Biofilm formation on human immune cells is a multicellular predation strategy of Vibrio cholerae

Lucia Vidakovic(University of Basel), Sofya Mikhaleva(École Polytechnique Fédérale de Lausanne), Hannah Jeckel(Philipps University of Marburg), Valerya Nisnevich(Weizmann Institute of Science), Kerstin Strenger(University of Basel), Konstantin Neuhaus(Philipps University of Marburg), K. N. Ganesan and T. S. Raveendran(Max Planck Institute for Terrestrial Microbiology), Noa Bossel Ben‐Moshe(Weizmann Institute of Science), Marina Aznaourova(Philipps University of Marburg), Kazuki Nosho(University of Basel), Antje Drescher(University of Basel), Bernd Schmeck(Philipps University of Marburg), Leon N. Schulte(Philipps University of Marburg), Alexandre Persat(École Polytechnique Fédérale de Lausanne), Roi Avraham(Weizmann Institute of Science), Knut Drescher(University of Basel)
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Abstract

Biofilm formation is generally recognized as a bacterial defense mechanism against environmental threats, including antibiotics, bacteriophages, and leukocytes of the human immune system. Here, we show that for the human pathogen Vibrio cholerae, biofilm formation is not only a protective trait but also an aggressive trait to collectively predate different immune cells. We find that V. cholerae forms biofilms on the eukaryotic cell surface using an extracellular matrix comprising primarily mannose-sensitive hemagglutinin pili, toxin-coregulated pili, and the secreted colonization factor TcpF, which differs from the matrix composition of biofilms on other surfaces. These biofilms encase immune cells and establish a high local concentration of a secreted hemolysin to kill the immune cells before the biofilms disperse in a c-di-GMP-dependent manner. Together, these results uncover how bacteria employ biofilm formation as a multicellular strategy to invert the typical relationship between human immune cells as the hunters and bacteria as the hunted.


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