Abstract
Adaptive immune responses to commensal flagellins are hallmarks of Crohn's disease, but it is unclear whether flagellins themselves promote inflammation or whether flagellated commensals can also be colitogenic. Here, we show that the arrangement of motility loci and the diversity of encoded flagellins can separate flagellated gut-derived Clostridia into at least 2 functionally distinct groups. In gnotobiotic mice, both groups induce tolerogenic responses but only one group promoted tissue inflammation following barrier disruption. Accordingly, specific flagellins expressed by members of this pro-inflammatory group displayed a heightened capacity for TLR5 activation which could be altered by modification of a defined region of the flagellin D0 domain. Finally, bacteria belonging to the pro-inflammatory group were found to be elevated in Crohn's disease biopsies. Collectively, our study identified key features of specific commensal bacteria that possess colitogenic potential and revealed one mechanism whereby these organisms can potentially initiate intestinal inflammation.