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Active Not Recruiting INTERVENTIONAL NCT04733534

An Open-Label Intervention Trial to Reduce Senescence and Improve Frailty in Adult Survivors of Childhood Cancer

SEN-SURVIVORS: An Open-Label Intervention Trial to Reduce Senescence and Improve Frailty in Adult Survivors of Childhood Cancer

Sponsor: National Cancer Institute (NCI)

Updated 20 times since 2021 Last updated: Apr 23, 2026 Started: Jun 6, 2022 Primary completion: Dec 1, 2026 Completion: Dec 1, 2027
This information is for research purposes only and is not medical advice. Consult a healthcare provider before making any medical decision.

Listed as NCT04733534, this observational or N/A phase trial focuses on Childhood Cancer and Frailty and remains ongoing. Sponsored by National Cancer Institute (NCI), it has been updated 20 times since 2022, reflecting substantial change activity. This study contributes to the evolving evidence base for cancer treatment protocols.

Study Description(click to expand)

Eligible subjects who meet inclusion criteria will be randomized, stratified on sex, 1:1 and age ( ≥40 vs \< 40) to receive Dasatinib (100 mg/day) plus Quercetin (500 mg twice daily) on days 1, 2, 3, 30, 31, and 32 taken orally or Fisetin (20 mg/kg/day) alone on days 1, 2, 30 and 31 taken orally. At the visit on day 7, we will assess blood CD3+ T lymphocyte p16\^INK4A mRNA and other markers of inflammation and senescence to verify that senescent cells have been cleared by the intervention. Post-treatment follow-up will occur on day 60 (primary endpoints) and day 150 to assess the permanence of change after completion of the trial. Treatment adherence will be confirmed by the study coordinator who will administer the Dasatinib + Quercetin in clinic on days 1, 2, 3, 30, 31, and 32 or Fisetin alone on days 1, 2, 30 and 31.

Eligible subjects who meet inclusion criteria will be randomized, stratified on sex, 1:1 and age ( ≥40 vs \< 40) to receive Dasatinib (100 mg/day) plus Quercetin (500 mg twice daily) on days 1, 2, 3, 30, 31, and 32 taken orally or Fisetin (20 mg/kg/day) alone on days 1, 2, 30 and 31 taken orally. At the visit on day 7, we will assess blood CD3+ T lymphocyte p16\^INK4A mRNA and other markers of inflammation and senescence to verify that senescent cells have been cleared by the intervention. Post-treatment follow-up will occur on day 60 (primary endpoints) and day 150 to assess the permanence of change after completion of the trial. Treatment adherence will be confirmed by the study coordinator who will administer the Dasatinib + Quercetin in clinic on days 1, 2, 3, 30, 31, and 32 or Fisetin alone on days 1, 2, 30 and 31.

Status Flow

~Mar 2021 – ~Jun 2021 · 3 months · monthly snapshot~Jun 2021 – ~Sep 2021 · 3 months · monthly snapshot~Sep 2021 – ~Oct 2021 · 30 days · monthly snapshot~Oct 2021 – ~Dec 2021 · 2 months · monthly snapshot~Dec 2021 – ~Jan 2022 · 31 days · monthly snapshot~Jan 2022 – ~Feb 2022 · 31 days · monthly snapshot~Feb 2022 – ~Apr 2022 · 59 days · monthly snapshot~Apr 2022 – ~May 2022 · 30 days · monthly snapshot~May 2022 – ~Jun 2022 · 31 days · monthly snapshot~Jun 2022 – ~Jul 2022 · 30 days · monthly snapshot~Jul 2022 – ~Jul 2023 · 12 months · monthly snapshot~Jul 2023 – ~Sep 2023 · 2 months · monthly snapshot~Sep 2023 – ~Jul 2024 · 10 months · monthly snapshot~Jul 2024 – ~Sep 2024 · 2 months · monthly snapshot~Sep 2024 – ~Jan 2025 · 4 months · monthly snapshot~Jan 2025 – ~Apr 2025 · 3 months · monthly snapshot~Apr 2025 – ~Sep 2025 · 5 months · monthly snapshot~Sep 2025 – ~Feb 2026 · 5 months · monthly snapshot~Feb 2026 – ~Apr 2026 · 3 months · monthly snapshotApr 28, 2026 – present · 2 months · daily API

Change History

20 versions recorded
  1. Apr 28, 2026 — Present [daily]

    Active Not Recruiting

    Phase: PHASE2None

  2. Feb 2026 — Apr 2026 [monthly]

    Active Not Recruiting PHASE2

  3. Sep 2025 — Feb 2026 [monthly]

    Active Not Recruiting PHASE2

    Status: RecruitingActive Not Recruiting

  4. Apr 2025 — Sep 2025 [monthly]

    Recruiting PHASE2

  5. Jan 2025 — Apr 2025 [monthly]

    Recruiting PHASE2

Show 15 earlier versions
  1. Sep 2024 — Jan 2025 [monthly]

    Recruiting PHASE2

  2. Jul 2024 — Sep 2024 [monthly]

    Recruiting PHASE2

  3. Sep 2023 — Jul 2024 [monthly]

    Recruiting PHASE2

  4. Jul 2023 — Sep 2023 [monthly]

    Recruiting PHASE2

  5. Jul 2022 — Jul 2023 [monthly]

    Recruiting PHASE2

  6. Jun 2022 — Jul 2022 [monthly]

    Recruiting PHASE2

  7. May 2022 — Jun 2022 [monthly]

    Recruiting PHASE2

  8. Apr 2022 — May 2022 [monthly]

    Recruiting PHASE2

    Status: Not Yet RecruitingRecruiting

  9. Feb 2022 — Apr 2022 [monthly]

    Not Yet Recruiting PHASE2

  10. Jan 2022 — Feb 2022 [monthly]

    Not Yet Recruiting PHASE2

  11. Dec 2021 — Jan 2022 [monthly]

    Not Yet Recruiting PHASE2

  12. Oct 2021 — Dec 2021 [monthly]

    Not Yet Recruiting PHASE2

  13. Sep 2021 — Oct 2021 [monthly]

    Not Yet Recruiting PHASE2

  14. Jun 2021 — Sep 2021 [monthly]

    Not Yet Recruiting PHASE2

  15. Mar 2021 — Jun 2021 [monthly]

    Not Yet Recruiting PHASE2

    First recorded

Eligibility Summary

This is a first-in survivor pilot study with the goal of establishing preliminary evidence of efficacy, safety, and tolerability of two senolytic regimens to reduce markers of cellular senescence (primary outcome: p16\^INK4a) and improve frailty (primary outcome: walking speed) in adult survivors of childhood cancer. If successful, this pilot would provide the preliminary evidence needed for a phase 2, randomized, placebo-controlled trial to establish efficacy. Primary Objective * The primary aim of this proposal is to test the efficacy of two, short duration senolytic regimens: 1) combination of Dasatinib plus Quercetin and 2) Fisetin alone, to improve walking speed and decrease senescent cell abundance in blood (p16\^INKA): * Primary endpoints of this trial will be change in walking speed and senescent cell abundance in blood (p16\^INK4A) determined at baseline and again at 60 days, within an individual arm. Extended follow up at 150 days will assess the permanence of change after completion of the trial. Secondary endpoints of this trial will be effect of intervention on additional measures of frailty (beyond walking speed; Fried criteria) and on other cell senescence markers, markers of inflammation, insulin resistance, bone resorption, and cognitive function. Secondary Objectives The secondary aim is to test the safety and tolerability of two different senolytic therapies. Exploratory Objectives * To compare the efficacy of the two senolytic regimens in improving walking speed and decreasing senescent cell abundance * To evaluate the longitudinal pattern in measures of frailty.

Contact Information

Sponsor contact:
  • National Cancer Institute (NCI)
  • National Institutes of Health (NIH)
  • St. Jude Children's Research Hospital
Data source: ClinicalTrials.gov

For direct contact, visit the study record on ClinicalTrials.gov .

Study Locations