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Fluorescence Lifetime Measurement of Prefibrillar Sickle Hemoglobin Oligomers as a Platform for Drug Discovery in Sickle Cell Disease.

Nagamani VunnamScott HansenDillon C WilliamsMaryJane Olivia BeenChih Hung LoAnil K PandeyCarolyn N PaulsonJohn A RohdeDavid D ThomasJonathan N SachsDavid K Wood
Published in: Biomacromolecules (2022)
The molecular origin of sickle cell disease (SCD) has been known since 1949, but treatments remain limited. We present the first high-throughput screening (HTS) platform for discovering small molecules that directly inhibit sickle hemoglobin (HbS) oligomerization and improve blood flow, potentially overcoming a long-standing bottleneck in SCD drug discovery. We show that at concentrations far below the threshold for nucleation and rapid polymerization, deoxygenated HbS forms small assemblies of multiple α 2 β 2 tetramers. Our HTS platform leverages high-sensitivity fluorescence lifetime measurements that monitor these temporally stable prefibrillar HbS oligomers. We show that this approach is sensitive to compounds that inhibit HbS polymerization with or without modulating hemoglobin oxygen binding affinity. We also report the results of a pilot small-molecule screen in which we discovered and validated several novel inhibitors of HbS oligomerization.
Keyphrases
  • sickle cell disease
  • drug discovery
  • blood flow
  • high throughput
  • small molecule
  • single molecule
  • red blood cell
  • randomized controlled trial
  • single cell
  • binding protein