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Variability of Activated Clotting Time by Site of Sample Draw During Percutaneous Coronary Intervention: A Prospective Single-Center Study. | LitMetric

AI Article Synopsis

  • The ACT assay monitors anticoagulation therapy with unfractionated heparin during PCI, raising concerns about differences in ACT values from different arterial sites.
  • A study measured simultaneous ACT values from both the access sheath and guide catheter in patients, revealing that guide catheter values were significantly higher on average.
  • The findings suggest that the increased ACT from the guide catheter could be influenced by factors like heparin dosage and diabetes status, indicating a need for further research on its biological basis and implications for clinical practice.

Article Abstract

The activated clotting time (ACT) assay is used to monitor and titrate anticoagulation therapy with unfractionated heparin during percutaneous coronary intervention (PCI). Observations at our institution suggested a considerable difference between ACT values drawn from varying arterial sites, prompting the current study. Patients undergoing PCI with unfractionated heparin therapy were prospectively enrolled. Simultaneous arterial blood samples were drawn from the access sheath and the coronary guide catheter. Differences between Hemochron ACT values were determined, and potential interactions with clinical variables were analyzed. Immediately postprocedure, the simultaneous mean guide and sheath ACTs were 327 ± 62 seconds and 257 ± 44 seconds, respectively, with a mean difference of 70 ± 60 seconds (P < .001). Nearly all (90%) ACT values obtained via the guide catheter were higher than the concurrent ACT drawn from the sheath. Logistic regression analysis demonstrated that lower weight-adjusted heparin doses and absence of diabetes were associated with a greater difference between the ACT values. We conclude that the ACT value is substantially greater when assessed via the guide catheter versus the access sheath. Although the biological mechanisms require further study, this difference should be considered when managing anticoagulation during PCI and when reporting ACT as part of research protocols.

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Source
http://dx.doi.org/10.1177/0003319721992237DOI Listing

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