Crystal Structures of Diaryl Hydrazone and Sulfone Stabilizers in Complex with an Amyloidogenic Light Chain Reveal an Alternate Ligand-Binding Cavity

二芳基腙和砜稳定剂与淀粉样蛋白轻链复合物的晶体结构揭示了一种替代的配体结合腔

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Abstract

Stabilization of amyloidogenic immunoglobulin light chains (LCs) by binding of small molecule "kinetic stabilizers" is under development as a novel treatment for light chain amyloidosis. From a high-throughput screen, we previously identified 16 full-length (FL) LC stabilizers from five distinct chemotypes. We then obtained structural biological information on two classes of hits, coumarins and hydantoins, revealing that both chemotypes bind to a pocket at the V(L)-V(L) interface of the FL LC dimer. Here, we report crystal structures of three screening hits from two other chemotypes, diaryl hydrazones and sulfones, in complex with an amyloidogenic FL LC. While two of these hits bind to the previously identified pocket, one diaryl hydrazone binds to a different pocket bisected by the C(2) symmetry axis of the dimer. These data further expand on the FL LC stabilizer-binding surface that could be used in design of more potent FL LC aggregation inhibitors.

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