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חזרה לחיפוש

PREvention of CardIovascular and DiabEtic kidNey Disease in Type 2 Diabetes (PRECIDENTD) שלב IV 6,000 אקראי תווית פתוחה מניעה

מגייס
פרטי הניסויים הקליניים זמינים בעיקר באנגלית. רדאר קליני AI יכול לעזור! לחץ על 'הסבר את המחקר' כדי לצפות ולשוחח על מידע מהמחקר בשפה המועדפת עליך.
ניסוי קליני NCT05390892 (PRECIDENTD) מתקיים כדי לבדוק את מניעה עבור סוכרת סוג 2, מחלת לב וכלי דם טרשתית. זהו מחקר שלב IV מסוג התערבותי שנמצא כעת במצב מגייס. המחקר התחיל ב-26 בספטמבר 2022 ומתוכנן לכלול 6,000 משתתפים. המחקר מנוהל על ידי בית החולים בריגהאם אנד וימנ'ס וצפוי להסתיים ב-1 במרץ 2029. מידע זה עודכן לאחרונה באתר ClinicalTrials.gov ב-21 בנובמבר 2025.
סיכום קצר
PRECIDENTD is a randomized, open label, pragmatic clinical trial designed to compare rates of the total number of cardiovascular, kidney, and death events among two alternative treatments for patients with type 2 diabetes (T2D) and either established atherosclerotic cardiovascular disease (ASCVD) or at high risk for ASCVD. To accomplish this objective, we will randomly assign 6,000 patients with established T2D and A...הצג עוד
כותרת רשמית

PRECIDENTD: PREvention of CardIovascular and DiabEtic kidNey Disease in Type 2 Diabetes

מצבים רפואיים
סוכרת סוג 2מחלת לב וכלי דם טרשתית
פרסומים
מאמרים מדעיים וניירות מחקר שפורסמו על ניסוי קליני זה:
מזהי מחקר נוספים
  • PRECIDENTD
  • 2022p001160
מספר NCT
NCT05390892
תחילת המחקר (בפועל)
2022-09-26
עדכון אחרון שפורסם
2025-11-21
סיום המחקר (מוערך)
2029-03-01
משתתפים (מתוכנן)
6,000
סוג המחקר
התערבותי
שלב
שלב IV
סטטוס
מגייס
מטרה ראשית
מניעה
הקצאת טיפול
אקראי
דגם מתערב
קבוצות מקבילות
עיוורון
אין (מחקר פתוח)
זרועות / התערבויות
קבוצת משתתפים/זרועהתערבות/טיפול
משווה פעילSodium-glucose cotransporter-2 inhibitor (SGLT2i)
Therapy with an SGLT2i with proven cardiovascular benefit. This means either canagliflozin, dapagliflozin, or empagliflozin
SGLT2 inhibitor
Empagliflozin, dapagliflozin, or canagliflozin
משווה פעילGlucagon-like peptide-1 receptor agonist (GLP-1 RA)
Therapy with a GLP-1 RA with proven cardiovascular benefit. This means either dulaglutide, liraglutide, or semaglutide.
GLP-1 receptor agonist
Dulaglutide, liraglutide, semaglutide
מדדי תוצאה ראשיים
מדד תוצאהתיאור המדידהטווח זמן
Total (first and recurrent) cardiovascular, kidney, and death events
total (first and recurrent) number of episodes of myocardial infarction (MI), stroke, arterial revascularization, hospitalization for heart failure, development of end-stage kidney disease, kidney transplantation, and mortality
Through study completion, with an average follow up of approximately 3 years
עוזר השתתפות
קריטריוני זכאות

גילאים מוערכים למחקר
מבוגר, גיל שלישי
גיל מינימלי למחקר
40 Years
מגדרים מוערכים למחקר
הכל

  • Type 2 diabetes based on clinical diagnosis

  • HbA1c ≥6% measured within 12 months prior to screening

  • Secondary prevention cohort (at least 70% of cohort):

    • Age 40 to 80 years
    • Evidence of established atherosclerotic cardiovascular disease (ASCVD), as defined by one or more of the following
    • Coronary heart disease defined by at least one of the following: prior myocardial infarction, prior coronary percutaneous coronary intervention, ≥50% stenosis of a coronary artery documented by invasive or non-invasive imaging (including CT coronary angiography), positive stress test, or coronary artery calcium score >400 Agatston units;
    • Cerebrovascular disease defined by at least one of the following: prior ischemic stroke, prior carotid revascularization procedure, carotid stenosis ≥ 50% documented by X-ray angiography, MR angiography, CT angiography, or Doppler ultrasound;
    • Symptomatic peripheral artery disease defined by at least one of the following: leg symptoms with an ABI ≤ 0.9, leg symptoms with imaging evidence of a stenosis ≥50% in a peripheral artery documented by X-ray angiography, MR angiography, CT angiography, or Doppler ultrasound, or prior amputation for atherosclerotic disease.

  • Primary prevention cohort (capped at 30% of cohort):

    • Age 60-80 years and at least 1 additional high-risk feature:
    • Cardiovascular risk factors/high-risk features:
    • Active smoking (combustible tobacco or marijuana)
    • HbA1c ≥ 8% measured within 12 months prior to screening. The most recent value available at the time of screening will be used for screening and to determine eligibility.
    • Stage 3a CKD, eGFR 45-59 ml/min/1.73m2 measured within 12 months prior to screening. The most recent value available at screening will be used for screening and to determine eligibility.

  • Willingness to be randomly assigned to medication class (SGLT2i or GLP-1 RA or both) and fill prescription through personal pharmacy benefit while having other medications adjusted for safety

  • Willingness to avoid starting a therapy in the alternative treatment group (e.g., if randomized to GLP-1 RA, avoid starting an SGLT2i) unless strongly recommended by the participant's usual care provider.

  • If taking one of the study medication classes, willingness to stop SGLT2i or GLP-1 RA and be randomly assigned to one of the two medication classes

  • Willingness to consent to data collection using the electronic health record and sign a medical release to obtain future medical records from other health care facilities

  • Known or suspected diabetes of other cause (type 1 diabetes, pancreatogenic diabetes, monogenic diabetes, etc.)

  • Any background diabetes medication regimen will be allowed in this pragmatic trial with the following proviso:

    o Participants taking basal-bolus, prandial, or multiple daily injection insulin (MDI) regimens (e.g., short-acting in combination with long-acting insulin, called MDI regimens) are eligible only if the research staff attests that there has been communication with the usual diabetes care provider and that the provider has agreed to manage insulin adjustment with initiation of study medications. If such agreement has not been obtained, participants taking MDI regimens are excluded.

  • History of diabetic ketoacidosis

  • Active diabetic foot ulcer

  • History of pancreatitis

  • Heart failure as a primary reason for hospitalization within the past year

  • Known left ventricular ejection fraction <40%

  • Known urinary albumin-to-creatinine ratio >200 mg/g at screening

  • Estimated glomerular filtration rate (eGFR) less than 45 ml/min/1.73m2 measured within 12 months prior to screening. The most recent value available at screening will be used for screening and to determine eligibility.

  • Known inability to afford study medication through current insurance coverage.

  • If a woman of child-bearing potential, the patient or partner is unwilling to use birth control

  • Active treatment for cancer, planned treatment for cancer, or recent active cancer with likelihood of recurrence or progression, which, in the opinion of the site investigator, has a likelihood of recurrence that would interfere with study therapy prior to 2028

    • Treated cancer with no evidence of disease, no evidence of disease progression, and no planned change in therapy is allowed. Examples of allowable cancers include:
    • Breast cancer stable after active treatment, managed with long-term anti-estrogen therapy
    • Prostate cancer being observed
    • Stage 0 or 1 tumors status post resection or other definitive treatment
    • Other similarly stable cancer comorbidities

  • History of solid organ or bone marrow transplant

  • Allergy to SGLT2 inhibitor or GLP-1 receptor agonist

Brigham and Women's Hospital logoבית החולים בריגהאם אנד וימנ'ס398 מחקרים פעילים לחקור
Patient-Centered Outcomes Research Institute logoPatient-Centered Outcomes Research Institute
הגורם האחראי למחקר
Brendan M. Everett, חוקר ראשי, Associate Physician and Associate Professor, Brigham and Women's Hospital
איש קשר מרכזי למחקר
איש קשר: Brendan Everett, MD, MPH, 617-732-8790, [email protected]
איש קשר: Maureen Malloy, 617-732-8773, [email protected]
8 מיקומי המחקר ב-1 מדינות

Maryland

Johns Hopkins School of Medicine, Baltimore, Maryland, 21205, United States
Jamie Hyman, איש קשר, 443-927-8723, [email protected]
Rita Kalyani, MD, חוקר ראשי
Jodi Segal, MD, חוקר משנה
Dan Ford, MD, חוקר משנה
מגייס

Minnesota

Essentia Health, Duluth, Minnesota, 55805, United States
Leah Tatelovich, איש קשר, 218-576-0480, [email protected]
Catherine Benziger, MD, MPH, חוקר ראשי
מגייס

Missouri

University of Missouri-Columbia, Columbia, Missouri, 65212, United States
Tea Goletiani, איש קשר, 833-970-0046, [email protected]
Camilla Manrique Acevedo, MD, חוקר ראשי
Guido Lastra, MD, חוקר משנה
מגייס

New York

Naomi Berrie Diabetes Center at New York Presbyterian-Columbia University, New York, New York, 10032, United States
Jacqueline Lonier, MD, איש קשר, 212-851-5492, [email protected]
Jacqueline Lonier, MD, חוקר ראשי
Robin Goland, MD, חוקר משנה
מגייס

North Carolina

Duke University Hospital, Durham, North Carolina, 27710, United States
Chad Harrell, איש קשר, 919-668-9049, [email protected]
W. Schuyler Jones, MD, חוקר ראשי
Ranee Chatterjee, MD, חוקר משנה
מגייס

South Carolina

Medical University of South Carolina, Charleston, South Carolina, 29425, United States
Ebony Panaccione, איש קשר, 843-792-4675, [email protected]
Harsha Karanchi, MD, חוקר ראשי
Marc Cornier, MD, חוקר משנה
מגייס

Tennessee

Vanderbilt University Medical Center, Nashville, Tennessee, 37232, United States
Lance Roller, איש קשר, 615-875-6811, [email protected]
Leslee Matheny, MD, חוקר ראשי
Russell Rothman, MD, חוקר משנה
מגייס

Wisconsin

Medical College of Wisconsin, Milwaukee, Wisconsin, 53226, United States
Kailie Roth, איש קשר, 414-805-8104, [email protected]
Jake Decker, MD, חוקר ראשי
Jeffrey Whittle, MD, חוקר משנה
מגייס