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• Another independent Analysis of the FOURIER data is required
  Jochen Schuler
  Published on: 9 February 2023
• “Re: Letter to the Editor RE: "Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data". BMJ Open. 2022;12:3060172.”
  Folkert van Bruggen, Dika Luijendijk
  Published on: 30 January 2023
• Response to Dr. Guijarro
  Juan Erviti, James M Wright, MD, PhD, Ken Bassett, MD, PhD, Mohamed Ben-Eltriki, PharmD, Ciprian Jauca, Luis C Saiz, Pharm D, PhD, Leire Leache, Pharm D, PhD, Marta Gutiérrez-Valencia, PharmD, PhD and Thomas L Perry, MD, PhD
  Published on: 25 January 2023
• Response to Dr. Sabatine et al.
  Juan Erviti, Pharm D, PhD, James M Wright, MD, PhD, Ken Bassett, MD, PhD, Mohamed Ben-Eltriki, PharmD, Ciprian Jauca, Luis C Saiz, Pharm D, PhD, Leire Leache, Pharm D, PhD, Marta Gutiérrez-Valencia, PharmD, PhD and Thomas L Perry, MD, PhD
  Published on: 19 January 2023
• Restoring the credit of PSCK inhibitors for the prevention of cardiovascular events
  Carlos Guijarro
  Published on: 19 January 2023
• Was it a methodical failure?
  Luis Mendoza
  Published on: 19 January 2023
• Letter to the Editor RE: "Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data". BMJ Open. 2022;12:3060172.
  Marc S. Sabatine, MD, MPH, Stephen D. Wiviott, MD, Anthony C. Keech, MD, Peter S. Sever, PhD, FRCP and Robert P. Giugliano, MD, SM
  Published on: 13 January 2023
• Sceptical?
  John W Davis
  Published on: 10 January 2023
• Re: “Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data”
  Folkert van Bruggen, Dika Luijendijk
  Published on: 10 January 2023

• Published on: 9 February 2023

  Another independent Analysis of the FOURIER data is required

  • Jochen Schuler, Cardiologist, Research Associate Institute of General Practice, Family Medicine and Preventive Medicine, Paracelsus Private Medical University Salzburg AT

  The question raised by Juan Ervriti and Colleagues (1) whether the obvious benefit of evolocumab is offset by a currently unknown risk is justified and of high clinical relevance. We know active ingredients that effectively lower the atherogenic lipopoproteins, but have an unfavorable benefit-risk ratio under the bottom line (2). Therefore, the raised concerns must be addressed.
  The chosen methodology by Ervriti and Colleagues seems to me feasible, although not perfect. For a comprehensive reanalysis the raw data are required. Unfortunately they never received such data, although they have made many efforts to do so.
  To my opinion, scientific misconduct – as intended by Sabatine et. al. (3) - is not the case with Evriti et al. but rather with the FOURIER authors and the study sponsor, who apparently never answered the questions that were put to them repeatedly and publicly (4).
  The announcement by the FOURIER authors that they will respond to the accusations now promptly (3) is no longer sufficient. They are biased in a number of ways, but primarily because their scientific reputation is at stake. There is no other way to understand their rude reaction.
  From my point of view, it is also highly irritating that neither EMA nor Health Canada seem to have scrutinized the case report forms (CRF) when they approved this new drug. It looks like they've never laid their hands on a FOURIER-CRF. If that is the case, then they trusted the investigators bl...

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  The question raised by Juan Ervriti and Colleagues (1) whether the obvious benefit of evolocumab is offset by a currently unknown risk is justified and of high clinical relevance. We know active ingredients that effectively lower the atherogenic lipopoproteins, but have an unfavorable benefit-risk ratio under the bottom line (2). Therefore, the raised concerns must be addressed.
  The chosen methodology by Ervriti and Colleagues seems to me feasible, although not perfect. For a comprehensive reanalysis the raw data are required. Unfortunately they never received such data, although they have made many efforts to do so.
  To my opinion, scientific misconduct – as intended by Sabatine et. al. (3) - is not the case with Evriti et al. but rather with the FOURIER authors and the study sponsor, who apparently never answered the questions that were put to them repeatedly and publicly (4).
  The announcement by the FOURIER authors that they will respond to the accusations now promptly (3) is no longer sufficient. They are biased in a number of ways, but primarily because their scientific reputation is at stake. There is no other way to understand their rude reaction.
  From my point of view, it is also highly irritating that neither EMA nor Health Canada seem to have scrutinized the case report forms (CRF) when they approved this new drug. It looks like they've never laid their hands on a FOURIER-CRF. If that is the case, then they trusted the investigators blindly and failed to do their job. This would disqualify theses institutions for a trusting reanalysis of the data.
  Ultimately, only another independent reanalysis of the FOURIER raw data by a recognized independent institution should clarify the facts as soon as possible.

  References:
  1. Erviti J, Wright J, Bassett K, Ben-Eltriki M, Jauca C, Saiz LC, Leache L, Gutierrez-Valencia M and Perry TL. Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data. BMJ open. 2022;12:e060172.
  2. Rossouw JE, Anderson GL, Prentice RL, LaCroix AZ, Kooperberg C, Stefanick ML, Jackson RD, Beresford SA, Howard BV, Johnson KC, Kotchen JM, Ockene J, Writing Group for the Women's Health Initiative Investigators. Risks and benefits of estrogen plus progestin in healthy postmenopausal women: principal results From the Women's Health Initiative randomized controlled trial. JAMA. 2002;288(3):321.
  3. Marc S. Sabatine, MD, MPH, Stephen D. Wiviott, MD, Anthony C. Keech, MD, Peter S. Sever, PhD, FRCP and Robert P. Giugliano, MD, SM. Letter to the Editor RE: "Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data". BMJ Open. 2022;12:3060172.
  Published on: 11 January 2023
  4. Erviti J, et al. Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data. BMJ Open 2022;12:e060172. doi: 10.1136/bmjopen-2021-060172

  Conflicts of Interests: None

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  Conflict of Interest:
  None declared.

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• Published on: 30 January 2023

  “Re: Letter to the Editor RE: "Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data". BMJ Open. 2022;12:3060172.”

  • Folkert van Bruggen, GP and PhD candidate University Medical Centre Groningen, the Netherlands
  • Other Contributors:
    • Dika Luijendijk, Senior Researcher

  “Re: Letter to the Editor RE: "Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data". BMJ Open. 2022;12:3060172.”

  Dear editor,
  In their letter to the editor, Sabatine et al. comment on the restoration study of the FOURIER trial by Erviti et al.1 We agree that some discrepancies in locally established and adjudicated causes of deaths can be expected as part of the adjudication process. However, the trial investigators do not explain why there were so many discrepancies in FOURIER: 41.4% of locally established causes of deaths were not confirmed after central adjudication by the clinical-events committee. The site investigators attributed 358 of 870 deaths (41.1%) to a cardiovascular cause, and the committee 491 (56.4%): a difference of +15.3%. The high rate of discrepancies is surprising because both groups had all detailed clinical information at their disposal as well as the study protocol with definitions for cardiovascular events, and were blinded to the treatment status of the participants. Moreover, several previous studies have shown much lower discrepancy rates in other clinical outcomes trials that tested a drug for the prevention of cardiovascular disease. One recent study concerned the COMPASS trial among 27,395 patients that received rivaroxaban with aspirin, rivaroxaban monotherapy or aspirin monotherapy.2 There were 552 investiga...

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  “Re: Letter to the Editor RE: "Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data". BMJ Open. 2022;12:3060172.”

  Dear editor,
  In their letter to the editor, Sabatine et al. comment on the restoration study of the FOURIER trial by Erviti et al.1 We agree that some discrepancies in locally established and adjudicated causes of deaths can be expected as part of the adjudication process. However, the trial investigators do not explain why there were so many discrepancies in FOURIER: 41.4% of locally established causes of deaths were not confirmed after central adjudication by the clinical-events committee. The site investigators attributed 358 of 870 deaths (41.1%) to a cardiovascular cause, and the committee 491 (56.4%): a difference of +15.3%. The high rate of discrepancies is surprising because both groups had all detailed clinical information at their disposal as well as the study protocol with definitions for cardiovascular events, and were blinded to the treatment status of the participants. Moreover, several previous studies have shown much lower discrepancy rates in other clinical outcomes trials that tested a drug for the prevention of cardiovascular disease. One recent study concerned the COMPASS trial among 27,395 patients that received rivaroxaban with aspirin, rivaroxaban monotherapy or aspirin monotherapy.2 There were 552 investigator-reported (52.2%) and 558 (52.8%) adjudicated cardiovascular deaths among 1057 deaths (difference +0.6%).
  A second study investigated the events of the REDUCE-IT trial.3 This trial assessed the effects of icosapent ethyl versus placebo in 8,179 patients with elevated triglycerides that used a statin. The number of investigator-reported and adjudicated cardiovascular deaths was the same: 387 of 592 (65.4%) deaths (difference 0.0%).
  A third study analysed the STABILITY trial that compared darapladib to placebo in 15,828 patients with stable coronary disease.4 There were 667 (62.7%) investigator-reported and 638 (60.0%) adjudicated cardiovascular deaths of 1064 deaths (difference -2.7%).
  A fourth paper concerned the SOCRATES trial that evaluated the effects of ticagrelor versus aspirin in 13,199 patients after stroke or transient ischemic attack.5 There were 87 (58.8%) investigator-reported and 93 (62.8%) adjudicated cardiovascular deaths among 148 all-cause deaths (difference +4.0%).
  The four cited studies demonstrate a high concordance in the number of cardiovascular deaths reported by local investigators and adjudicated by central adjudication committees. Similar results were found for the primary composite outcomes of the investigated trials, which included non-fatal myocardial infarcts and strokes. Hence, the question remains why there was such a large discrepancy in investigator-reported and adjudicated cardiovascular deaths in FOURIER, and whether the non-fatal cardiovascular events show the same discrepancy. If Sabatine et al. have “complete confidence in the adjudicated events”, then why not share the raw data for independent restoration and reanalysis?

  F.H. van Bruggen, H. J. Luijendijk
  Department of General Practice, UMCG, PO Box 196, 9700 AD Groningen, The Netherlands. E-mail: h.j.luijendijk@umcg.nl

  1. Erviti J, Wright J, Bassett K, et al. Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data. BMJ Open. 2022;12(12):e060172. doi:10.1136/bmjopen-2021-060172
  2. Gaba P, Bhatt DL, Dagenais GR et al. Comparison of Investigator-Reported vs Centrally Adjudicated Major Adverse Cardiac Events: A Secondary Analysis of the COMPASS Trial. JAMA Netw Open. 2022;5(11):e224. doi:10.1001/jamanetworkopen.2022.43201
  3. Gaba P, Bhatt DL, Giugliano RP, et al. Comparative Reductions in Investigator-Reported and Adjudicated Ischemic Events in REDUCE-IT. J Am Coll Cardiol. 2021. doi:10.1016/j.jacc.2021.08.009
  4. Held C, White HD, Stewart RAH, et al. Characterization of cardiovascular clinical events and impact of event adjudication on the treatment effect of darapladib versus placebo in patients with stable coronary heart disease: Insights from the STABILITY trial. Am Heart J. 2019. doi:10.1016/j.ahj.2018.10.010
  5. Easton JD, Denison H, Evans SR, et al. Estimated treatment effect of ticagrelor versus aspirin by investigator-assessed events compared with judgement by an independent event adjudication committee in the SOCRATES trial. Int J Stroke. 2019. doi:10.1177/1747493019851282

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  Conflict of Interest:
  None declared.

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• Published on: 25 January 2023

  Response to Dr. Guijarro

  • Juan Erviti, senior researcher Innovation and Organization Unit, Navarre Health Service, Pamplona, Spain
  • Other Contributors:
    • James M Wright, MD, PhD, Professor
    • Ken Bassett, MD, PhD, Professor
    • Mohamed Ben-Eltriki, PharmD, researcher
    • Ciprian Jauca, Research Associate
    • Luis C Saiz, Pharm D, PhD, researcher
    • Leire Leache, Pharm D, PhD, researcher
    • Marta Gutiérrez-Valencia, PharmD, PhD, researcher
    • Thomas L Perry, MD, PhD, Associate professor

  We thank Dr. Guijarro for his comments (1) and are pleased to respond to his main concerns on our article. He states that “the claim of increased cardiovascular mortality is thus numerically compensated by a reduction in non-cardiovascular mortality”. However, we should bear in mind that both total and cardiovascular mortality were numerically increased in the evolocumab group compared to placebo, which is inconsistent with a significant reduction in cardiovascular events. Additionally, this drug is indicated for patients with previous cardiovascular disease. If potential cardiac harm were confirmed, additional concerns with evolocumab in this population would be reasonably expected.

  We acknowledge that “none of our concerns is supported by any statistically significant difference”. However, since cardiovascular mortality is included in the composite primary endpoint, an exaggerated assessment of cardiovascular mortality could have contributed to inappropriate early termination of the trial ‘for benefit’. If the point estimate we identified of a 20% relative risk increase in cardiovascular mortality were maintained, the non-significant increase from evolocumab might have reached statistical significance before the end of the prespecified 56-month follow-up.

  Dr. Guijarro also mentions that “the FOURIER open label extension study suggests that longer treatment with evolocumab may indeed reduce cardiovascular mortality”(2). However, the results of this study di...

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  We thank Dr. Guijarro for his comments (1) and are pleased to respond to his main concerns on our article. He states that “the claim of increased cardiovascular mortality is thus numerically compensated by a reduction in non-cardiovascular mortality”. However, we should bear in mind that both total and cardiovascular mortality were numerically increased in the evolocumab group compared to placebo, which is inconsistent with a significant reduction in cardiovascular events. Additionally, this drug is indicated for patients with previous cardiovascular disease. If potential cardiac harm were confirmed, additional concerns with evolocumab in this population would be reasonably expected.

  We acknowledge that “none of our concerns is supported by any statistically significant difference”. However, since cardiovascular mortality is included in the composite primary endpoint, an exaggerated assessment of cardiovascular mortality could have contributed to inappropriate early termination of the trial ‘for benefit’. If the point estimate we identified of a 20% relative risk increase in cardiovascular mortality were maintained, the non-significant increase from evolocumab might have reached statistical significance before the end of the prespecified 56-month follow-up.

  Dr. Guijarro also mentions that “the FOURIER open label extension study suggests that longer treatment with evolocumab may indeed reduce cardiovascular mortality”(2). However, the results of this study differ to a great extent from those in the parent FOURIER trial. This may be related to the methodological limitations of open trials. Furthermore, a systematic review based on the results published at ClinicalTrials.gov shows that evolocumab probably increases the risk of all-cause mortality compared to placebo (OR 1.12; 95% CI 1.00-1.25) (3).

  Dr. Guijarro also states that “no one disputes its favourable effects not simply on lipid levels, but in cardiovascular event reduction in patients with established atherosclerotic cardiovascular disease”. We respectfully disagree on this aspect, since the aim of the FOURIER trial was precisely to shed light on the cardiovascular effects of evolocumab. Once the trial had started, the manufacturer amended the protocol in order to split cardiovascular events into two categories, namely, “efficacy” and “safety” outcomes. For those included as “efficacy” outcomes, no narratives are available in the Clinical Study Report (CSR), whereas information on cardiovascular events labelled as “adverse events” (safety outcomes) was given. The proportion of patients with at least one cardiac event in the evolocumab group was 13.7% (1885/13769) vs 14.2% (1948/13756) in the placebo group. No statistically significant differences were observed between groups, RR 1.03 (95%CI, 0.98 to 1.10) (CSR report body part 1, page 1197 of 5092). The lack of efficacy of evolocumab in the prevention of cardiac events labelled as “safety” outcomes is not consistent with the reported efficacy in the reduction of the incidence of cardiac events labelled as “efficacy” outcomes in the NEJM 2017 publication. Since Dr. Guijarro thinks that “it is worth carefully reviewing the adjudication of cardiovascular mortality”, he may share our conclusion that independent review of the adjudication of efficacy endpoints is also desirable. For this, we need companies and regulators to be more transparent and provide full access to the trial’s information.

  Additionally, Dr Guijarro states that “the higher the extension of cardiovascular disease, the higher the potential absolute benefit of PCSK9 inhibition therapy”. This statement is based on the Recommendations of the Spanish Society of Arteriosclerosis (4). In this document, authors acknowledge that recommendations for patients with more than two uncontrolled additional risk factors are rather weak, with a “low” level of evidence (page 137 in the Journal article). In the FOURIER trial, patients with prior myocardial infarction experienced no benefit of evolocumab vs placebo in the primary endpoint after one year follow-up (CSR report body part 1, page 125 of 5092). This is inconsistent with the belief that people with more severe coronary artery disease will obtain a greater benefit from the drug.

  Finally, Dr. Guijarro states that “we should ask ourselves why so many atherosclerotic patients with uncontrolled LDL cholesterol levels are not receiving adequate lipid-lowering therapy, including PCSK9 Inhibitors if required”. However, we think that we and others, should first ask, after evolucumab reduced LDL-c levels so dramatically in the FOURIER trial, why did it show no reduction in mortality, and why benefits assessed as a reduction of cardiovascular events were so small, if real.

  References

  (1) Erviti J, Wright J, Bassett K, et al. Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data. BMJ Open 2022;12:e060172. doi:10.1136/bmjopen-2021-060172

  (2) O’Donoghue ML, Giugliano RP, Wiviott SD, et al. Long-Term Evolocumab in Patients With Established Atherosclerotic Cardiovascular Disease. Circulation 2022;146:1109–19. doi:10.1161/CIRCULATIONAHA.122.061620

  (3) van Bruggen FH, Nijhuis GBJ, Zuidema SU, Luijendijk H. Serious adverse events and deaths in PCSK9 inhibitor trials reported on ClinicalTrials.gov: a systematic review. Expert Rev Clin Pharmacol. 2020 Jul;13(7):787-796. doi: 10.1080/17512433.2020.1787832. Epub 2020 Jul 13. PMID: 32597252.

  (4) Ascaso JF, Civeira F, Guijarro C, et al. Indications of PCSK9 inhibitors in clinical practice. Recommendations of the Spanish Society of Arteriosclerosis (SEA), 2019. Clin Investig Arterioscler 2019;31:128–39. doi:10.1016/j.arteri.2019.04.002

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  Conflict of Interest:
  None declared.

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• Published on: 19 January 2023

  Response to Dr. Sabatine et al.

  • Juan Erviti, Pharm D, PhD, senior researcher Innovation and Organization Unit, Navarre Health Service, Pamplona, Spain
  • Other Contributors:
    • James M Wright, MD, PhD, Professor
    • Ken Bassett, MD, PhD, Professor
    • Mohamed Ben-Eltriki, PharmD, researcher
    • Ciprian Jauca, Research Associate
    • Luis C Saiz, Pharm D, PhD, researcher
    • Leire Leache, Pharm D, PhD, researcher
    • Marta Gutiérrez-Valencia, PharmD, PhD, researcher
    • Thomas L Perry, MD, PhD, Associate professor

  We thank Dr. Sabatine, Wiviott, Keech, Sever and Giuliano, who have posted Rapid Responses to our article (1), and are pleased that BMJ Open metrics indicate substantial interest.

  We respectfully disagree with Dr. Sabatine et al., with regard to a number of issues they raise.

  1. Dr. Sabatine and colleagues maintain that additional information available in patient dossiers and hospital records would have led us to different results. On the following dates: 13/02/2019, 18/03/2019, and 08/05/2019, we requested assistance to obtain such information from Dr. Sabatine, the corresponding author for the N Engl J Med 2017 report of FOURIER. Additionally, we emailed Dr Sabatine on 11/04/2019 to inform him that a ‘call-to-action’ on the FOURIER trial had been published in the BMJ (2) with the intention to restore the FOURIER trial. Neither Dr. Sabatine nor his colleagues made any reply.

  The problems of event ascertainment, adjudication, and reporting in complex clinical trials will not go away without substantial changes. This is highlighted by the new Lancet inquiry into how the RECORD 4 trial of rivaroxaban was conducted and reported (3). The solution is openness and scientific collaboration, not “data hogging.”

  Patients who volunteer for clinical trials enter an ethical agreement to help discover scientific truth. What would the same patients think if they realized that sponsors and investigators make sure that no one can effectively double check the...

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  We thank Dr. Sabatine, Wiviott, Keech, Sever and Giuliano, who have posted Rapid Responses to our article (1), and are pleased that BMJ Open metrics indicate substantial interest.

  We respectfully disagree with Dr. Sabatine et al., with regard to a number of issues they raise.

  1. Dr. Sabatine and colleagues maintain that additional information available in patient dossiers and hospital records would have led us to different results. On the following dates: 13/02/2019, 18/03/2019, and 08/05/2019, we requested assistance to obtain such information from Dr. Sabatine, the corresponding author for the N Engl J Med 2017 report of FOURIER. Additionally, we emailed Dr Sabatine on 11/04/2019 to inform him that a ‘call-to-action’ on the FOURIER trial had been published in the BMJ (2) with the intention to restore the FOURIER trial. Neither Dr. Sabatine nor his colleagues made any reply.

  The problems of event ascertainment, adjudication, and reporting in complex clinical trials will not go away without substantial changes. This is highlighted by the new Lancet inquiry into how the RECORD 4 trial of rivaroxaban was conducted and reported (3). The solution is openness and scientific collaboration, not “data hogging.”

  Patients who volunteer for clinical trials enter an ethical agreement to help discover scientific truth. What would the same patients think if they realized that sponsors and investigators make sure that no one can effectively double check their analyses? As Cochrane authors, we have obtained the individual-patient data of different trials to carry out systematic reviews that provide high added value to patients and health systems. There are no legal constraints nor ethical reasons to refuse to share anonymized data. We encourage Dr. Sabatine and colleagues to share the full database of the FOURIER trial with the scientific community.

  2. Our re-adjudication of the deaths in FOURIER was done exclusively by a panel of 5 blinded re-adjudicators. Anything that could provide a hint as to treatment was redacted by a researcher from outside the panel before the narratives were seen by the re-adjudicators. We explained this in the publication and there should be no misunderstanding. Additionally, readers can double-check all re-adjudications made, their justification, and read the original narratives in the CSR that support all decisions taken (supplemental table S2).

  3. We recruited as volunteer re-adjudicators JMW, KB, MBE, CJ and TLP, who have extensive experience in Clinical Pharmacology, Internal Medicine, Family Practice, Pharmacy, and critical appraisal. The 5 adjudicators took on this project during the Covid-19 pandemic as work additional to their University of British Columbia academic appointments. For the re-adjudications, we followed the definitions specified in the FOURIER trial protocol. For most sessions, all 5 were present to review each case, and never fewer than 4 re-adjudicators, operating by consensus. The role of TLP was to resolve any dispute, but in no case did this arise. The online supplement to our report provides all possible details when our re-adjudication diverged from the original adjudication by the FOURIER Clinical Events Committee.

  4. In the FOURIER protocol there is no mention about autopsies being carried out. Had they been performed in the trial, this should have been included in the protocol. The Clinical Study Report (over 25 000 pages) provides no evidence of any autopsies. To the contrary, in a few cases, the narratives confirmed that an autopsy was not performed.

  5. We applied a very conservative approach and re-adjudicated the cause of mortality only if there was compelling evidence in the CSR to support changes.

  References:

  1. Erviti J, Wright J, Bassett K, et alRestoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory dataBMJ Open 2022;12:e060172. doi: 10.1136/bmjopen-2021-060172
  2. Erviti J, Saiz LC, Leache L. Rapid response to: Restoring invisible and abandoned trials: a call for people to publish the findings. BMJ2013;346.
  3. Demasi M. Rivaroxaban: Lancet opens investigation into anticlotting drug trial after BMJ report. BMJ. 2022 Dec 30;379:o3071. doi: 10.1136/bmj.o3071. PMID: 36585025.

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  Conflict of Interest:
  None declared.

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• Published on: 19 January 2023

  Restoring the credit of PSCK inhibitors for the prevention of cardiovascular events

  • Carlos Guijarro, Internal Medicne. Cardiovascular risk clinic Hospital Universitari Fundacion Alcorcon - Universidad Rey Juan Carlos . Madrid, Spain

  Dear Sir
  The article by Erviti et al. [1] is a provocative reinterpretation of the data from the FOURIER trial [2]. However, their conclusion indicating that clinicians should be ‘sceptical about prescribing evolocumab for patients with established atherosclerotic cardiovascular disease’ is not adequately supported by the data provided.
  First, global mortality did not statistically differ between placebo and evolocumab groups. Therefore, given that total mortality remains unchanged in both groups by Erviti’s analysis, any increase in cardiovascular mortality must be identical numerically to a reduction in non-cardiovascular (+ undetermined) mortality. The claim of increased cardiovascular mortality is thus numerically compensated by a reduction in non cardiovascular mortality. Of note, the FORIER trial was not powered to discriminate the effect of evolocumab on cardiovascular and non cardiovascular mortality; this lack of power remains for Ertivi’s analysis: none of their concerns is supported by any statistically significant difference. Further speculation regarding other individual end point sub group analysis must be interpreted with caution: it is fun to look at, but do not believe them [3]. While it is worth carefully reviewing the adjudication of cardiovascular mortality, FOURIER open label extension study suggest that longer treatment with evolocumab may indeed reduce cardiovascular mortality. [4]
  Even if we remain sceptical about a potential red...

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  Dear Sir
  The article by Erviti et al. [1] is a provocative reinterpretation of the data from the FOURIER trial [2]. However, their conclusion indicating that clinicians should be ‘sceptical about prescribing evolocumab for patients with established atherosclerotic cardiovascular disease’ is not adequately supported by the data provided.
  First, global mortality did not statistically differ between placebo and evolocumab groups. Therefore, given that total mortality remains unchanged in both groups by Erviti’s analysis, any increase in cardiovascular mortality must be identical numerically to a reduction in non-cardiovascular (+ undetermined) mortality. The claim of increased cardiovascular mortality is thus numerically compensated by a reduction in non cardiovascular mortality. Of note, the FORIER trial was not powered to discriminate the effect of evolocumab on cardiovascular and non cardiovascular mortality; this lack of power remains for Ertivi’s analysis: none of their concerns is supported by any statistically significant difference. Further speculation regarding other individual end point sub group analysis must be interpreted with caution: it is fun to look at, but do not believe them [3]. While it is worth carefully reviewing the adjudication of cardiovascular mortality, FOURIER open label extension study suggest that longer treatment with evolocumab may indeed reduce cardiovascular mortality. [4]
  Even if we remain sceptical about a potential reduction in cardiovascular mortality by evolocumab, no one disputes its favourable effects not simply on lipid levels, but in cardiovascular event reduction in patients with established atherosclerotic cardiovascular disease., as it is the case for alirocumab The higher the extension of cardiovascular disease, the higher the potential absolute benefit of PCSK9 inhibition therapy [5].
  With the present level of evidence our concern should not be that we are prescribing evolocumab for too many patients with cardiovascular disease. Rather, we should ask ourselves why so many atherosclerotic patients with uncontrolled LDL cholesterol levels are not receiving adequate lipid-lowering therapy, including PCSK.9 Inhibtors if required.

  1 Erviti J, Wright J, Bassett K, et al. Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data. BMJ Open 2022;12:e060172. doi:10.1136/bmjopen-2021-060172
  2 Sabatine MS, Giugliano RP, Keech AC, et al. Evolocumab and Clinical Outcomes in Patients with Cardiovascular Disease. New England Journal of Medicine 2017;376:1713–22. doi:10.1056/NEJMoa1615664
  3 Sleight P. Debate: Subgroup analyses in clinical trials: fun to look at - but don’t believe them! Curr Control Trials Cardiovasc Med 2000;1:25–7. doi:10.1186/cvm-1-1-025
  4 O’Donoghue ML, Giugliano RP, Wiviott SD, et al. Long-Term Evolocumab in Patients With Established Atherosclerotic Cardiovascular Disease. Circulation 2022;146:1109–19. doi:10.1161/CIRCULATIONAHA.122.061620
  5 Ascaso JF, Civeira F, Guijarro C, et al. Indications of PCSK9 inhibitors in clinical practice. Recommendations of the Spanish Sociey of Arteriosclerosis (SEA), 2019. Clin Investig Arterioscler 2019;31:128–39. doi:10.1016/j.arteri.2019.04.002

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  Conflict of Interest:
  I have received fees for lectures and advisory boards from AMGEN and Sanofi

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• Published on: 19 January 2023

  Was it a methodical failure?

  • Luis Mendoza, Medical Director IQVIA

  I reviewed Dr. Erviti et all's article and found that the RIAT team likely missed something important related to the trial itself when they analyzed the study data published in the NEJM on February 13, 2019.
  The main point is that the article does not describe the data review process to adjudicate cardiovascular outcomes. The article only mentions the participation of the Data Monitoring Committee for the review of safety events and the adjudication of cases of death related or not to evolocumab. There is no mention of how the Committee was composed and what process was put in place for the adjudications. I can assume that the members of the Committee were physicians trained in cardiology for the review of major cardiovascular events and related deaths. Members of such Committees often request a lot of additional information from sites to review prior to the adjudications. The complete documentation generated for the adjudication of each case is usually not included in the Clinical Study Report (CSR) and is filed in the safety database. The authors also presented in Figures 1 and 2 examples of reports used in their review to determine inconsistent data. Looking at the format of those reports, it appears that they were automatically generated by the study data manager for a high-level description of the cases to include in the CSR. Those reports don’t show all the data that is normally collected in severe events on the CIOMS form for reporting to authorities and...

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  I reviewed Dr. Erviti et all's article and found that the RIAT team likely missed something important related to the trial itself when they analyzed the study data published in the NEJM on February 13, 2019.
  The main point is that the article does not describe the data review process to adjudicate cardiovascular outcomes. The article only mentions the participation of the Data Monitoring Committee for the review of safety events and the adjudication of cases of death related or not to evolocumab. There is no mention of how the Committee was composed and what process was put in place for the adjudications. I can assume that the members of the Committee were physicians trained in cardiology for the review of major cardiovascular events and related deaths. Members of such Committees often request a lot of additional information from sites to review prior to the adjudications. The complete documentation generated for the adjudication of each case is usually not included in the Clinical Study Report (CSR) and is filed in the safety database. The authors also presented in Figures 1 and 2 examples of reports used in their review to determine inconsistent data. Looking at the format of those reports, it appears that they were automatically generated by the study data manager for a high-level description of the cases to include in the CSR. Those reports don’t show all the data that is normally collected in severe events on the CIOMS form for reporting to authorities and archiving in the security database. The authors based all their investigations and judgments on such reports and repeatedly reproduced that "The narrative contained no evidence to support the cause of death adjudicated by the FOURIER Clinical Events Committee," as shown in Supplement 2.
  I agree with the RIAT initiative, however, the lack of information related to the Safety Data Committee, the adjudication process, the detailed safety information, and the generation of the CSR has probably caused a misinterpretation of the data by the authors and draw erroneous conclusions. I also wonder if the journal's reviewers realized these points before accepting the article for publication. I cannot be conclusive about the above, but surely Amgen would further clarify the consistency of the data presented in the NEJM article by providing more robust data from the results of 130 evolocumab clinical trials registered on Clinicaltrial.gov. Finally, the article also mentions that the RIAT team contacted the main author of the article published in NEJM without success. In that sense, a more effective approach might have been to contact Amgen directly and discuss with them the intentions of reviewing the study data. Certainly, this may have helped the authors to gain access to the full safety data and ensure proper review of it.

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  Conflict of Interest:
  None declared.

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• Published on: 13 January 2023

  Letter to the Editor RE: "Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data". BMJ Open. 2022;12:3060172.

  • Marc S. Sabatine, MD, MPH, Professor of Medicine; Cardiologist Brigham & Women's Hospital/Harvard Medical School
  • Other Contributors:
    • Stephen D. Wiviott, MD, Professor of Medicine; Cardiologist
    • Anthony C. Keech, MD, Professor of Medicine; Cardiologist
    • Peter S. Sever, PhD, FRCP, Professor of Clinical Pharmacology and Therapeutics
    • Robert P. Giugliano, MD, SM, Professor of Medicine/Cardiologist

  The article by Erviti et al.1 is fundamentally flawed, using incomplete data to reach incorrect conclusions. In FOURIER,2 event adjudication followed a rigorous, pre-specified, blinded process by the TIMI Clinical Events Committee (CEC). The occurrence of potential cardiovascular events of interest triggered collection of a full dossier containing all relevant and available source documents, including hospital notes, laboratory, ECG and imaging data, procedure reports, resuscitation or code summaries, death certificates, and autopsy reports. Each dossier was independently evaluated by 2 experienced, board-certified cardiologists (cardiovascular events) or neurologists (cerebrovascular events), blinded to treatment allocation. The CEC followed well-accepted practices used for 2 decades and supporting multiple peer-reviewed manuscripts and world-wide regulatory filings. Criteria for outcomes were consistent with FDA definitions.3 The adjudication charter was approved by the FDA before the trial commenced. At the end of the trial the FDA audited the adjudication process and results and had no findings of concern.
  In contrast, the authors’ work was post hoc and relied only on one document: the CSR narrative, which was generated predominantly based on limited information provided by the site upon learning of the event and not intended for the purpose of formal event adjudication. It is unclear what training and expertise, if any, those classifying events for this paper ha...

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  The article by Erviti et al.1 is fundamentally flawed, using incomplete data to reach incorrect conclusions. In FOURIER,2 event adjudication followed a rigorous, pre-specified, blinded process by the TIMI Clinical Events Committee (CEC). The occurrence of potential cardiovascular events of interest triggered collection of a full dossier containing all relevant and available source documents, including hospital notes, laboratory, ECG and imaging data, procedure reports, resuscitation or code summaries, death certificates, and autopsy reports. Each dossier was independently evaluated by 2 experienced, board-certified cardiologists (cardiovascular events) or neurologists (cerebrovascular events), blinded to treatment allocation. The CEC followed well-accepted practices used for 2 decades and supporting multiple peer-reviewed manuscripts and world-wide regulatory filings. Criteria for outcomes were consistent with FDA definitions.3 The adjudication charter was approved by the FDA before the trial commenced. At the end of the trial the FDA audited the adjudication process and results and had no findings of concern.
  In contrast, the authors’ work was post hoc and relied only on one document: the CSR narrative, which was generated predominantly based on limited information provided by the site upon learning of the event and not intended for the purpose of formal event adjudication. It is unclear what training and expertise, if any, those classifying events for this paper had. The authors claim to have followed the definitions used in FOURIER, but their own commentary calls into question their understanding of the definitions. Most critically, the authors admit their results were overread by an unblinded “Validation Committee” which irreparably taints the process and would not be accepted by regulatory agencies.4
  The authors note that in 26% of deaths, the FOURIER CEC final adjudication differed from the investigators’ initial categorization. Curiously, they describe these differences as “inconsistencies.” But the very purpose of the CEC is for trained and qualified experts to apply standardized definitions to properly classify events in a consistent manner using medical source documentation. Such a process will naturally result in reclassification, that is the point.
  The authors apply their flawed process to attempt to reassign categories of death. Unsurprisingly, given their reliance on very limited data, primarily they simply increased the number of “undetermined” deaths by more than 50%. The authors describe their 2 best examples of what they felt were “errors” by the FOURIER CEC. In the first case, the authors state the patient “clearly” had an MI, which was “neglected” by the FOURIER CEC. In reality, the source documents show this patient died in his sleep, and thus according to the FDA definitions, the FOURIER CEC properly adjudicated this as sudden cardiac death. In the second case, the authors state the patient died of an MI that was “misadjudicated” by the FOURIER CEC as a non-cardiovascular death. In reality, the source documents show this patient slipped in his kitchen, struck his head, was admitted to the ED with head trauma and died, which would not be considered a CV death.
  In their post-hoc, unblinded process, the authors differentially shifted slightly more deaths out of the cardiovascular bin (largely to “undetermined”) in the placebo arm than in the evolocumab arm. That resulted in 25 more cardiovascular deaths in the evolocumab than the placebo arm. However, they deliberately ignore the converse result of their process, which was now 20 fewer undetermined deaths in the evolocumab than the placebo arm.
  We have complete confidence in the FOURIER results adjudicated by the TIMI CEC. The paper by Erviti et al. is flawed in design and execution and, in our opinion, a gross disservice to the medical literature, cardiovascular health care providers, and patients.

  Disclosures

  MSS reports research grant support to the TIMI Study Group through Brigham and Women’s Hospital from: Abbott; Amgen; Anthos Therapeutics; AstraZeneca; Daiichi-Sankyo; Eisai; Intarcia; Ionis; Merck; Novartis; Pfizer; and honoraria for consulting from: Althera; Amgen; Anthos Therapeutics; AstraZeneca; Beren Therapeutics; Boehringer Ingelheim; Fibrogen; Intarcia; Merck; Moderna; Novo Nordisk; Precision BioSciences; Silence Therapeutics.

  SDW reports research grant support to the TIMI Study Group through Brigham and Women’s Hospital from: Amgen, AstraZeneca, Daiichi Sankyo, Eisai, Janssen, Merck, and Pfizer. Consulting fees from AstraZeneca, Boston Clinical Research Institute, Icon Clinical, and NovoNordisk. Dr. Wiviott’s wife is a former employee of Merck.

  ACK reports grants and personal fees from Abbott and Mylan; personal fees from Amgen, AstraZeneca and Pfizer; grants from Sanofi and Novartis; and personal fees from Bayer.

  PSS reports support from the Biomedical Research Centre, Imperial College NHS Trust, grant support from Pfizer, Amgen, and Servier, honoraria and lectures from Amgen, Pfizer and Viatris.

  RPG reports research grant support to the TIMI Study Group through Brigham and Women’s Hospital from: Amgen; Anthos Therapeutics; Ionis; Daiichi Sankyo; honoraria for lectures and/or consulting from: Amarin; Amgen; Artivion; Caladrius; Centrix; CSL Behring; Daiichi Sankyo; Dr. Reddy’s Laboratories; Esperion; Gilead; Hengrui; Inari; Janssen; Labcorp; Medical Education Resources; Medscape; Menarini; Merck; Novartis; Paratek; Pfizer; PhaseBio; SAJA; Servier; Shanghai Medical Group; St. Lukes Hospital (Kansas City); Sanofi; Voxmedia.

   
  References

  1. Erviti J, Wright J, Bassett K, Ben-Eltriki M, Jauca C, Saiz LC, Leache L, Gutierrez-Valencia M and Perry TL. Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data. BMJ open. 2022;12:e060172.
  2. Sabatine MS, Giugliano RP, Keech AC, Honarpour N, Wiviott SD, Murphy SA, Kuder JF, Wang H, Liu T, Wasserman SM, Sever PS, Pedersen TR, for the FOURIER Steering Committee and Investigators. Evolocumab and Clinical Outcomes in Patients with Cardiovascular Disease. N Engl J Med. 2017;376:1713-1722.
  3. Hicks KA, Tcheng JE, Bozkurt B, Chaitman BR, Cutlip DE, Farb A, Fonarow GC, Jacobs JP, Jaff MR, Lichtman JH, Limacher MC, Mahaffey KW, Mehran R, Nissen SE, Smith EE and Targum SL. 2014 ACC/AHA Key Data Elements and Definitions for Cardiovascular Endpoint Events in Clinical Trials: A Report of the American College of Cardiology/American Heart Association Task Force on Clinical Data Standards (Writing Committee to Develop Cardiovascular Endpoints Data Standards). Circulation. 2015;132:302-61.
  4. Sharma A, Mahaffey KW, Gibson CM, Hicks KA, Alexander KP, Ali M, Chaitman BR, Held C, Hlatky M, Jones WS, Mehran R, Menon V, Rockhold FW, Seltzer J, Spitzer E, Wilson M and Lopes RD. Clinical events classification (CEC) in clinical trials: Report on the current landscape and future directions - proceedings from the CEC Summit 2018. Am Heart J. 2022;246:93-104.

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  Conflict of Interest:
  MSS reports research grant support through Brigham and Women’s Hospital from: Abbott; Amgen; Anthos Therapeutics; AstraZeneca; Daiichi-Sankyo; Eisai; Intarcia; Ionis; Merck; Novartis; Pfizer; and honoraria for consulting from: Althera; Amgen; Anthos Therapeutics; AstraZeneca; Beren Therapeutics; Boehringer Ingelheim; Fibrogen; Intarcia; Merck; Moderna; Novo Nordisk; Precision BioSciences; Silence Therapeutics. SDW reports grants to the TIMI Study Group through institution from Amgen; AstraZeneca; Daiichi-Sankyo; Eisai; Janssen; Merck; Pfizer, and consulting fees from AstraZeneca; Boston Clinical Research Institute; Icon Clinical; and NovoNordisk. Dr. Wiviott’s wife is a former employee of Merck. RPG reports research grant support through Brigham and Women’s Hospital from: Amgen; Anthos Therapeutics; Ionis; Daiichi-Sankyo; honoraria for lectures or CME programs from Amgen; Centrix; Daiichi-Sankyo; Dr. Reddy’s Laboratories; Medical Education Resources (MER); Medscape; Menarini; Merck; Pfizer; SAJA Pharmaceuticals; Servier; Shanghai Medical Telescope; Voxmedia, and consulting from: Amarin; Amgen; Artivion, Inc.; Bayer; Boston Scientific; Caladrius; CSL Behring; CVS Caremark; Daiichi-Sankyo; Esperion; Gilead; Hengrui; Inari; Janssen; Novartis; Paratek; Pfizer; PhaseBio Pharmaceuticals; Samsung. ACK reports grants and personal fees from Abbott and Mylan; personal fees from Amgen, AstraZeneca and Pfizer; grants from Sanofi and Novartis; and personal fees from Bayer. PSS reports support from the Biomedical Research Centre, Imperial College NHS Trust, grant support from Pfizer, Amgen, and Servier, honoraria and lectures from Amgen, Pfizer and Viatris.

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• Published on: 10 January 2023

  Sceptical?

  • John W Davis, Physician-Scientist Trainee University Of Texas Medical Branch At Galveston

  I read your article with great interest, as a physician-scientist trainee who has Familial Hypercholesterolemia and takes Evolocumab as additive therapy. This article demonstrates important discrepancies to address for a very large trial critical to the uptake of PCSK9 inhibitors everywhere. It is disappointing to see such discrepancies.

  My concern with your conclusions, however, is that it seems to vastly overstate the impact of the findings. You suggest that clinicians ought to be sceptical in prescribing this medication. However, the discrepancies you reported did not change any trial conclusions. It does not affect that average change in LDL, which is the primary purpose in prescribing the medication. It also does not offer a plausible explanation why a PCSK9 inhibitor might cause increased cardiac death or vascular event rates. Further, meta-analysis of PCSK9 trials, even with the reported discrepancies, is unlikely to change the overall scientific evidence that PCSK9 inhibitors are safe and effective drugs.

  It is important to be watchful for pharma-biased presentations of RCT results, but likewise is important to avoid sensationalism. I see no reason in these results to discontinue or be sceptical of the power of PCSK9s, and we should be careful as scientists to avoid whiplashing the public towards scepticism of a well-tested drug.

  Statins already have been maligned in the public eye without great cause; let's avoid doing the same to this...

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  I read your article with great interest, as a physician-scientist trainee who has Familial Hypercholesterolemia and takes Evolocumab as additive therapy. This article demonstrates important discrepancies to address for a very large trial critical to the uptake of PCSK9 inhibitors everywhere. It is disappointing to see such discrepancies.

  My concern with your conclusions, however, is that it seems to vastly overstate the impact of the findings. You suggest that clinicians ought to be sceptical in prescribing this medication. However, the discrepancies you reported did not change any trial conclusions. It does not affect that average change in LDL, which is the primary purpose in prescribing the medication. It also does not offer a plausible explanation why a PCSK9 inhibitor might cause increased cardiac death or vascular event rates. Further, meta-analysis of PCSK9 trials, even with the reported discrepancies, is unlikely to change the overall scientific evidence that PCSK9 inhibitors are safe and effective drugs.

  It is important to be watchful for pharma-biased presentations of RCT results, but likewise is important to avoid sensationalism. I see no reason in these results to discontinue or be sceptical of the power of PCSK9s, and we should be careful as scientists to avoid whiplashing the public towards scepticism of a well-tested drug.

  Statins already have been maligned in the public eye without great cause; let's avoid doing the same to this lipid-lowering drug.

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  Conflict of Interest:
  I take Evolocumab for Familial Hypercholesterolemia.

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• Published on: 10 January 2023

  Re: “Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data”

  • Folkert van Bruggen, GP and pH-D candidate University Medical Centre Groningen, the Netherlands
  • Other Contributors:
    • Dika Luijendijk, Researher

  Dear editor,
  Erviti et al. recently restored the causes of death data in the FOURIER trial with the information in the clinical study report (CSR).1 The rationale was that evolocumab had been reported to reduce the risk of myocardial infarction and stroke, but (numerically) increase the risk of cardiovascular death (HR 1.05; 95% CI 0.88 to 1.25).2 Erviti et al. found that the clinical events committee did not confirm the local clinical investigator’s cause of death for 41.4% of cases often without clear supportive clinical evidence.1 As a result, less cardiac and cardiovascular deaths were reported to have occurred in the evolocumab group and more in the placebo group. Re-analysis with the original causes of death data resulted in a higher risk of cardiovascular death (RR 1.20; 95% CI 0.95 to 1.51) and cardiac death (RR 1.28; 95%CI 0.97 to 1.69) than previously reported.1 Erviti et al. concluded that possible cardiac harm due to evolocumab could not be ruled out.1
  Erviti et al could not restore the non-fatal cardiovascular events due to a lack of detailed information for these events in the CSR. We think this is unfortunate, because the reported events raise a number of questions. First, hospitalization for unstable angina (UA) made up 30.0% of the acute coronary syndrome events, which is a considerably higher proportion than that reported for similar populations.2 In the ODYSSEY OUTCOMES trial about alirocumab, it was 5.4%,3 and in the IMPROVE-IT trial about e...

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  Dear editor,
  Erviti et al. recently restored the causes of death data in the FOURIER trial with the information in the clinical study report (CSR).1 The rationale was that evolocumab had been reported to reduce the risk of myocardial infarction and stroke, but (numerically) increase the risk of cardiovascular death (HR 1.05; 95% CI 0.88 to 1.25).2 Erviti et al. found that the clinical events committee did not confirm the local clinical investigator’s cause of death for 41.4% of cases often without clear supportive clinical evidence.1 As a result, less cardiac and cardiovascular deaths were reported to have occurred in the evolocumab group and more in the placebo group. Re-analysis with the original causes of death data resulted in a higher risk of cardiovascular death (RR 1.20; 95% CI 0.95 to 1.51) and cardiac death (RR 1.28; 95%CI 0.97 to 1.69) than previously reported.1 Erviti et al. concluded that possible cardiac harm due to evolocumab could not be ruled out.1
  Erviti et al could not restore the non-fatal cardiovascular events due to a lack of detailed information for these events in the CSR. We think this is unfortunate, because the reported events raise a number of questions. First, hospitalization for unstable angina (UA) made up 30.0% of the acute coronary syndrome events, which is a considerably higher proportion than that reported for similar populations.2 In the ODYSSEY OUTCOMES trial about alirocumab, it was 5.4%,3 and in the IMPROVE-IT trial about ezetimibe 12.7%.4 Several cohort studies reported proportions between 7.2% and 18.3%.5–7 No explanation for this high proportion was provided even though hospitalization for UA was a component of the primary composite outcome.
  Secondly, evolocumab did not affect the risk of hospitalization for UA (HR 0.99; 95% CI 0.82 to 1.18), but significantly reduced the risk of non-ST-elevation myocardial infarction (NSTEMI; HR 0.77; 95% CI 0.68 to 0.88) and ST-elevation myocardial infarction (STEMI; HR 0.64; 95% CI 0.49 to 0.84).8 UA, NSTEMI and STEMI are all acute coronary syndromes and share common pathophysiological pathways that involve atherosclerosis and thrombosis.9 Therefore, one would expect that lipid lowering therapy would prevent UA, as well as NSTEMI and STEMI. Alirocumab reduced the risk of UA (HR 0.61; 95% CI 0.41-0.92) and NSTEMI (HR 0.82; 95% CI 0.72-0.93) statistically significantly in ODYSSEY OUTCOMES. The risk of STEMI was also (numerically) lower (HR 0.84; 0.64 to 1.11).3,10
  Thirdly, as we observed before, the clinical events committee did not confirm a large proportion of the local clinical investigators’ diagnoses of myocardial infarction and stroke either (8% respectively 17%).11 Moreover, the proportion of unconfirmed strokes was higher in the evolocumab group than the placebo group of FOURIER (21% and 14%; p = 0.044).11 The study protocol contained clear definitions for all cardiovascular outcomes that should have ensured appropriate clinical diagnoses for most events.
  The inconsistencies in the reported non-fatal cardiovascular events in FOURIER question how these events were adjudicated. Erviti et al’s findings did not reassure us. Therefore, it is necessary to investigate how many non-fatal events were reclassified by the clinical events committee, and what the original clinical diagnoses were. To enable such a restoration of the non-fatal cardiovascular events in FOURIER, we ask the medication authorization agencies to request a CSR that includes the related case report forms and make it publicly available.

  F.H. van Bruggen, H. J. Luijendijk
  Department of General Practice, UMCG, PO Box 196, 9700 AD Groningen, The Netherlands. E-mail: h.j.luijendijk@umcg.nl

  References
  1. Erviti J, Wright J, Bassett K et al. Restoring mortality data in the FOURIER cardiovascular outcomes trial of evolocumab in patients with cardiovascular disease: a reanalysis based on regulatory data. BMJ Open. 2022;12:e060172. doi:10.1136/bmjopen-2021-060172
  2. Sabatine MS, Giugliano RP, Keech AC, et al. Evolocumab and Clinical Outcomes in Patients with Cardiovascular Disease. N Engl J Med. 2017;376(18):1713-1722. doi:10.1056/nejmoa1615664
  3. Schwartz GG, Steg PG, Szarek M, et al. Alirocumab and Cardiovascular Outcomes after Acute Coronary Syndrome. N Engl J Med. 2018;379(22):2097-2107. doi:10.1056/nejmoa1801174
  4. Cannon CP, Blazing MA, Giugliano RP, et al. Ezetimibe Added to Statin Therapy after Acute Coronary Syndromes. N Engl J Med. 2015;372(25):2387-2397. doi:10.1056/nejmoa1410489
  5. Eggers KM, Jernberg T, Lindahl B. Unstable Angina in the Era of Cardiac Troponin Assays with Improved Sensitivity—A Clinical Dilemma. Am J Med. 2017. doi:10.1016/j.amjmed.2017.05.037
  6. D’Souza M, Sarkisian L, Saaby L, et al. Diagnosis of Unstable Angina Pectoris Has Declined Markedly with the Advent of More Sensitive Troponin Assays. Am J Med. 2015. doi:10.1016/j.amjmed.2015.01.044
  7. Toušek P, Bauer D, Neuberg M, Nováčková M, Mašek P, Tu Ma P, Kočka V, Moťovská Z WP. Patient characteristics, treatment strategy, outcomes, and hospital costs of acute coronary syndrome: 3 years of data from a large high-volume centre in Central Europe. Eur Hear J. 2022;Mar 30;24. doi:10.1093/eurheartjsupp/suac001
  8. Wiviott SD, Giugliano RP, Morrow DA, et al. Effect of Evolocumab on Type and Size of Subsequent Myocardial Infarction: A Prespecified Analysis of the FOURIER Randomized Clinical Trial. JAMA Cardiol. 2020;5(7):787-793. doi:10.1001/jamacardio.2020.0764
  9. Falk E, Nakano M, Bentzon JF, Finn A V., Virmani R. Update on acute coronary syndromes: The pathologists’ view. Eur Heart J. 2013. doi:10.1093/eurheartj/ehs411
  10. White HD, Gabriel Steg P, Szarek M, et al. Effects of alirocumab on types of myocardial infarction: Insights from the ODYSSEY OUTCOMES trial. Eur Heart J. 2019;40(33):2801-2809. doi:10.1093/eurheartj/ehz299
  11. van Bruggen FH, Nijhuis GBJ, Zuidema SU, Luijendijk HJ. Response to letter to the editor re: ‘serious adverse events and deaths in PCSK9 inhibitor trials reported on ClinicalTrials.gov: a systematic review.’ Expert Rev Clin Pharmacol. 2021. doi:10.1080/17512433.2021.1874350

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  Conflict of Interest:
  None declared.

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