Published July 29, 2021 | Version v1
Journal article Open

Novel Transaminase and Laccase from Streptomyces spp. Using Combined Identification Approaches

  • 1. Istituto di Scienze e Tecnologie Chimiche (SCITEC)
  • 2. Institute of Molecular Genetics and Genetic Engineering
  • 3. Fraunhofer Institute for Interfacial Engineering
  • 4. Trinity College Dublin

Description

Three Streptomyces sp. strains with a multitude of target enzymatic activities confirmed by functional screening, namely BV129, BV286 and BV333, were subjected to genome sequencing aiming at the annotation of genes of interest, in-depth bioinformatics characterization and functional expression of the biocatalysts. A whole-genome shotgun sequencing followed by de novo genome assembly and annotation was performed revealing genomes of 6.4, 9.4 and 7.3 Mbp, respectively. Functional annotation of the proteins of interest resulted in between 2047 and 2763 putative targets. Among the various enzymatic activities that the three Streptomyces strains demonstrated to produce by functional screening, we focused our attention on transaminases (TAs) and laccases due to their high biocatalytic potential. Bioinformatics search allowed the identification of a putative TA from Streptomyces sp. BV333 as a potentially novel broad substrate scope TA and a putative laccase from Streptomyces sp. BV286 as potentially novel blue multicopper oxidase. The two sequences were cloned and overexpressed in Escherichia coli and the two novel enzymes, transaminase Sbv333-TA and laccase Sbv286-LAC, were characterized. Interestingly, both enzymes resulted to be exceptionally thermostable, Sbv333-TA showing a melting temperature (TM = 85 ◦C) only slightly lower compared to the TM of the most thermostable transaminases described to date (87–88 ◦C) and Sbv286-LAC being even thermoactivated at temperature >60 ◦C. Moreover, Sbv333-TA showed a broad substrate scope and remarkably demonstrated to be active in the transamination of β-ketoesters, which are rarely accepted by currently known TAs. On the other hand, Sbv286-LAC showed an improved activity in the presence of the cosolvent acetonitrile. Overall, it was shown that a combination of approaches from standard microbiological and biochemical screens to genome sequencing and analysis is required to afford novel and functional biocatalysts.

Files

catalysts-11-00919.pdf

Files (4.4 MB)

Name Size Download all
md5:8ca2633cbf554ce3dae54f35d110c8b3
4.4 MB Preview Download

Additional details

Funding

BioICEP – Bio Innovation of a Circular Economy for Plastics 870292
European Commission