The oligopeptide transport system of Bacillus subtilis plays a role in the initiation of sporulation

生物 枯草芽孢杆菌 操纵子 突变体 寡肽 生物化学 肽聚糖 氨基酸 信号肽 肽序列 突变 基因 细菌 遗传学
作者
M. Perego,Christopher F. Higgins,Stephen R. Pearce,Martin J. Gallagher,J A Hoch
出处
期刊:Molecular Microbiology [Wiley]
卷期号:5 (1): 173-185 被引量:329
标识
DOI:10.1111/j.1365-2958.1991.tb01838.x
摘要

Bacillus subtilis spo0K mutants are blocked at the first step in sporulation. The spo0K strain was found to contain two mutations: one was linked to the trpS locus, and the other was elsewhere on the chromosome. The mutation linked to trpS was responsible for the sporulation defect (spo-). The unlinked mutation enhanced this sporulation deficiency but had no phenotype on its own. The spo- mutation was located in an operon of five genes highly homologous to the oligopeptide transport (Opp) system of Gram-negative species. Studies with toxic peptide analogues showed that this operon does indeed encode a peptide-transport system. However, unlike the Opp system of Salmonella typhimurium, one of the two ATP-binding proteins, OppF, was not required for peptide transport or for sporulation. The OppA peptide-binding protein, which is periplasmically located in Gram-negative species, has a signal sequence characteristic of lipoproteins with an amino-terminal lipo-amino acid anchor. Cellular location studies revealed that OppA was associated with the cell during exponential growth, but was released into the medium in stationary phase. A major role of the Opp system in Gram-negative bacteria is the recycling of cell-wall peptides as they are released from the growing peptidoglycan. We postulate that the accumulation of such peptides may play a signalling role in the initiation of sporulation, and that the sporulation defect in opp mutants results from an inability to transport these peptides.
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