccessible for cultivation and exploration. Culturing recalcitrant bacteria is a stochastic process. But conventional methods are limited to low throughput. By increasing (i) throughput and (ii) sensitivity by miniaturization, we innovate microbiological cultivation to comply with biological stochasticity. Here, we introduce a droplet-based microscale cultivation system, which is directly coupled to a high-throughput screening for antimicrobial activity prior to strain isolation. We demonstrate that highly parallelized in-droplet cultivation starting from single cells results in the cultivation of yet uncultured species and a significantly higher bacterial diversity than standard agar plate cultivation. Strains able to inhibit intact reporter strains were isolated from the system. A variety of antimicrobial compounds were detected for a selected potent antibiotic producer.Entities:
Keywords: antibiotics; antimicrobial compound; high-throughput cultivation; infectious disease; microbiology; strain isolation; uncultured microorganisms
Year: 2021 PMID: 33764297 DOI: 10.7554/eLife.64774
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140