Implications of MMP-12 in the Pathophysiology of Ischaemic Stroke

Overview

Journal Stroke Vasc Neurol

Specialty Cardiology & Vascular Diseases

Date 2023 Jun 19

PMID 37336584

Authors

Krishna Kumar Veeravalli

Affiliations

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Abstract

This article focuses on the emerging role of matrix metalloproteinase-12 (MMP-12) in ischaemic stroke (IS). MMP-12 expression in the brain increases dramatically in animal models of IS, and its suppression reduces brain damage and promotes neurological, sensorimotor and cognitive functional outcomes. Thus, MMP-12 could represent a potential target for the management of IS. This article provides an overview of MMP-12 upregulation in the brain following IS, its deleterious role in the post-stroke pathogenesis (blood-brain barrier disruption, inflammation, apoptosis and demyelination), possible molecular interactions and mechanistic insights, its involvement in post-ischaemic functional deficits and recovery as well as the limitations, perspectives, challenges and future directions for further research. Prior to testing any MMP-12-targeted therapy in patients with acute IS, additional research is needed to establish the effectiveness of MMP-12 suppression against IS in older animals and in animals with comorbidities. This article also examines the clinical implications of suppressing MMP-12 alone or in combination with MMP-9 for extending the currently limited tissue plasminogen activator therapy time window. Targeting of MMP-12 is expected to have a profound influence on the therapeutic management of IS in the future.

Citing Articles

Association of GWAS-Reported Variant of Matrix Metalloproteinase 12 Gene with Susceptibility to Ischemic Stroke in Southern Chinese Population.

Chen L, Liao K, Zhang Y, Zheng S, He J, Tang H J Inflamm Res. 2024; 17:9231-9241.

PMID: 39583862 PMC: 11585993. DOI: 10.2147/JIR.S487321.

Perspective from single-cell sequencing: Is inflammation in acute ischemic stroke beneficial or detrimental?.

Deng X, Hu Z, Zhou S, Wu Y, Fu M, Zhou C CNS Neurosci Ther. 2023; 30(1):e14510.

PMID: 37905592 PMC: 10805403. DOI: 10.1111/cns.14510.

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