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Cyclic di-GMP in the control of multicellular differentiation in antibiotic-producing bacteria Streptomyces.

Subject Area Metabolism, Biochemistry and Genetics of Microorganisms
Term from 2016 to 2022
Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 282982160
 
Streptomyces are the most abundant source of clinically important antibiotics and other natural products used in human medicine. The production of these secondary metabolites is temporally and genetically coordinated with a complex developmental life cycle involving growth as vegetative mycelium of branching hyphae and dispersion via spores formed on specialized reproductive structures called aerial hyphae. We have recently discovered that the nucleotide second messenger c-di-GMP, which is produced by GGDEF-domain proteins and degraded by either EAL- or HD-GYP-domain proteins, plays a crucial role in controlling Streptomyces development. We identified the developmental master regulator BldD as a first c-di-GMP effector in the genus Streptomyces and demonstrated that BldD binds a tetrameric form of c-di-GMP, which results in transcription factor dimerization and effective repression of sporulation genes during vegetative growth. However, our knowledge about c-di-GMP signalling components in Streptomyces is still very limited. The aim of the proposed work is to systematically analyse and characterize in molecular detail the functions and regulatory aspects of all GGDEF, EAL, HD-GYP domain proteins in Streptomyces venezuelae. My initial data show that four of the c-di-GMP metabolizing enzymes have an impact on differentiation and are under the control of multiple developmental regulators but the underlying mechanisms are not understood. Moreover, in my pull-down experiments, which led to the identification of BldD as a c-di-GMP effector protein, multiple other putative c-di-GMP binding proteins were enriched. To validate these candidates as c-di-GMP effectors and to uncover their function(s) is planned in this proposal. Altogether, the proposed research aims at finding the mechanism(s) of action of these c-di-GMP signalling components, elucidation of their position(s) in cellular regulatory pathways and uncovering of their physiological role(s). This work will greatly improve our understanding of Streptomyces physiology and c-di-GMP signalling in a new physiological context involving multicellular differentiation and secondary metabolite production and can contribute to a better exploitation of genetic engineering in Streptomyces for the production of antibiotics.
DFG Programme Independent Junior Research Groups
 
 

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