Chromium(III) ion and thyroxine cooperate to stabilize the transthyretin tetramer and suppress in vitro amyloid fibril formation

Abstract

Transthyretin (TTR) amyloid fibril formation, which is triggered by the dissociation of tetrameric TTR, appears to be the causative factor in familial amyloidotic polyneuropathy and senile systemic amyloidosis. Binding of thyroxine (T₄), a native ligand of TTR, stabilizes the tetramer, but the bioavailability of T₄ for TTR binding is limited due to the preferential binding of T₄ to globulin, the major T₄ carrier in plasma. Here, we show that Cr³⁺ increased the T₄‐binding capacity of wild‐type (WT) and amyloidogenic V30M‐TTR. Moreover, we demonstrate that Cr³⁺ and T₄ cooperatively suppressed in vitro fibril formation due to the stabilization of WT‐TTR and V30M‐TTR.