Safety and Tolerability of CSL112, a Reconstituted, Infusible, Plasma-Derived Apolipoprotein A-I, After Acute Myocardial Infarction: The AEGIS-I Trial (ApoA-I Event Reducing in Ischemic Syndromes I).

dc.contributor.author

Michael Gibson, C

dc.contributor.author

Korjian, Serge

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Tricoci, Pierluigi

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Daaboul, Yazan

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Yee, Megan

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Jain, Purva

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Alexander, John H

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Steg, P Gabriel

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Lincoff, A Michael

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Kastelein, John JP

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Mehran, Roxana

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D'Andrea, Denise M

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Deckelbaum, Lawrence I

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Merkely, Bela

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Zarebinski, Maciej

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Ophuis, Ton Oude

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Harrington, Robert A

dc.date.accessioned

2021-05-10T18:11:53Z

dc.date.available

2021-05-10T18:11:53Z

dc.date.issued

2016-12

dc.date.updated

2021-05-10T18:11:52Z

dc.description.abstract

Background

Human or recombinant apolipoprotein A-I (apoA-I) has been shown to increase high-density lipoprotein-mediated cholesterol efflux capacity and to regress atherosclerotic disease in animal and clinical studies. CSL112 is an infusible, plasma-derived apoA-I that has been studied in normal subjects or those with stable coronary artery disease. This study aimed to characterize the safety, tolerability, pharmacokinetics, and pharmacodynamics of CSL112 in patients with a recent acute myocardial infarction.

Methods

The AEGIS-I trial (Apo-I Event Reducing in Ischemic Syndromes I) was a multicenter, randomized, double-blind, placebo-controlled, dose-ranging phase 2b trial. Patients with myocardial infarction were stratified by renal function and randomized 1:1:1 to CSL112 (2 g apoA-I per dose) and high-dose CSL112 (6 g apoA-I per dose), or placebo for 4 consecutive weekly infusions. Coprimary safety end points were occurrence of either a hepatic safety event (an increase in alanine transaminase >3 times the upper limit of normal or an increase in total bilirubin >2 times the upper limit of normal) or a renal safety event (an increase in serum creatinine >1.5 times the baseline value or a new requirement for renal replacement therapy).

Results

A total of 1258 patients were randomized, and 91.2% received all 4 infusions. The difference in incidence rates for an increase in alanine transaminase or total bilirubin between both CSL112 arms and placebo was within the protocol-defined noninferiority margin of 4%. Similarly, the difference in incidence rates for an increase in serum creatinine or a new requirement for renal replacement therapy was within the protocol-defined noninferiority margin of 5%. CSL112 was associated with increases in apoA-I and ex vivo cholesterol efflux similar to that achieved in patients with stable coronary artery disease. In regard to the secondary efficacy end point, the risk for the composite of major adverse cardiovascular events among the groups was similar.

Conclusions

Among patients with acute myocardial infarction, 4 weekly infusions of CSL112 are feasible, well tolerated, and not associated with any significant alterations in liver or kidney function or other safety concern. The ability of CSL112 to acutely enhance cholesterol efflux was confirmed. The potential benefit of CSL112 to reduce major adverse cardiovascular events needs to be assessed in an adequately powered phase 3 trial.

Clinical trial registration

URL: https://clinicaltrials.gov. Unique identifier: NCT02108262.
dc.identifier

CIRCULATIONAHA.116.025687

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0009-7322

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1524-4539

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https://hdl.handle.net/10161/22871

dc.language

eng

dc.publisher

Ovid Technologies (Wolters Kluwer Health)

dc.relation.ispartof

Circulation

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10.1161/circulationaha.116.025687

dc.subject

Humans

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Myocardial Infarction

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Acute Disease

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Hemorrhage

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Creatinine

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Bilirubin

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Alanine Transaminase

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Lipoproteins, HDL

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Treatment Outcome

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Drug Administration Schedule

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Proportional Hazards Models

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Double-Blind Method

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Placebo Effect

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Dose-Response Relationship, Drug

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Half-Life

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Adult

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Aged

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Middle Aged

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Female

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Male

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Biomarkers

dc.title

Safety and Tolerability of CSL112, a Reconstituted, Infusible, Plasma-Derived Apolipoprotein A-I, After Acute Myocardial Infarction: The AEGIS-I Trial (ApoA-I Event Reducing in Ischemic Syndromes I).

dc.type

Journal article

duke.contributor.orcid

Alexander, John H|0000-0002-1444-2462

pubs.begin-page

1918

pubs.end-page

1930

pubs.issue

24

pubs.organisational-group

Faculty

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Duke

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School of Medicine

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Duke Clinical Research Institute

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Medicine, Cardiology

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Institutes and Centers

pubs.organisational-group

Medicine

pubs.organisational-group

Clinical Science Departments

pubs.publication-status

Published

pubs.volume

134

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