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Fluorinated synthetic anion carriers: experimental and computational insights into transmembrane chloride transport. | LitMetric

AI Article Synopsis

  • - Fluorinated tripodal tris-thioureas are effective anion transporters that operate differently than non-fluorinated variants due to their inability to diffuse freely through cell membranes.
  • - These fluorinated transporters depend on oleic acid to form complexes for recycling, while non-fluorinated ones can diffuse on their own and work alongside proton transporters.
  • - By combining molecular dynamics simulations with experimental assays, researchers can better understand and improve the design of these anion transporters for potential medical uses.

Article Abstract

A series of fluorinated tripodal tris-thioureas function as highly active anion transporters across lipid bilayers and cell membranes. Here, we investigate their mechanism of action using anion transport assays in cells and synthetic vesicles and molecular modelling of transporter-lipid interactions. When compared with non-fluorinated analogues, fluorinated compounds demonstrate a different mechanism of membrane transport because the free transporter cannot effectively diffuse through the membrane. As a result, in H/Cl cotransport assays, fluorinated transporters require the presence of oleic acid to form anionic oleate complexes for recycling of the transporter, whereas non-fluorinated analogues readily diffuse through the membrane as free transporters and show synergistic transport with the proton transporter gramicidin. Molecular dynamics simulations revealed markedly stronger transporter-lipid interactions for fluorinated compounds compared with non-fluorinated analogues and hence, higher energy barriers for fluorinated compounds to cross the membrane as free transporters. With use of appropriate proton transporters to ensure measurement of the correct rate-limiting steps, the transport rates determined in synthetic vesicle assays show excellent agreement with the anion transport rates determined in cell-based assays. We conclude that integration of computational and experimental methods provides a strategy to optimise transmembrane anion transporter design for biomedical applications.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6381411PMC
http://dx.doi.org/10.1039/c8sc05155kDOI Listing

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