| Literature DB >> 29944936 |
Adelfia Talà1, Fabrizio Damiano1, Giuseppe Gallo2, Eva Pinatel3, Matteo Calcagnile1, Mariangela Testini1, Daniela Fico4, Daniela Rizzo4, Alberto Sutera2, Giovanni Renzone5, Andrea Scaloni5, Gianluca De Bellis3, Luisa Siculella1, Giuseppe Egidio De Benedetto4, Anna Maria Puglia6, Clelia Peano7, Pietro Alifano8.
Abstract
Pirins are evolutionarily conserved iron-containing proteins that are found in all kingdoms of life, and have been implicated in diverse molecular processes, mostly associated with cellular stress. In the present study, we started from the evidence that the insertional inactivation of pirin-like gene SAM23877_RS18305 (pirA) by ΦC31 Att/Int system-based vectors in spiramycin-producing strain Streptomyces ambofaciens ATCC 23877 resulted in marked effects on central carbon and energy metabolism gene expression, high sensitivity to oxidative injury and repression of polyketide antibiotic production. By using integrated transcriptomic, proteomic and metabolite profiling, together with genetic complementation, we here show that most of these effects could be traced to the inability of the pirA-defective strain to modulate beta-oxidation pathway, leading to an unbalanced supply of precursor monomers for polyketide biosynthesis. Indeed, in silico protein-protein interaction modeling and in vitro experimental validation allowed us to demonstrate that PirA is a novel redox-sensitive negative modulator of very long-chain acyl-CoA dehydrogenase, which catalyzes the first committed step of the beta-oxidation pathway.Entities:
Keywords: Actinomycetes; Antibiotics; Beta-oxidation of fatty acids; Pirin; Secondary metabolism
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Year: 2018 PMID: 29944936 DOI: 10.1016/j.ymben.2018.06.008
Source DB: PubMed Journal: Metab Eng ISSN: 1096-7176 Impact factor: 9.783