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Review
. 2018 Apr;10(2):219-227.
doi: 10.1007/s12551-017-0343-x. Epub 2017 Dec 8.

"Just a spoonful of sugar...": import of sialic acid across bacterial cell membranes

Affiliations
Review

"Just a spoonful of sugar...": import of sialic acid across bacterial cell membranes

Rachel A North et al. Biophys Rev. 2018 Apr.

Abstract

Eukaryotic cell surfaces are decorated with a complex array of glycoconjugates that are usually capped with sialic acids, a large family of over 50 structurally distinct nine-carbon amino sugars, the most common member of which is N-acetylneuraminic acid. Once made available through the action of neuraminidases, bacterial pathogens and commensals utilise host-derived sialic acid by degrading it for energy or repurposing the sialic acid onto their own cell surface to camouflage the bacterium from the immune system. A functional sialic acid transporter has been shown to be essential for the uptake of sialic acid in a range of human bacterial pathogens and important for host colonisation and persistence. Here, we review the state-of-play in the field with respect to the molecular mechanisms by which these bio-nanomachines transport sialic acids across bacterial cell membranes.

Keywords: ABC transporter; NanT; Porins; Sialic acid; Sodium solute symporters; TRAP transporter.

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Conflict of interest statement

Conflict of interest

Rachel A. North declares that she has no conflict of interest. Christopher R. Horne declares that he has no conflict of interest. James S. Davies declares that he has no conflict of interest. Daniela M. Remus declares that she has no conflict of interest. Andrew C. Muscroft-Taylor declares that he has no conflict of interest. Parveen Goyal declares that he has no conflict of interest. Weixiao Yuan Wahlgren declares that she has no conflict of interest. S. Ramaswamy declares that he has no conflict of interest. Rosmarie Friemann declares that she has no conflict of interest. Renwick C. J. Dobson declares that he has no conflict of interest.

Ethical approval

This article does not contain any studies with human participants or animals performed by any of the authors.

Figures

Fig. 1
Fig. 1
Structure of sialic acids and overview of bacterial sialic acid utilisation. a The most common sialic acid, N-acetylneuraminic acid. An asterisk represents positions that are modified to give variation. These include acetyl groups or the less common lactyl, phosphate, succinyl and methyl groups. b Lactone derivative, the third highest detected sialyl metabolite in the human gut. c 9-O-Acetylated derivative, the second highest detected sialyl metabolite in the human gut. d N-Glycolylneuraminic acid. Differing at the C-5 acetamido group, this sialyl metabolite is common in most mammals, but is not synthesised by humans
Fig. 2
Fig. 2
Sialic acid transporter types. Within Gram-negative bacteria, sialic acid must first cross the outer cell membrane before it can be imported into the cell. This can occur by simple diffusion through the non-specific porins, OmpF and OmpC (grouped together). Specific channels, such as NanC, allow for the facilitated diffusion of sialic acid, whereas the NanOU system allows for the active transport of sialic acid. This is mediated by an extracellular uptake protein NanU, which binds sialic acid, the β-barrel NanO and the TonB complex, which energises the transport. Once in the periplasmic space, the processing enzymes NanM (yellow square) and NanS (yellow triangle) are known to mutarotate between the anomeric states of sialic acid and deacetylate the 9 position of 9-O-acetylated derivative, respectively. Some transporter systems require a periplasmic or cell surface-associated substrate binding protein (green circles) which interacts with the membrane component of the respective transporter. Finally, to traverse the inner membrane, bacterial pathogens have evolved multiple mechanisms of sialic acid transport which vary between species. ABC transporters are primary transporters that couple solute translocation with the hydrolysis of ATP by the ATPase domains. TRAP, NanT and SiaT transporters are secondary transporters that couple solute translocation with an electrochemical gradient. It is unclear whether TRAP sialic acid transporters are proton- or sodium ion-dependent, but NanT sialic acid transporters have been shown to be proton-dependent, while SiaT sialic acid transporters have been shown to be sodium ion-dependent. The stoichiometry of ions required for transport is not well understood. YjhB is a putative permease, which is similar in topology to NanT, although it lacks the central hydrophilic domain. While the other transporters are believed to transport N-acetylneuraminic acid, YjhB is suggested to transport less common derivatives. For simplicity, sialic acids are depicted as orange circles, while the membranes are in grey

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