Identification of Hypoxia-Inducible Factor-2alpha Activators for Chronic Kidney Disease Anemia

Information

  • Research Project
  • 10133642
  • ApplicationId
    10133642
  • Core Project Number
    R01DK118297
  • Full Project Number
    5R01DK118297-05
  • Serial Number
    118297
  • FOA Number
    PA-16-374
  • Sub Project Id
  • Project Start Date
    8/10/2018 - 6 years ago
  • Project End Date
    4/30/2022 - 2 years ago
  • Program Officer Name
    GOSSETT, DANIEL ROBERT
  • Budget Start Date
    5/1/2021 - 3 years ago
  • Budget End Date
    4/30/2022 - 2 years ago
  • Fiscal Year
    2021
  • Support Year
    05
  • Suffix
  • Award Notice Date
    3/30/2021 - 3 years ago
Organizations

Identification of Hypoxia-Inducible Factor-2alpha Activators for Chronic Kidney Disease Anemia

PROJECT SUMMARY Anemia is a common and significant complication of chronic kidney disease (CKD), leading to multiple adverse consequences including, increased hospitalizations and mortality, cardiovascular disease, cognitive impairment, and diminished quality of life. Nearly half of all patients with stage 3-5 CKD experience anemia. In these patients, the underlying cause is from the diminished kidney production of erythropoietin (EPO). EPO is a glycoprotein cytokine secreted by the kidney in response to low oxygen stress to stimulate red blood cell production in the bone marrow. The hypoxia-inducible factor-2 alpha (HIF-2?) forms heterodimer with aryl hydrocarbon receptor nuclear translocator (ARNT) to form a productive transcription factor that drives physiological EPO expression by binding to the hypoxia response element (HRE) upstream of the EPO gene. Our detailed structural elucidation of the multi-domain heterodimeric complex of HIF-2?/ARNT has allowed Certain small-molecules such as PT2385 and OX3 can act as inhibitors of HIF-2? by disrupting the HIF-2?/ARNT heterodimer. We hypothesize that other small-molecules can be identified to stabilize the HIF-2?/ARNT heterodimer and act as activators. However, no attempts have yet been undertaken to identify HIF-2? activators. Driven by our recent crystallographic discovery of multiple ligand-binding cavities within this heterodimer, we designed and conducted small pilot screens based on a sensitive biochemical protein-protein interaction assay. These efforts allowed the identification of small- molecules that biochemically stabilize the HIF-2?/ARNT heterodimer and led to enhanced EPO expression within cells. In response to new appreciation for its drug-binding potentials. NIDDK PA-16-374, we now propose to conduct a comprehensive high-throughput screen using a 350,000-compound library, together with the suite of secondary and tertiary confirmatory assays to identify HIF-2?/-ARNT selective activators for preclinical development. These activators will have substantial advantages over the current treatments involving recombinant EPO injections, and should be significantly safer and more effective than the prolyl-hydroxylase inhibitors undergoing development.

IC Name
NATIONAL INSTITUTE OF DIABETES AND DIGESTIVE AND KIDNEY DISEASES
  • Activity
    R01
  • Administering IC
    DK
  • Application Type
    5
  • Direct Cost Amount
    344026
  • Indirect Cost Amount
    27522
  • Total Cost
    371548
  • Sub Project Total Cost
  • ARRA Funded
    False
  • CFDA Code
    847
  • Ed Inst. Type
  • Funding ICs
    NIDDK:371548\
  • Funding Mechanism
    Non-SBIR/STTR RPGs
  • Study Section
    ZRG1
  • Study Section Name
    Special Emphasis Panel
  • Organization Name
    UNIVERSITY OF OXFORD
  • Organization Department
  • Organization DUNS
    226694883
  • Organization City
    OXFORD
  • Organization State
  • Organization Country
    UNITED KINGDOM
  • Organization Zip Code
    OX1 2JD
  • Organization District
    UNITED KINGDOM