Type VIIb secretion system recruits a dedicated cell wall hydrolase EssH to enable effector secretion by Staphylococcus aureus

Staphylococcus aureus is a pervasive human pathogen that heavily relies on protein secretion to exert its virulence strategies. S. aureus encodes a specialized type VIIb secretion system (T7SSb) that contributes to virulence and persistence in the host. T7SSb supports secretion of small proteins belonging to a WXG100 family as well as larger LXG polymorphic toxins. Secretion of these proteins is facilitated by the T7SSb complex that assembles in the cell envelope from core components EsaA, EssA, EssB, and the conserved ATPase EssC. T7SSb-mediated secretion also requires the cell wall hydrolase EssH that bears a cystine histidine-dependent amidase/peptidase (CHAP) domain. Hereby, we show that the N-terminal domain of EssH functions together with the CHAP domain to support T7SSb secretion. We find that EssH copurifies with the T7SSb core components and is required for the assembly of EsaA across the cell wall. Finally, secreted EssH is released into the extracellular milieu and degraded by the secreted staphylococcal protease, staphopain A. We propose a model to capture the function of the dedicated cell wall hydrolase EssH for T7SSb in S. aureus .