Американское общество гирудотерапии

Impact of Bivalirudin on Ischemia/Reperfusion Injury in Patients with Reperfused STEMI Assessed by Cardiac Magnetic Resonance

Zhang Y, Zou Z, Xu B, Chen B, Ge H, Ding S, Pu J (2024) · Pharmaceuticals · n=42

RCT evidence detailTrial reference
GRADE LowCohort / case series
Sample size of this trial compared with other venous-congestion-flap trialsMarquard JM 20251215Bishop JL 2023843Doğan S 2024570Troeltzsch M 2016330Kucur C 2015260Wang ZD 2022210Lehnhardt M 202196Kruer RM 201459Mozafari N 201056Zhang Y 202442
This trial (highlighted) by sample size alongside other indexed venous-congestion-flap trials. Larger trials generally carry more statistical weight.

Study Profile

Design
small prospective comparative study (n=42) of bivalirudin vs unfractionated heparin in primary PCI for STEMI patients, with serial cardiac magnetic resonance imaging at acute, 1-month, and 3-month follow-up; EARLY Assessment of Myocardial Tissue Characteristics by CMR in STEMI registry (NCT03768453, Shanghai Renji Hospital)
Sample size (n)
42
Intervention
Bivalirudin (n=21) for STEMI primary PCI anticoagulation
Comparator
Unfractionated heparin (n=21) for STEMI primary PCI anticoagulation
Primary endpoint
Myocardial edema volume, microvascular obstruction (MVO) volume/incidence, and intramyocardial hemorrhage (IMH) incidence on CMR
Primary result
Bivalirudin group: significantly less acute myocardial edema; only 4.7% had edema at 1 month vs 33.3% in heparin group; complete edema resolution by 3 months vs persistence in heparin group; significantly lower MVO incidence/volume acutely; significantly lower IMH incidence acutely and at follow-up; corroborated by T2/T1 mapping; bivalirudin associated with attenuated ischemia/reperfusion injury
Follow-up duration
3 months (serial CMR)

Key Findings

  • CMR-quantified myocardial edema, MVO, and IMH all significantly reduced with bivalirudin vs heparin
  • Bivalirudin appears to reduce ischemia/reperfusion injury at the tissue level
  • First imaging-endpoint corroboration of bivalirudin tissue-protective effects in STEMI
  • n=21 per arm — small but adequately powered for primary CMR endpoints
  • Reinforces drug-pathway development of synthetic hirudin derivatives

Limitations

  • Small sample (n=42 total)
  • Single-center registry-based design
  • Open-label (no blinding)
  • Outcomes are imaging surrogates, not hard clinical endpoints
  • Not generalizable beyond STEMI patient population

Clinical Implications

Zhang 2024 adds imaging-based mechanistic evidence to the bivalirudin literature. For ASH, the trial serves as a pharmacology and regulatory reference for distinguishing FDA-approved synthetic hirudin-derivative drug indications (bivalirudin in STEMI) from the K040187 device indication (whole-leech hirudotherapy in microsurgical flap salvage). Not directly applicable to US hirudotherapy clinical practice.

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