Synergy and remarkable specificity of antimicrobial peptides in vivo using a systematic knockout approach

Antimicrobial peptides (AMPs) are host-encoded antibiotics that combat invading microorganisms. These short, cationic peptides have been implicated in many biological processes, primarily involving innate immunity. In vitro studies have shown AMPs kill bacteria and fungi at physiological concentrations, but little validation has been done in vivo. We utilized CRISPR gene editing to delete all known immune-inducible AMPs of Drosophila, namely: 4 Attacins, 4 Cecropins, 2 Diptericins, Drosocin, Drosomycin, Metchnikowin and Defensin. Using individual and multiple knockouts, including flies lacking all 14 AMP genes, we characterize the in vivo function of individual and groups of AMPs against diverse bacterial and fungal pathogens. We found that Drosophila AMPs act primarily against Gram-negative bacteria and fungi, contributing either additively or synergistically. We also describe remarkable specificity wherein certain AMPs contribute the bulk of microbicidal activity against specific pathogens, providing functional demonstrations of highly specific AMP-pathogen interactions in an in vivo setting.

Synergy and remarkable specificity of antimicrobial peptides in vivo using a systematic knockout approach

Functional characterization of Drosophila melanogaster immune effectors

Simple optical nanomotion method for single-bacterium viability and antibiotic response testing

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

Functional characterization of Drosophila melanogaster immune effectors

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

Simple optical nanomotion method for single-bacterium viability and antibiotic response testing