Involvement of Matrix Metalloproteinase 9 in Vertebral Arterial Dissection With Posterior Circulation Ischemic Stroke

Author:

Chen Chun‐Yu12,Chang Feng‐Chi32,Lee I‐Hui124ORCID,Chung Chih‐Ping12ORCID

Affiliation:

1. Department of Neurology Neurological Institute Taipei Veterans General Hospital Taipei Taiwan

2. Department of Neurology National Yang‐Ming University Taipei Taiwan

3. Department of Radiology Taipei Veterans General Hospital Taipei Taiwan

4. Institute of Brain Science School of Medicine National Yang‐Ming University Taipei Taiwan

Abstract

Background Spontaneous vertebral arterial dissection (VAD) is an important cause of posterior circulation ischemic stroke (PCS), but its pathogenesis remains elusive. Matrix metalloproteinase 9 (MMP‐9) is a gelatinase involved in inflammation process and several vascular diseases, such as aorta dissection, but its role in VBD is unclear yet. The present study aimed to determine the association between serum MMP‐9 level and VAD‐related PCS. Methods and Results We recruited 149 patients with PCS, of which 30 were VAD and 119 had other determined etiologies (non‐VAD), and 219 non‐stroke individuals. Serum MMP‐9 was measured within 14 days from stroke onset. The age of VAD group was 59.6±15.0 years, which is similar to non‐stroke group ( P =0.510) but significantly younger than non‐VAD group (69.9±14.0 years, P <0.001). Males and vascular risk factors were significantly more prevalent in VAD and non‐VAD groups than non‐stroke group ( P <0.001). Multivariate logistic regression analysis adjusting potential confounders revealed that every 100 ng/mL of serum MMP‐9 level increment significantly predicted VAD (versus non‐stroke group: odds ratio (OR), 4.572; 95% CI, 2.240–9.333, P <0.001; versus non‐VAD group: OR, 1.819; 95% CI, 1.034–3.200, P =0.038). Conclusions Patients with VAD‐related PCS had higher levels of serum MMP‐9 at the acute stage of stroke compared with non‐stroke individuals and PCS of other causes, supporting the potential involvement of extracellular matrix‐degrading protease in the mechanism of VAD, which leads to ischemic events.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

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