Colchicine in the Management of Acute Coronary Syndrome: A Meta-analysis

Jason Nogic; Ojas Mehta; David Tong; Adam J Brown; Jamie Layland

doi:10.1007/s40119-022-00298-y

. 2023 Jan 6;12(1):171–181. doi: 10.1007/s40119-022-00298-y

Colchicine in the Management of Acute Coronary Syndrome: A Meta-analysis

Jason Nogic ¹, Ojas Mehta ², David Tong ², Adam J Brown ¹, Jamie Layland ^2,^✉

PMCID: PMC9986187 PMID: 36609745

Abstract

Introduction

Colchicine, thought to exert its effect via reduction of inflammation, has recently been studied in patients following acute coronary syndromes (ACS). We performed a meta-analysis of all available randomized controlled trials (RCTs) in this high-risk cohort, evaluating efficacy and safety.

Methods

MEDLINE, PubMed, EMBASE, clinical trial registries, and select conference proceedings were searched for RCTs comparing colchicine to placebo in patients following ACS. The primary outcome was trial-defined major adverse cardiovascular events (MACE). Secondary endpoints included stroke, myocardial infarction (MI), all-cause and cardiovascular death, and urgent revascularization. Analysis was performed at the longest available clinical follow-up.

Results

Two RCTs with a pooled sample size of 5540 patients with 2778 (50.1%) receiving colchicine and 2762 (49.9%) placebo were included. In order to maximize consistency, composite efficacy endpoints between trials were modified. Compared to placebo, patients receiving colchicine had reduction in study-defined composite endpoint (5.5% vs. 7.6%) OR 0.67 (95% CI 0.46–0.98, p = 0.04, I² = 46%). Similarly, there was a significant reduction in cerebrovascular accidents (OR 0.31, 95% CI 0.14–0.69, p = 0.004, I² = 0%) and repeat revascularization OR 0.36 (95% CI 0.14–0.90, p = 0.03, I² = 54%). There was no difference between cardiovascular death (OR 0.92, 95% CI 0.52–1.62, p = 0.78, I² = 0%), non-cardiovascular death OR 1.27 (95% CI 0.72–2.24, p = 0.41, I² = 0%), MI at longest available follow-up OR 0.89 (95% CI 0.67–1.17, p = 0.39, I² = 0%) or resuscitated cardiac arrest OR 0.88 (95% CI 0.32–2.43, p = 0.81, I² = 0%) in those receiving colchicine.

Conclusions

These data suggest colchicine, in addition to guideline-directed medical therapy following acute coronary syndrome reduces MACE, cerebrovascular accidents, and rates of urgent revascularization at 2 years of follow-up.

Supplementary Information

The online version contains supplementary material available at 10.1007/s40119-022-00298-y.

Keywords: Colchicine, Acute coronary syndrome, Myocardial infarction, MACE

Key Summary Points

Despite improvements in medical therapy, there is ongoing morbidity and mortality following an acute coronary syndrome (ACS).

Recent data have explored the utility of colchicine, a broadly acting anti-inflammatory therapy, to improve outcomes amongst patients with ACS with favorable outcomes.

We performed an updated meta-analysis with modified primary endpoints from our groups study exploring the utility of colchicine amongst patients with recent ACS.

We found that the early administration of colchicine led to reduced rates of major adverse cardiac events.

We await the results of the CLEAR SYNERGY trial to provide more data on the role of colchicine amongst patients with recent ACS.

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Introduction

Acute coronary syndromes remain a major cause of morbidity and mortality worldwide despite improving treatment in recent decades [1]. The role of revascularization, anti-thrombotic, cholesterol lowering, and anti-anginal therapy are now widely accepted as mainstay therapy in patients with coronary artery disease and have seen significant improvement in clinical outcomes [2–4].

Recent studies investigating the use of anti-inflammatory agents have shown promise. Colchicine, an inexpensive and widely available agent with decades of clinical experience, has recently emerged as an adjunct therapy in the treatment of patients with coronary artery disease. It is a broadly acting sophisticated anti-inflammatory therapy that antagonizes the NOD-Like Receptor Protein 3 (NLRP3) inflammasome and cholesterol crystal-induced inflammation [5, 6].

A growing body of evidence supporting the role of colchicine in the management of acute coronary syndromes is emerging. The recent COLCOT and COPS randomized controlled trials have both shown a reduction in ischemic cardiovascular events with the daily use of colchicine in patients who have presented with an acute coronary syndrome [7, 8]. Additionally, the benefit of early administration of colchicine has been studied in ST-segment-elevation myocardial infarction (STEMI), with colchicine showing reduced myocardial infarct size as measured by volume of scar on cardiac MRI and creatine kinase [9]. Although early results are promising, long-term data are still lacking.

While prior meta-analyses have examined the role of colchicine in more chronic cardiovascular disease, there has not been a specific assessment in an extended follow-up ACS cohort. Therefore, we performed a meta-analysis of randomized controlled trials that studied the effects of early colchicine administration in patients who present with acute coronary syndromes compared to placebo at longest available follow-up.

Methods

Study Endpoints and Selection Criteria

Pre-specified primary and secondary endpoints were determined prior to literature search. The primary endpoint was the study-defined combination of major adverse cardiovascular events (MACE). Secondary endpoints included all-cause mortality, cardiovascular death, myocardial infarction (MI), stroke, and need for revascularization. Study criteria for inclusion were as follows: (1) Randomized controlled trials (RCT), (2) studies comparing those receiving colchicine vs. placebo, (3) studies reporting clinical endpoints, (4) at least 1 year of follow-up. Studies were excluded if the primary study population was not acute coronary syndrome.

Literature Search

A comprehensive search of all electronic literature was conducted from inception through to August 2021. PubMed, MEDLINE, and EMBASE databases and Google Scholar, along with conference proceedings and online clinical trial registries, were searched with no restrictions. Searches were performed using Medical Subject Heading (MeSH) and keywords that included, but were not limited to; ‘coronary artery disease’, ‘acute coronary syndrome’, ‘colchicine’, ‘coronary artery disease’. The study protocol was prospectively registered with PROSPERO (CRD42021236504) and adhered to the Preferred Reporting Items For Systematic Reviews and Meta-Analyses (PRISMA) guidelines [10]. An example search strategy for the MEDLINE database and results are provided in Supplementary Table S1.

Two review authors (JN and OM) independently conducted searches based on the pre-specified selection criteria to identify potential trials for inclusion. All citations returned were first screened at title/abstract level to determine suitability for inclusion. Full-text articles and/or conference proceedings were then retrieved and reviewed with studies meeting the inclusion criteria included in the analysis. Additionally, reference lists of the eligible trials were searched for identification of further potential trials to be included. The individual patient inclusion and exclusion criteria for the included trials are provided in Supplementary Table S2.

Data Extraction

Two authors (JN and OM) independently extracted data. Baseline patient characteristics, treatment variables, cardiovascular risk factors, sample size of trials, dosage and duration of colchicine, and clinical follow-up data were recorded. The senior author (JL) subsequently verified the extracted data with discrepancies resolved by consensus.

Bias Assessment

Risk of bias for each trial in the analysis was assessed independently by two review authors (JN and OM) using the Cochrane Collaboration Assessment Tool [11], providing reasons for judgment at a study level. Full details on the risk of bias assessment are presented in Supplementary Fig. S1.

Statistical Analysis

Statistical analysis was performed using Review Manager (RevMan) version 5.3 in line with recommendations from the Cochrane Collaboration and the PRISMA guidelines. Outcomes were analyzed using a Peto random effect models and summary estimates reported as pooled odds ratios (OR) with 95% confidence intervals (CI). Statistical heterogeneity was quantified with the I² statistic. Heterogeneity was defined as low, moderate, or high based on I² values of 25, 50, and 75%, respectively [12]. Analysis was performed on an intention-to-treat basis. Publication bias was estimated visually by funnel plot assessment. A two-sided p value of < 0.05 was considered significant.

Results

As shown in Fig. 1, the search returned two studies of the 74 articles initially screened. These two RCTs included 5540 patients, with 2778 (50.1%) patients receiving colchicine and 2762 (49.9%) patients receiving placebo. The two trials included were the COLCOT and COPS trials, both of which were multi-center randomized trials with mean duration of follow-up of 22.6 and 24 months, respectively. Characteristics of the included trials are outlined in Supplementary Table S3 with summary patient characteristics at baseline shown in Table 1. In brief, 19.4% of patients were female, with 20% having diabetes mellitus and 30.6% being current smokers. Follow-up was available in 96% of study participants in COPS and 98.1% in COLCOT. With regard to colchicine dosing, study participants in COPS received 0.5 mg twice daily for 1 month and then 0.5 mg daily for the remaining 11 months. Patients enrolled in COLCOT received 0.5 mg daily for the duration of the study.

Table 1.

Patient baseline demographics

Study	Age (years)	Male	Smoker	HTN	HChol	Diabetes	Family Hx	STEMI	NSTEMI
COPS 2020	60/60	81/78	32/37	51/50	46/46	19/19	45/36	48/53	48/44
COLCOT 2019	61/61	80/82	30/30	50/52	NR/NR	20/21	NR/NR	NR/NR	NR/NR

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(Colchicine/Placebo) (%)

PCI percutaneous coronary intervention, HTN hypertension, HChol hypercholesterolemia, MI myocardial infarction, NR not-reported, NA not applicable, LVEF left ventricular ejection fraction, CABG coronary artery bypass grafting, ACS acute coronary syndrome

Clinical Outcomes

Both studies reported a composite as their primary endpoint. In order to equalize pooling of composite efficacy endpoints between trials, the primary endpoint of COPS, our groups study, were modified to match the COLCOT definition of MACE. With these amendments, we found that in patients presenting with an acute coronary syndrome, there was a significant reduction in the equalized composite endpoint in patients receiving colchicine compared to placebo (5.5 vs. 7.6%) with an OR of 0.67 (95% CI 0.46–0.98, p = 0.04, I² = 46%) (Fig. 2A). When assessing type of death, there was no significant difference between all-cause death (OR 1.24, 95% CI 0.59–2.63, p = 0.57, I² = 43%) (Fig. 2B), cardiovascular death (OR 0.92, 95% CI 0.52–1.62, p = 0.78, I² = 0%) (Fig. 2C), non-cardiovascular death (OR 1.27, 95% CI 0.72–2.24, p = 0.41, I² = 0%) (Fig. 2D), or resuscitated cardiac arrest (OR 0.88, 95% CI 0.32–2.43, p = 0.81, I² = 0%) (Fig. 2E) in those receiving colchicine versus placebo respectively.

Fig. 2 — Clinical outcomes. Forest plot displaying summary odds ratio (OR) and 95% confidence interval (CI) for A study composite primary endpoint, B all-cause death, C cardiovascular death, D non-cardiovascular death, E resuscitated cardiac arrest, F myocardial infarction, G cerebrovascular accident, and H repeat evascularization

Both trials reported events with regards to vascular outcomes. In patients receiving colchicine, there was no difference in regard to rates of myocardial infarction at longest available follow-up with an OR of 0.89 (95% CI 0.67–1.17, p = 0.39, I² = 0%) (Fig. 2F). There was, however, a significant reduction in the rates of cerebrovascular accidents (OR 0.31, 95% CI 0.14–0.69, p = 0.004, I² = 0%) (Fig. 2G) and repeat revascularization (OR 0.36, 95% CI 0.14–0.90, p = 0.03, I² = 54%) (Fig. 2H) in patients receiving colchicine. A numerical summary of the findings is outlined in Table 2.

Table 2.

Study outcomes

	COPS		COLCOT
	Colchicine, N = 396	Placebo, N = 399	Colchicine, N = 2366	Placebo, N = 2379
Equalized primary composite endpoint: Cardiovascular mortality, resuscitated arrest, myocardial infarction, ischemic stroke, urgent revascularization
Events, N (%)	21 (5.3%)	40 (10.0%)	126 (5.3%)	164 (6.9%)
Combined events, N (%)	Colchicine 152 (5.5%)		Placebo 210 (7.6%)
Summary OR (95% CI)	0.67 (0.46–0.98)
Cardiovascular death
Events, N (%)	4 (1.0%)	2 (0.5%)	20 (0.8%)	24 (1.0%)
Combined events, N (%)	Colchicine 24 (0.9%)		Placebo 26 (0.9%)
Summary OR (95% CI)	0.92 (0.52–1.62)
Resuscitated cardiac arrest
Events, N (%)	2 (2.3%)	2 (1.0%)	5 (1.6%)	6 (1.8%)
Combined events, N (%)	Colchicine 7 (0.25%)		Placebo 8 (0.29%)
Summary OR (95% CI)	0.88 (0.32–2.43)
All-cause death
Events, N (%)	9 (2.3%)	4 (1.0%)	43 (1.6%)	44 (1.8%)
Combined events, N (%)	Colchicine 52 (1.9%)		Placebo 48 (1.7%)
Summary OR (95% CI)	1.24 (0.59–2.63)
Myocardial infarction
Events, N (%)	11 (2.8%)	15 (3.8%)	89 (3.8%)	98 (4.1%)
Combined events, N (%)	Colchicine 100 (3.7%)		Placebo 125 (4.5%)
Summary OR (95% CI)	0.89 (0.67–1.17)
Cerebrovascular accident
Events, N (%)	3 (0.8%)	7 (1.8%)	5 (0.2%)	19 (0.8%)
Combined events, N (%)	Colchicine 8 (0.3%)		Placebo 26 (0.9%)
Summary OR (95% CI)	0.31 (0.14–0.69)
Urgent revascularization
Events, N (%)	3 (0.8%)	16 (4.0%)	25 (0.9%)	50 (1.8%)
Combined events, N (%)	Colchicine 28 (1.0%)		Placebo 66 (2.4%)
Summary OR (95% CI)	0.36 (0.14–0.90)

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N number, OR odds ratio

Publication Bias

The authors abandoned the planned assessment of publication bias given there were less than ten studies in the meta-analysis.

Discussion

This contemporary meta-analysis evaluated randomized studies which evaluated the impact of colchicine administration in patients presenting with an acute coronary syndrome. The addition of colchicine to optimal guideline-directed medical therapy was shown to reduce the adjusted composite endpoint of major adverse cardiovascular events, rates of cerebrovascular events, and the need for urgent coronary revascularization, but did not result in any difference in all cause or cardiovascular mortality. Colchicine is an inexpensive drug with a favorable safety profile that has potential long-term benefits when used early in patients specifically presenting with acute coronary syndromes.

The studies included in this meta-analysis, COLCOT and COPS, had comparable inclusion criteria, patient demographics, and follow-up periods however had a higher proportion of male patients (~ 80%) in both studies. The pooled results demonstrated a reduction in the adjusted composite endpoint of major cardiovascular events, which was primarily driven by a reduction in ischemic stroke and urgent revascularization, both of which showed a statistically significant reduction with the use of colchicine. However, despite not reaching statistical significance, there was a large numerical reduction in myocardial infarction with the use of colchicine. Importantly, given our group conducted the COPS trial, we were able to adjust our combined primary endpoint to include resuscitated cardiac arrest, which brought it in line with COLCOT and is the first time that this specific data have been published. This substantially increases the reliability of the analysis compared to others who have post hoc adjusted composites of the primary endpoint based on limited published data and then undertaken analysis. This gives our study reliability and novelty, along with analysis at 2 years of follow-up.

Both COPS and COLCOT initiated treatment with colchicine either prior to discharge (COPS) or within 30 days of index event (COLCOT). Moreover, a prespecified analysis of time to treatment in the COLCOT supported a premise of earlier administration of colchicine within 3 days. Thus, early administration of colchicine appears to be important in reducing future events.

The original COPS trial reported an increase in all-cause death (8 vs. 1, P = 0.017) with the use of colchicine. At that time, we recognized the possibility of a type 1 error, given the small number of events. Recognizing that, as the study drug was discontinued at 12 months in COPS, the extended results over 24 months demonstrated this difference became non-significant (9 vs. 4, p = 0.17). This meta-analysis provides reassurance as to the safety of colchicine when administered in the acute phase of an ACS.

Both studies reported a similarity in adverse events between colchicine and placebo groups. Gastrointestinal (GI) adverse events, commonly associated with the use of colchicine, occurred at similar rates in the colchicine and placebo groups. The COPS study, which had twice the dose of colchicine administered initially (0.5 mg twice daily compared to 0.5 mg daily), reported a 23% incidence of GI events, compared to COLCOT, which reported a 17.5%. Dose-related comparison in GI adverse events is limited however due to the presence of similar rates of GI events in the placebo group in both studies. The incidence of GI events in these studies is comparable to what is commonly reported with the use of colchicine [13]. The COLCOT trial detected an increased rate of pneumonia with the colchicine arm (21 vs. 9, p = 0.03). While it could be theorized that this difference is explained by immunosuppressive properties of colchicine, this effect was not observed in COPS with no significant differences in other infections or septic shock. Although a different patient population, a systematic review on the use of colchicine did not find a greater rate of infection [13]. Overall, these findings support that colchicine has an acceptable safety profile and given it was discontinued after 1 year, further analysis on side-effects was neither warranted nor possible.

Colchicine is an efficacious, cost-effective, and safe drug. Similar to canakinumab in the CANTOS trial, its mechanisms in cardiovascular disease hinge on the interaction between atherosclerosis and inflammation. The NLRP3 inflammasome is a cytoplasmic protein complex that promotes the formation of proinflammatory interleukins, including IL-1β [14, 15] with NLRP3 inflammasomes an important component in the development of atherosclerotic disease. Animal studies support this with Duewell et al. showing that NLRP3-deficient mice, when fed a high-cholesterol diet, had significantly less atherosclerosis [14]. The presence of cholesterol crystals are themselves triggers for the activation of the NLRP3 inflammasome and do so in a dose-dependent manner, establishing the relationship between inflammation and cholesterol metabolism [15].

Inhibitors of angiotensin-converting enzyme (ACE) and beta-blockers have both been shown to be efficacious when initiated early in patients presenting with acute coronary syndromes. ACE inhibitors exert their effect through a reduction of neurohormonal activation and thus favorably alter ventricular remodeling. Meta-analysis of over 100,000 patients showed a significant benefit with ACE inhibitor use with a 7% reduction in 30-day mortality [16, 17]. Similarly, beta-blockers, through their reduction of myocardial workload and oxygen demand, heart rate, blood pressure, catecholamine levels, and decrease of myocardial demand, have been shown to have a mortality benefit of up to 23% in long-term trials [18–21]. However, the importance of this effect has been met with controversy, as many older trials pre-date the era of statin and coronary reperfusion therapy, where beta-blockers have had equivocal benefit [22]. In fact, the ongoing DANBLOCK trial seeks to investigate the benefit of beta-blockers in patients post myocardial infarction with preserved ejection fraction [23]. In contrast to the modes of action of beta-blockers and ACE inhibitors, colchicine alters patient prognosis by modifying conditions that would portend a risk of plaque rupture, through its anti-inflammatory action. Although our results did not show mortality benefit, they revealed a significant 32% reduction in adjusted MACE, along with a 69% reduction in CVA and 67% reduction in the need for urgent revascularization with little risk of medication side effects. These data suggest that colchicine may be of benefit post ACS; however, prior to being incorporated into guidelines, it would be prudent to await the results of the CLEAR SYNERGY trial with 7000 patients and COLCARDIO-ACS trial with 3000 patients assessing similar outcomes also in an acute coronary syndrome cohort.

Limitations

This meta-analysis confers greater confidence in the efficacy and safety of colchicine when used early in patients presenting with acute coronary syndrome. These results, however, must be viewed with regard to their limitations. Firstly, long-term follow-up periods are currently not available. With only 2 years of data published, the optimal duration of treatment and long-term benefit is still not known. Longer follow-up periods are necessary to establish the long-term efficacy. Second, there were differences in the definition of primary outcome between the two trials. Although we attempted to minimize heterogeneity through the adjustment of outcomes to be more consistent with each other, it must be noted that there are differences in the original trial outcomes and that only two studies are included in this analysis.

Conclusions

In patients presenting with an acute coronary syndrome, these data suggest that the addition of colchicine commenced during index hospitalization, in combination with guideline directed medical therapy reduces rates of major adverse cardiovascular events, cerebrovascular accidents, and need for revascularization compared to standard therapy alone.

Supplementary Information

Below is the link to the electronic supplementary material.

Supplementary file1 (PDF 158 KB)^{(157.7KB, pdf)}

Acknowledgements

Funding

No funding or sponsorship was received for this study or publication of this article.

Author Contributions

JL: Designed study, involved in initial manuscript writing and all further versions of the paper. AB: Provided appraisal of paper and all further versions of manuscript.JN: Performed initial literature review, statistical analysis, wrote initial version of manuscript.DT: Provided appraisal of paper and all further versions of manuscript.OM: Provided appraisal of paper and all further versions of manuscript.All authors take responsibility for all aspects of the reliability and freedom from bias of the data presented and their discussed interpretation.

Disclosures

Jason Nogic, Ojas Mehta, David Tong, Adam J. Brown, and Jamie Layland have nothing to disclose.

Compliance with Ethics Guidelines

This article is based on previously conducted studies and does not contain any new studies with human participants or animals performed by any of the authors.

Data Availability

The data underlying this article are available online, in the article and in its online supplementary material.

Footnotes

Original online version of this article was revised: Correct version of figure 1 updated.

The original online version of this article was revised: Corrected version of figure 2 updated.

Change history

7/6/2023

A Correction to this paper has been published: 10.1007/s40119-023-00324-7

Change history

2/15/2023

A Correction to this paper has been published: 10.1007/s40119-023-00306-9

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Associated Data

This section collects any data citations, data availability statements, or supplementary materials included in this article.

Supplementary Materials

Supplementary file1 (PDF 158 KB)^{(157.7KB, pdf)}

Data Availability Statement

The data underlying this article are available online, in the article and in its online supplementary material.

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PERMALINK

Colchicine in the Management of Acute Coronary Syndrome: A Meta-analysis

Jason Nogic

Ojas Mehta

David Tong

Adam J Brown

Jamie Layland

Abstract

Introduction

Methods

Results

Conclusions

Supplementary Information

Key Summary Points

Introduction

Methods

Study Endpoints and Selection Criteria

Literature Search

Data Extraction

Bias Assessment

Statistical Analysis

Results

Fig. 1.

Table 1.

Clinical Outcomes

Fig. 2.

Table 2.

Publication Bias

Discussion

Limitations

Conclusions

Supplementary Information

Acknowledgements

Funding

Author Contributions

Disclosures

Compliance with Ethics Guidelines

Data Availability

Footnotes

References

Associated Data

Supplementary Materials

Data Availability Statement

ACTIONS

PERMALINK

RESOURCES

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