Dora Elisabeth Finkeisen scite author profile

Peptide antibiotics are produced by a wide range of microorganisms. Most of them target the cell envelope, often by inhibiting cell wall synthesis. One of the resistance mechanisms against antimicrobial peptides is a detoxification module consisting of a two-component system and an ABC transporter. Upon the detection of such a compound, the two-component system induces the expression of the ABC transporter, which in turn removes the antibiotic from its site of action, mediating the resistance of the cell. Three such peptide antibiotic-sensing and detoxification modules are present in Bacillus subtilis. Here we show that each of these modules responds to a number of peptides and confers resistance against them. BceRS-BceAB (BceRS-AB) responds to bacitracin, plectasin, mersacidin, and actagardine. YxdJK-LM is induced by a cationic antimicrobial peptide, LL-37. The PsdRS-AB (formerly YvcPQ-RS) system responds primarily to lipid II-binding lantibiotics such as nisin and gallidermin. We characterized the psdRS-AB operon and defined the regulatory sequences within the P psdA promoter. Mutation analysis demonstrated that P psdA expression is fully PsdR dependent. The features of both the P bceA and P psdA promoters make them promising candidates as novel whole-cell biosensors that can easily be adjusted for high-throughput screening.

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Genetic characterization of Bhanja virus and Palma virus, two tick-borne phleboviruses

Dilcher

Alves

Finkeisen

et al. 2012

Virus Genes

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Entwicklung von diagnostischen Methoden zum Nachweis von europäischen humanpathogenen Arboviren

Finkeisen¹

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