Counterclockwise rotation of the flagellum promotes biofilm initiation in Helicobacter pylori .

Autor: Liu X; Department of Microbiology and Environmental Toxicology, University of California, Santa Cruz, California, USA., Lertsethtakarn P; Department of Microbiology and Environmental Toxicology, University of California, Santa Cruz, California, USA., Mariscal VT; Department of Microbiology and Environmental Toxicology, University of California, Santa Cruz, California, USA., Yildiz F; Department of Microbiology and Environmental Toxicology, University of California, Santa Cruz, California, USA., Ottemann KM; Department of Microbiology and Environmental Toxicology, University of California, Santa Cruz, California, USA.
Jazyk: angličtina
Zdroj: MBio [mBio] 2024 Jun 12; Vol. 15 (6), pp. e0044024. Date of Electronic Publication: 2024 May 03.
DOI: 10.1128/mbio.00440-24
Abstrakt: Motility promotes biofilm initiation during the early steps of this process: microbial surface association and attachment. Motility is controlled in part by chemotaxis signaling, so it seems reasonable that chemotaxis may also affect biofilm formation. There is a gap, however, in our understanding of the interactions between chemotaxis and biofilm formation, partly because most studies analyzed the phenotype of only a single chemotaxis signaling mutant, e.g., cheA . Here, we addressed the role of chemotaxis in biofilm formation using a full set of chemotaxis signaling mutants in Helicobacter pylori , a class I carcinogen that infects more than half the world's population and forms biofilms. Using mutants that lack each chemotaxis signaling protein, we found that chemotaxis signaling affected the biofilm initiation stage, but not mature biofilm formation. Surprisingly, some chemotaxis mutants elevated biofilm initiation, while others inhibited it in a manner that was not tied to chemotaxis ability or ligand input. Instead, the biofilm phenotype correlated with flagellar rotational bias. Specifically, mutants with a counterclockwise bias promoted biofilm initiation, e.g., ∆ cheA , ∆ cheW , or ∆ cheV1 ; in contrast, those with a clockwise bias inhibited it, e.g., ∆ cheZ , ∆ chePep , or ∆ cheV3 . We tested this correlation using a counterclockwise bias-locked flagellum, which induced biofilm formation independent of the chemotaxis system. These CCW flagella, however, were not sufficient to induce biofilm formation, suggesting there are downstream players. Overall, our work highlights the new finding that flagellar rotational direction promotes biofilm initiation, with the chemotaxis signaling system operating as one mechanism to control flagellar rotation.
Importance: Chemotaxis signaling systems have been reported to contribute to biofilm formation in many bacteria; however, how they regulate biofilm formation remains largely unknown. Chemotaxis systems are composed of many distinct kinds of proteins, but most previous work analyzed the biofilm effect of loss of only a few. Here, we explored chemotaxis' role during biofilm formation in the human-associated pathogenic bacterium Helicobacter pylori . We found that chemotaxis proteins are involved in biofilm initiation in a manner that correlated with how they affected flagellar rotation. Biofilm initiation was high in mutants with counterclockwise (CCW) flagellar bias and low in those with clockwise bias. We supported the idea that a major driver of biofilm formation is flagellar rotational direction using a CCW-locked flagellar mutant, which stays CCW independent of chemotaxis input and showed elevated biofilm initiation. Our data suggest that CCW-rotating flagella, independent of chemotaxis inputs, are a biofilm-promoting signal.
Competing Interests: The authors declare no conflict of interest.
Databáze: MEDLINE