Association Between Antiseizure Medication Use and Cardiovascular Events in Older People With Epilepsy

The incidence and prevalence of epilepsy are highest among adults older than 60 years. In our rapidly aging population, we will be caring for an increasing number of older adults with epilepsy, including those with chronic epilepsy and people with late-onset epilepsy. Epilepsy, especially late-onset epilepsy, in older adults is more responsive to antiseizure medications (ASMs) compared with that in younger adults.¹ However, there are some unique challenges in managing ASMs in this population, chiefly age-related comorbidities, polypharmacy, and frailty.^2,3

More than a decade ago, evidence started to emerge that enzyme-inducing ASMs (EIASMs) like phenytoin or carbamazepine worsen cholesterol control and vascular risks, which is reversible when the patient is switched to newer-generation ASMs like lamotrigine or levetiracetam.⁴ Further research has confirmed these findings and found that EIASM use is associated with higher healthcare expenditures.^5,6 Regardless, they remain the predominant ASM type used among this population in Western countries like the US, the UK, and Canada.^6-8 Now, one can hope that the article by Li et al discussed here would catalyze a reversal in this prescribing trend.

A previous study by the same group of researchers used 30 years of data from England's National Health Services and found that the hazard of new cardiovascular diseases (CVD; including myocardial infarction, stable or unstable angina, transient ischemic attack, and ischemic or hemorrhagic stroke) is significantly higher among patients prescribed EIASMs.⁹ However, the risk of CVD increases with age in the general population. CVD serves as a common cause of late-onset epilepsy.¹ Conversely, there is evidence to suggest that chronic epilepsy increases the CVD risk due to repeated seizure-related surges in catecholamines and hypoxemia, culminating in electrical and mechanical dysfunction.¹⁰ Li et try to tackle the problem of the "chicken or the egg" conundrum of increased CVD risk among older adults with epilepsy, specifically the role of EIASMs and typical CVD risk factors.

The investigators analyzed a prospective Canadian cohort of adults aged 45 years or older with 6 years of follow-up. They found that nearly a third of the heightened CVD risk among older adults with epilepsy could be attributed to EIASMs. Surprisingly, only 4% of the EIASM effect on CVD was mediated by incident dyslipidemia. This study has clear implications for clinical practice, particularly in medication selection for older patients with epilepsy who may already have cardiovascular risk factors. Clinicians managing epilepsy in older adults frequently balance seizure control with the patient's overall health status, including cardiovascular risk management. Given that many ASMs are associated with lipid abnormalities and other pro-atherogenic effects, this study suggests a re-evaluation of EIASM use in favor of non–enzyme-inducing ASMs (non-EIASMs), particularly in patients with a pre-existing cardiovascular risk. EIASMs, including carbamazepine, phenytoin, and phenobarbital, are shown to influence lipid levels and inflammatory markers like C-reactive protein, which contribute to atherosclerosis progression.¹¹ The study's mediation analysis supports this, revealing that strong EIASM use is the predominant modifiable risk factor among those studied.

Additionally, the findings emphasize the role of lifestyle factors, such as physical activity and obesity, in mediating the risk of cardiovascular events (CVEs) in patients with epilepsy. Lower physical activity and higher waist-to-hip ratios were found to be associated with an increased CVE risk, underscoring the value of a comprehensive approach to managing epilepsy in older adults. Encouraging physical activity and weight management, alongside careful medication selection, may help reduce the long-term cardiovascular burden in this population.

Ultimately, the study underscores the importance of cross-specialty collaboration in managing older adults with epilepsy. Neurologists, cardiologists, and primary care providers should work together to monitor these patients' cardiovascular health, mainly when using EIASMs. This collaborative approach is crucial in cases where seizure control necessitates EIASM use, as clinicians might consider adjunct therapies or more frequent monitoring of lipid profiles and inflammatory markers to mitigate these risks. The necessity of this teamwork should be felt by all healthcare professionals involved in the care of older adults with epilepsy.

A formidable clinical challenge may arise when older adults with well-controlled epilepsy on EIASMs develop CVD, requiring a switch to non-EIASMs for secondary prophylaxis. This may require nuanced, informed decision-making with the patient and other care providers to balance the risk of breakthrough seizures against preventing future CVDs. Although there are not much data to inform counsel, a small study found a modest breakthrough seizure risk of approximately 15% associated with switching EIASMs in well-controlled patients compared with maintaining the same regimen.

In conclusion, the highlighted study provides compelling evidence that EIASMs contribute substantially to CVD risk. This evidence should motivate clinicians treating older adults with epilepsy to avoid the use of EIASMs and shift their practice toward non-EIASMs. Integrating these findings into clinical practice could lead to improved long-term outcomes and quality of life for older adults managing both epilepsy and cardiovascular risks.​¹²

References

1. Punia V, Bhansali S, Tsai C. Late-Onset Epilepsy Clinic: From Clinical Diagnostics to Biomarkers. Seizure. 2024 Jun 26. Doi: 10.1016/j.seizure.2024.06.026. Online ahead of print. https://www.seizure-journal.com/article/S1059-1311(24)00192-4/fulltext
2. Hashmi SA, Sachdeva S, Sindhu U, et al. The Implications of Frailty in Older Adults with Epilepsy. Epilepsia Open. 2024 Sep 9. Doi: 10.1002/epi4.13046. Online ahead of print. https://onlinelibrary.wiley.com/doi/10.1002/epi4.13046
3. Punia V. Start Low and Go Slow: The General Principle of Managing Older Adults With Epilepsy Finds Robust Support From Frailty. Epilepsy Curr. 2023;23(4):235-237. https://journals.sagepub.com/doi/10.1177/15357597231178072
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6. Borghs S, Byram L, Chan J, et al. Comparing Healthcare Costs Associated with the Use of Enzyme-Inducing and Non-Enzyme Active Antiepileptic Drugs in Elderly Patients with Epilepsy in the UK: A Long-Term Retrospective, Matched Cohort Study. BMC Neurol. 2020;20(1):7. https://bmcneurol.biomedcentral.com/articles/10.1186/s12883-019-1587-9
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8. Mintzer S, Maio V, Foley K. Use of Antiepileptic Drugs and Lipid-Lowering Agents in the United States. Epilepsy Behav. 2014;34:105-108. https://www.epilepsybehavior.com/article/S1525-5050(14)00089-4/abstract
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12. Finamore JM, Sperling MR, Zhan T, et al. Seizure Outcome After Switching Antiepileptic Drugs: A Matched, Prospective Study. Epilepsia. 2016;57(8):1294-1300. https://onlinelibrary.wiley.com/doi/10.1111/epi.13435