A structural model of the human serotonin transporter in an outward-occluded state.
Eva HellsbergGerhard F EckerAnna Stary-WeinzingerLucy R ForrestPublished in: PloS one (2019)
The human serotonin transporter hSERT facilitates the reuptake of its endogenous substrate serotonin from the synaptic cleft into presynaptic neurons after signaling. Reuptake regulates the availability of this neurotransmitter and therefore hSERT plays an important role in balancing human mood conditions. In 2016, the first 3D structures of this membrane transporter were reported in an inhibitor-bound, outward-open conformation. These structures revealed valuable information about interactions of hSERT with antidepressant drugs. Nevertheless, the question remains how serotonin facilitates the specific conformational changes that open and close pathways from the synapse and to the cytoplasm as required for transport. Here, we present a serotonin-bound homology model of hSERT in an outward-occluded state, a key intermediate in the physiological cycle, in which the interactions with the substrate are likely to be optimal. Our approach uses two template structures and includes careful refinement and comprehensive computational validation. According to microsecond-long molecular dynamics simulations, this model exhibits interactions between the gating residues in the extracellular pathway, and these interactions differ from those in an outward-open conformation of hSERT bound to serotonin. Moreover, we predict several features of this state by monitoring the intracellular gating residues, the extent of hydration, and, most importantly, protein-ligand interactions in the central binding site. The results illustrate common and distinct characteristics of these two transporter states and provide a starting point for future investigations of the transport mechanism in hSERT.
Keyphrases
- molecular dynamics simulations
- endothelial cells
- minimally invasive
- induced pluripotent stem cells
- molecular docking
- pluripotent stem cells
- molecular dynamics
- major depressive disorder
- small molecule
- social media
- physical activity
- depressive symptoms
- spinal cord injury
- current status
- protein protein
- prefrontal cortex
- drug induced