自发性颈内动脉夹层:它真的是一种结缔组织病吗?一项全面综述。
Spontaneous cervical artery dissection: is it really a connective tissue disease? A comprehensive review.
作者信息
Gunduz Muhammed Enes, Kadirvel Ramanathan, Kallmes David F, Pezzini Alessandro, Keser Zafer
机构信息
Department of Neurology, University of Massachusetts Chan Medical School, Worcester, MA, United States.
Department of Neurosurgery, Mayo Clinic, Rochester, MN, United States.
出版信息
Front Neurol. 2023 Oct 11;14:1241084. doi: 10.3389/fneur.2023.1241084. eCollection 2023.
BACKGROUND
Spontaneous cervical artery dissection (sCeAD) is an important cause of stroke in young adults. The underlying pathophysiology remains unclear, without validated biomarkers to identify subjects at risk. Previous studies suggested the role of abnormalities in the connective component of the arterial wall.
PURPOSE
To assess dermal ultrastructural aberrations of connective tissue by skin biopsy and genetic variations in sCeAD patients.
METHOD
We searched the PubMed and Scopus databases until August 2023 with PRISMA guidelines. Original articles assessing skin biopsy in sCeAD patients were included. Two reviewers independently conducted the screening.
FINDINGS
We included 16 studies compromising 459 patients. Thirteen studies assessed ultrastructural changes and found aberrations of collagen and elastic fibers, described as irregular contours and calibers of collagen fibrils, composite flower-like fibrils, fragmented moth-eaten elastin, and microcalcifications, cumulatively in 50.5% of patients. Seven studies showed no causative mutations in collagen type I, III, V, or elastin genes. One study showed linkage between connective tissue alterations and mutation on chromosomes 15q2 and 10q26 using genome-wide linkage analysis, while another study found significant copy number variant enrichments in genes involved in extracellular matrix (COL5A2/COL3A1/SNTA1) and collagen fibril organizations (COL5A2/COL3A1). Finally, differential expression of extracellular proteins was linked to connective tissue disorder in patients with recurrent sCeAD using a quantitative proteomics approach.
CONCLUSION
Current literature supports the hypothesis that an underlying, subclinical connective tissue disorder, likely genetically determined, may predispose to arterial wall weakness and sCeAD. Further studies with larger sample sizes and robust methodology are needed to better define the role of connective tissue in sCeAD pathogenesis.
背景
自发性颈内动脉夹层(sCeAD)是年轻成年人中风的重要原因。其潜在的病理生理学仍不清楚,尚无经过验证的生物标志物来识别高危人群。先前的研究提示了动脉壁结缔组织成分异常的作用。
目的
通过皮肤活检评估sCeAD患者结缔组织的真皮超微结构异常及基因变异。
方法
我们按照PRISMA指南检索了截至2023年8月的PubMed和Scopus数据库。纳入评估sCeAD患者皮肤活检的原始文章。两名审阅者独立进行筛选。
结果
我们纳入了16项研究,共459例患者。13项研究评估了超微结构变化,发现胶原纤维和弹性纤维异常,表现为胶原原纤维轮廓和直径不规则、复合花状纤维、破碎虫蚀样弹性蛋白以及微钙化,累计见于50.5%的患者。7项研究显示I型、III型、V型胶原或弹性蛋白基因无致病突变。一项研究使用全基因组连锁分析显示结缔组织改变与15q2和10q26染色体上的突变之间存在连锁关系,而另一项研究发现细胞外基质相关基因(COL5A2/COL3A1/SNTA1)和胶原纤维组织相关基因(COL5A2/COL3A1)存在显著的拷贝数变异富集。最后,使用定量蛋白质组学方法发现复发性sCeAD患者细胞外蛋白的差异表达与结缔组织疾病有关。
结论
当前文献支持以下假说,即潜在的、可能由基因决定的亚临床结缔组织疾病可能易导致动脉壁薄弱和sCeAD。需要进一步开展样本量更大、方法更可靠的研究,以更好地明确结缔组织在sCeAD发病机制中的作用。
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