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Synthesis of Oxorhenium(V) and Oxotechnetium(V) Complexes That Bind to Amyloid‑β Plaques

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Figshare2016-08-09 更新2026-04-29 收录
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https://figshare.com/articles/dataset/Synthesis_of_Oxorhenium_V_and_Oxotechnetium_V_Complexes_That_Bind_to_Amyloid_Plaques/3501872
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Alzheimer’s disease is characterized by the presence of amyloid plaques in the brain. The primary constituents of the plaques are aggregated forms of the amyloid-β (Aβ) peptide. With the goal of preparing technetium-99m complexes that bind to Aβ plaques with the potential to be diagnostic imaging agents for Alzheimer’s disease, new tetradentate ligands capable of forming neutral and lipophilic complexes with oxotechentium­(V) and oxorhenium­(V) were prepared. Nonradioactive isotopes of technetium are not available so rhenium was used as a surrogate for exploratory chemistry. Two planar tetradentate N3O ligands were prepared that form charge-neutral complexes with oxorhenium­(v) as well as a ligand featuring a styrylpyridyl functional group designed to bind to Aβ plaques. All three ligands formed complexes with oxorhenium­(V), and each complex was characterized by NMR spectroscopy, mass spectrometry, and X-ray crystallography. The oxorhenium­(V) complex with a styrylpyridyl functional group binds to Aβ plaques present in post-mortem human brain tissue. The chemistry was extrapolated to technetium-99m at the tracer level for two of the ligands. The resulting oxotechnetium­(V) complexes were sufficiently lipophilic and charge-neutral to suggest that they have the potential to cross the blood–brain barrier but exhibited modest stability with respect to exchange with histidine. The chemistry presented here identifies a strategy to integrate styrylpyridyl functional groups into tetradentate ligands capable of forming complexes with [MO]3+ cores (M = Re or Tc).
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2016-08-09
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