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AbstractN2‐fixing heterocystous cyanobacteria grow as chains of cells that are connected by proteinaceous septal junctions, which traverse the septal peptidoglycan through nanopores and mediate intercellular molecular transfer. In the model organism Anabaena sp. strain PCC 7120, proteins SepJ, FraC and FraD, which are localized at the cell poles in the intercellular septa, are needed to produce septal junctions. The pentapeptide‐repeat, membrane‐spanning protein HglK has been described to be involved in the deposition of the heterocyst‐specific glycolipid layer, but the hglK mutant also showed intercellular septa broader than in the wild type. Here we found that hglK mutant of Anabaena is impaired in the expression of heterocyst‐related genes coxB2A2C2 (cytochrome c oxidase) and nifHDK (nitrogenase), indicating a defect in heterocyst differentiation. HglK was predominantly localized at the intercellular septa and was required to make long filaments, produce a normal number of nanopores and express full intercellular molecular transfer activity. However, the effects of hglK inactivation were not additive to those of the inactivation of sepJ and/or fraC‐fraD. We suggest that HglK contributes to the architecture of the intercellular septa with an impact on the function of septal junctions.
Heterocyst differentiation, Membrane Proteins, Septal junctions, Cyanobacteria, Anabaena, Pentapeptide-repeat protein, Intercellular communication, Nitrogen fixation, Bacterial Proteins, Bacterial development, Microbial Interactions
Heterocyst differentiation, Membrane Proteins, Septal junctions, Cyanobacteria, Anabaena, Pentapeptide-repeat protein, Intercellular communication, Nitrogen fixation, Bacterial Proteins, Bacterial development, Microbial Interactions
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