Allosteric effects of the coupling cation in melibiose transporter MelB
2026
Parameswaran Hariharan | Yuqi Shi | Amirhossein Bakhtiiari | Ruibin Liang | Rosa Viner | Lan Guan
The major facilitator superfamily (MFS) transporters play significant roles in human health and disease. Salmonella enterica serovar Typhimurium melibiose permease (MelBSt) catalyzes the symport of galactosides with Na+, H+, or Li+ and is a prototype of MFS transporters. We published the structures of MelBSt in both inward- and outward-facing conformations, bound to galactoside or Na+, and proposed that positive cooperativity of the co-transported solutes is crucial for the symport mechanism. Here, we elucidated the underlying mechanisms by analyzing MelBSt dynamics and the effects of melibiose, Na+, or both using hydrogen-deuterium exchange mass spectrometry (HDX-MS). We also refined the determinants of sugar recognition by solving the crystal structures of a uniporter D59C MelBSt complexed with melibiose and other sugars, and by identifying a critical water molecule involved in sugar recognition. Our integrated studies, combining structures, HDX-MS, and molecular dynamics simulations, support the conclusion that sugar-binding affinity is directly correlated with protein dynamics. Na+ acts as an allosteric activator, reducing the flexibility of dynamic residues in the sugar-binding site and in the cytoplasmic gating salt-bridge network, thereby increasing sugar-binding affinity. This study provides a molecular-level framework of the symport mechanism that could serve as a general model for cation-coupled symporters.
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