The sialate O -acetylesterase EstA from gut Bacteroidetes species enables sialidase-mediated cross-species foraging of 9- O -acetylated sialoglycans.

The gut harbors many symbiotic, commensal, and pathogenic microbes that break down and metabolize host carbohydrates. Sialic acids are prominent outermost carbohydrates on host glycoproteins called mucins and protect underlying glycan chains from enzymatic degradation. Sialidases produced by some members of the colonic microbiota can promote the expansion of several potential pathogens (, , and ) that do not produce sialidases. -Acetyl ester modifications of sialic acids help resist the action of many sialidases and are present at high levels in the mammalian colon. However, some gut bacteria, in turn, produce sialylate--acetylesterases to remove them. Here, we investigated -acetyl ester removal and sialic acid degradation by sialate--acetylesterases and sialidases, respectively, and subsequent utilization of host sialic acids by both commensal and pathogenic strains. foraging studies demonstrated that sialidase-dependent growth on mucin is enabled by EstA, a sialate -acetylesterase acting on glycosidically linked sialylate--acetylesterase substrates, particularly at neutral pH. Biochemical studies suggested that spontaneous migration of -acetyl esters on the sialic acid side chain, which can occur at colonic pH, may serve as a switch controlling EstA-assisted sialic acid liberation. Specifically, EstA did not act on -acetyl esters in their initial 7-position. However, following migration to the 9-position, glycans with -acetyl esters became susceptible to the sequential actions of bacterial esterases and sialidases. We conclude that EstA specifically unlocks the nutritive potential of 9--acetylated mucus sialic acids for foraging by bacteria that otherwise are prevented from accessing this carbon source.