Reasons for disparity in statin adherence rates between clinical trials and real-world observations: A review

Alexander Vonbank; Heinz Drexel; Stefan Agewall; Basil S. Lewis; Joern F. Dopheide; Keld Kjeldsen; Claudio Ceconi; Gianluigi Savarese; Giuseppe Rosano; Sven Wassmann; Alexander Niessner; Thomas Andersen Schmidt; Christoph H. Saely; Iris Baumgartner; Juan Tamargo

doi:10.1093/ehjcvp/pvy028

Reasons for disparity in statin adherence rates between clinical trials and real-world observations: A review

Alexander Vonbank, Heinz Drexel^*, Stefan Agewall, Basil S. Lewis, Joern F. Dopheide, Keld Kjeldsen, Claudio Ceconi, Gianluigi Savarese, Giuseppe Rosano, Sven Wassmann, Alexander Niessner, Thomas Andersen Schmidt, Christoph H. Saely, Iris Baumgartner, Juan Tamargo

^*Corresponding author af dette arbejde

Institut for Klinisk Medicin

18 Citationer (Scopus)

Abstract

With statins, the reported rate of adverse events differs widely between randomized clinical trials (RCTs) and observations in clinical practice, the rates being 1–2% in RCTs vs. 10–20% in the so-called real world. One possible explanation is the claim that RCTs mostly use a run-in period with a statin. This would exclude intolerant patients from remaining in the trial and therefore favour a bias towards lower rates of intolerance. We here review data from RCTs with more than 1000 participants with and without a run-in period, which were included in the Cholesterol Treatment Trialists Collaboration. Two major conclusions arise: (i) the majority of RCTs did not have a test dose of a statin in the run-in phase. (ii) A test dose in the run-in phase was not associated with a significantly improved adherence rate within that trial when compared to trials without a test dose. Taken together, the RCTs of statins reviewed here do not suggest a bias towards an artificially higher adherence rate because of a run-in period with a test dose of the statin. Other possible explanations for the apparent disparity between RCTs and real-world observations are also included in this review albeit mostly not supported by scientific data.

Originalsprog	Engelsk
Tidsskrift	European Heart Journal - Cardiovascular Pharmacotherapy
Vol/bind	4
Udgave nummer	4
Sider (fra-til)	230-236
Antal sider	7
ISSN	2055-6837
DOI	https://doi.org/10.1093/ehjcvp/pvy028
Status	Udgivet - 1 okt. 2018

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10.1093/ehjcvp/pvy028

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Vonbank, A., Drexel, H., Agewall, S., Lewis, B. S., Dopheide, J. F., Kjeldsen, K., Ceconi, C., Savarese, G., Rosano, G., Wassmann, S., Niessner, A., Schmidt, T. A., Saely, C. H., Baumgartner, I., & Tamargo, J. (2018). Reasons for disparity in statin adherence rates between clinical trials and real-world observations: A review. European Heart Journal - Cardiovascular Pharmacotherapy, 4(4), 230-236. https://doi.org/10.1093/ehjcvp/pvy028

Vonbank, A, Drexel, H, Agewall, S, Lewis, BS, Dopheide, JF, Kjeldsen, K, Ceconi, C, Savarese, G, Rosano, G, Wassmann, S, Niessner, A, Schmidt, TA, Saely, CH, Baumgartner, I & Tamargo, J 2018, 'Reasons for disparity in statin adherence rates between clinical trials and real-world observations: A review', European Heart Journal - Cardiovascular Pharmacotherapy, bind 4, nr. 4, s. 230-236. https://doi.org/10.1093/ehjcvp/pvy028

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abstract = "With statins, the reported rate of adverse events differs widely between randomized clinical trials (RCTs) and observations in clinical practice, the rates being 1–2% in RCTs vs. 10–20% in the so-called real world. One possible explanation is the claim that RCTs mostly use a run-in period with a statin. This would exclude intolerant patients from remaining in the trial and therefore favour a bias towards lower rates of intolerance. We here review data from RCTs with more than 1000 participants with and without a run-in period, which were included in the Cholesterol Treatment Trialists Collaboration. Two major conclusions arise: (i) the majority of RCTs did not have a test dose of a statin in the run-in phase. (ii) A test dose in the run-in phase was not associated with a significantly improved adherence rate within that trial when compared to trials without a test dose. Taken together, the RCTs of statins reviewed here do not suggest a bias towards an artificially higher adherence rate because of a run-in period with a test dose of the statin. Other possible explanations for the apparent disparity between RCTs and real-world observations are also included in this review albeit mostly not supported by scientific data.",

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author = "Alexander Vonbank and Heinz Drexel and Stefan Agewall and Lewis, {Basil S.} and Dopheide, {Joern F.} and Keld Kjeldsen and Claudio Ceconi and Gianluigi Savarese and Giuseppe Rosano and Sven Wassmann and Alexander Niessner and Schmidt, {Thomas Andersen} and Saely, {Christoph H.} and Iris Baumgartner and Juan Tamargo",

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T1 - Reasons for disparity in statin adherence rates between clinical trials and real-world observations

T2 - A review

AU - Vonbank, Alexander

AU - Drexel, Heinz

AU - Agewall, Stefan

AU - Lewis, Basil S.

AU - Dopheide, Joern F.

AU - Kjeldsen, Keld

AU - Ceconi, Claudio

AU - Savarese, Gianluigi

AU - Rosano, Giuseppe

AU - Wassmann, Sven

AU - Niessner, Alexander

AU - Schmidt, Thomas Andersen

AU - Saely, Christoph H.

AU - Baumgartner, Iris

AU - Tamargo, Juan

PY - 2018/10/1

Y1 - 2018/10/1

N2 - With statins, the reported rate of adverse events differs widely between randomized clinical trials (RCTs) and observations in clinical practice, the rates being 1–2% in RCTs vs. 10–20% in the so-called real world. One possible explanation is the claim that RCTs mostly use a run-in period with a statin. This would exclude intolerant patients from remaining in the trial and therefore favour a bias towards lower rates of intolerance. We here review data from RCTs with more than 1000 participants with and without a run-in period, which were included in the Cholesterol Treatment Trialists Collaboration. Two major conclusions arise: (i) the majority of RCTs did not have a test dose of a statin in the run-in phase. (ii) A test dose in the run-in phase was not associated with a significantly improved adherence rate within that trial when compared to trials without a test dose. Taken together, the RCTs of statins reviewed here do not suggest a bias towards an artificially higher adherence rate because of a run-in period with a test dose of the statin. Other possible explanations for the apparent disparity between RCTs and real-world observations are also included in this review albeit mostly not supported by scientific data.

AB - With statins, the reported rate of adverse events differs widely between randomized clinical trials (RCTs) and observations in clinical practice, the rates being 1–2% in RCTs vs. 10–20% in the so-called real world. One possible explanation is the claim that RCTs mostly use a run-in period with a statin. This would exclude intolerant patients from remaining in the trial and therefore favour a bias towards lower rates of intolerance. We here review data from RCTs with more than 1000 participants with and without a run-in period, which were included in the Cholesterol Treatment Trialists Collaboration. Two major conclusions arise: (i) the majority of RCTs did not have a test dose of a statin in the run-in phase. (ii) A test dose in the run-in phase was not associated with a significantly improved adherence rate within that trial when compared to trials without a test dose. Taken together, the RCTs of statins reviewed here do not suggest a bias towards an artificially higher adherence rate because of a run-in period with a test dose of the statin. Other possible explanations for the apparent disparity between RCTs and real-world observations are also included in this review albeit mostly not supported by scientific data.

KW - Adherence

KW - Intolerance

KW - Run in phase

KW - Statin therapy

U2 - 10.1093/ehjcvp/pvy028

DO - 10.1093/ehjcvp/pvy028

M3 - Review

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SN - 2055-6837

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EP - 236

JO - European Heart Journal - Cardiovascular Pharmacotherapy

JF - European Heart Journal - Cardiovascular Pharmacotherapy

IS - 4

ER -

Reasons for disparity in statin adherence rates between clinical trials and real-world observations: A review

Abstract

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