AI Article Synopsis
- * CVD complications in MS patients can worsen brain damage, increasing the severity of the disease, but the exact prevalence of cardiovascular problems in MS remains largely unknown and inconsistent.
- * More research, including preclinical studies with animal models, is needed to understand how MS affects cardiac function; clinicians should also monitor cardiovascular health when treating MS patients, as some medications may contribute to CVD risks.
Article Abstract
Autoimmune diseases, including multiple sclerosis (MS), are proven to increase the likelihood of developing cardiovascular disease (CVD) due to a robust systemic immune response and inflammation. MS can lead to cardiovascular abnormalities that are related to autonomic nervous system dysfunction by causing inflammatory lesions surrounding tracts of the autonomic nervous system in the brain and spinal cord. CVD in MS patients can affect an already damaged brain, thus worsening the disease course by causing brain atrophy and white matter disease. Currently, the true prevalence of cardiovascular dysfunction and associated death rates in patients with MS are mostly unknown and inconsistent. Treating vascular risk factors is recommended to improve the management of this disease. This review provides an updated summary of CVD prevalence in patients with MS, emphasizing the need for more preclinical studies using animal models to understand the pathogenesis of MS better. However, no distinct studies exist that explore the temporal effects and etiopathogenesis of immune/inflammatory cells on cardiac damage and dysfunction associated with MS, particularly in the cardiac myocardium. To this end, a thorough investigation into the clinical presentation and underlying mechanisms of CVD must be conducted in patients with MS and preclinical animal models. Additionally, clinicians should monitor for cardiovascular complications while prescribing medications to MS patients, as some MS drugs cause severe CVD.
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|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11337049 | PMC |
| http://dx.doi.org/10.1016/j.heliyon.2024.e35753 | DOI Listing |
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