4.7 Article

Novel chelators based on adamantane-derived semicarbazones and hydrazones that target multiple hallmarks of Alzheimer's disease

Journal

DALTON TRANSACTIONS
Volume 47, Issue 21, Pages 7190-7205

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/c8dt01099d

Keywords

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Funding

  1. National Health and Medical Research Council (NHMRC) Australia [1021607, 1048972]
  2. NHMRC Senior Principal Research Fellowship [1062607]
  3. NHMRC RD Wright Fellowship [1083057]
  4. Australian Research Council [DP1096029, DP150104672, DP150103345, DP1211465, DE170100628]
  5. Sydney Medical School
  6. Judith Jane Mason and Harold Stannett Williams Memorial Foundation National Medical Program Grant
  7. Cancer Institute NSW
  8. National Health and Medical Research Council of Australia [1083057] Funding Source: NHMRC
  9. Australian Research Council [DP1096029, DE170100628] Funding Source: Australian Research Council

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Alzheimer's disease (AD) is characterized by multiple pathological hallmarks, including -amyloid aggregation, oxidative stress, and metal dys-homeostasis. In the absence of treatments addressing its multi-factorial pathology, we designed novel multi-functional adamantane-based semicarbazones and hydrazones (1-12) targeting AD hallmarks. Of these, 2-pyridinecarboxaldehyde (N-adamantan-1-yl)benzoyl-4-amidohydrazone (10) was identified as the lead compound, which demonstrated: (1) pronounced iron chelation efficacy; (2) attenuation of Cu-II-mediated -amyloid aggregation; (3) low cytotoxicity; (4) inhibition of oxidative stress; and (5) favorable characteristics for effective blood-brain barrier permeation. Structure-activity relationships revealed that pyridine-derived hydrazones represent a promising pharmacophore for future design strategies due to their ability to bind critical Fe-II pools. Collectively, the unique multi-functional activity of these agents provides a novel therapeutic strategy for AD treatment.

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