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Sequence Symmetry Analysis as a Signal Detection Tool for Potential Heart Failure Adverse Events in an Administrative Claims Database

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  • Izyan A. Wahab

    (Cyberjaya University College of Medical Sciences)

  • Nicole L. Pratt

    (Sansom Institute, University of South Australia)

  • Lisa Kalisch Ellett

    (Sansom Institute, University of South Australia)

  • Elizabeth E. Roughead

    (Sansom Institute, University of South Australia)

Abstract

Introduction The potential for routine sequence symmetry analysis (SSA) signal detection in health claims databases to detect new safety signals of medicines is unknown. Objective Our objective was to assess the potential utility of SSA as a signal detection tool in health claims data for detecting medicines with potential heart failure (HF) adverse event signals. Methods We applied the SSA method to all subsidized single-ingredient medicines in Australia. The source of data was the Australian Government Department of Veterans’ Affairs (DVA) administrative claims database using data collected between 2002 and 2011. We used first ever HF hospitalization and frusemide initiation as indicators for HF. A signal was considered to be present if the lower limit of the 95 % confidence interval for the adjusted sequence ratio was greater than one. To identify potential new signals of HF, we excluded medicines where HF or edema was listed in the product information (PI) of that medicine or for any other medicine in the same class. We also excluded medicines that were used in HF treatment and medicines indicated for diseases that may contribute to the development of HF. Results We tested 691 medicines. HF signals were detected for 12 % (80/691) using the hospitalization event and 22 % (153/691) using frusemide initiation. Among medicines that did not have HF listed in the PI, SSA found 11 % (44/397) associated with HF hospitalization and 15 % (60/397) associated with frusemide initiation. Of the medicines tested in which no other medicine in the same class had HF or edema in the PI, and where the medicine was not indicated for a disease that is a risk factor for HF, potential new signals were generated for 2–3 % of these medicines tested (12 of 397 medicines using HF hospitalization and 9 of 397 medicines using frusemide initiation). Conclusion SSA generated potential new signals of HF for some anti-glaucoma and anti-dyspepsia medicines. For some of the potential signals, the event is biologically plausible and some have pre-marketing and post-marketing case reports to support the finding. Confirmation of these signals using cohort studies is required.

Suggested Citation

  • Izyan A. Wahab & Nicole L. Pratt & Lisa Kalisch Ellett & Elizabeth E. Roughead, 2016. "Sequence Symmetry Analysis as a Signal Detection Tool for Potential Heart Failure Adverse Events in an Administrative Claims Database," Drug Safety, Springer, vol. 39(4), pages 347-354, April.
  • Handle: RePEc:spr:drugsa:v:39:y:2016:i:4:d:10.1007_s40264-015-0391-8
    DOI: 10.1007/s40264-015-0391-8
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    Cited by:

    1. Ed Whalen & Manfred Hauben & Andrew Bate, 2018. "Time Series Disturbance Detection for Hypothesis-Free Signal Detection in Longitudinal Observational Databases," Drug Safety, Springer, vol. 41(6), pages 565-577, June.
    2. Clare E. King & Nicole L. Pratt & Nichole Craig & Loc Thai & Margaret Wilson & Neillan Nandapalan & Lisa Kalisch Ellet & Eirene C. Behm, 2020. "Detecting Medicine Safety Signals Using Prescription Sequence Symmetry Analysis of a National Prescribing Data Set," Drug Safety, Springer, vol. 43(8), pages 787-795, August.
    3. Kouichi Hosomi & Mai Fujimoto & Kazutaka Ushio & Lili Mao & Juran Kato & Mitsutaka Takada, 2018. "An integrative approach using real-world data to identify alternative therapeutic uses of existing drugs," PLOS ONE, Public Library of Science, vol. 13(10), pages 1-19, October.
    4. Maja Hellfritzsch & Lotte Rasmussen & Jesper Hallas & Anton Pottegård, 2018. "Using the Symmetry Analysis Design to Screen for Adverse Effects of Non-vitamin K Antagonist Oral Anticoagulants," Drug Safety, Springer, vol. 41(7), pages 685-695, July.

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