Current trends, molecular insights, and future directions toward precision medicine in the management of pediatric cerebral arteriovenous malformations.

IF 2.1 3区 医学 Q3 CLINICAL NEUROLOGY
Journal of neurosurgery. Pediatrics Pub Date : 2024-09-06 Print Date: 2024-11-01 DOI:10.3171/2024.6.PEDS22354
H Westley Phillips, Regan M Shanahan, Clementina Aiyudu, Tracy A Miller, Hilary Y Liu, Stephanie Greene
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引用次数: 0

Abstract

Pediatric arteriovenous malformations (AVMs) are rare but carry a risk of devastating neurological morbidity and mortality. Rupture of a cerebral AVM is the most common cause of spontaneous intracranial hemorrhage in children, with an unruptured AVM having an approximate hemorrhage risk of 2%-4% per year. The complex etiology of pediatric AVMs persists as an impediment to a comprehensive understanding of pathogenesis and subsequent targeted gene therapies. While AVMs secondary to vascular malformation syndromes have a clearer pathogenesis, a variety of gene mutations have been identified within sporadic AVM cases. The Ephrin B2/EphB4 (RASA-1, KRAS, and MEK) signaling axis, hemorrhagic telangiectasia, NOTCH, and TIE2 receptor complexes (PIK3CA and mTOR), in addition to other isolated gene variants, have been implicated in AVM pathogenesis. Furthering the understanding of the molecular mechanisms of AVM pathogenesis will lead to future novel therapies and treatment paradigms. Given the expected lifespan of a child, pediatric patients have an unacceptably high cumulative lifetime risk of hemorrhage. AVM treatment strategies are dependent on AVM grade, provider preference, and institutional resources. While open microsurgery is the mainstay of treatment for some AVMs, radiosurgery for definitive treatment and adjunctive endovascular embolization are also used extensively. There is increasing evidence indicating that all three modalities play important and potentially synergistic roles in the armamentarium for pediatric AVM treatment. This review serves to report current understanding in the genetic and molecular mechanisms of pediatric AVMs, review clinical diagnostic and classification criteria, and detail treatment options and subsequent outcomes of pediatric AVM patients.

小儿脑动静脉畸形精准医疗管理的当前趋势、分子见解和未来方向。
小儿动静脉畸形(AVM)虽然罕见,但却有可能导致毁灭性的神经系统发病和死亡。脑动静脉畸形破裂是导致儿童自发性颅内出血的最常见原因,未破裂的动静脉畸形每年约有 2%-4% 的出血风险。小儿动静脉畸形的病因复杂,一直阻碍着人们对其发病机制的全面了解和后续的靶向基因疗法。虽然继发于血管畸形综合征的 AVM 的发病机制较为明确,但在散发性 AVM 病例中也发现了多种基因突变。Ephrin B2/EphB4(RASA-1、KRAS 和 MEK)信号轴、出血性毛细血管扩张症、NOTCH 和 TIE2 受体复合物(PIK3CA 和 mTOR)以及其他孤立的基因变异都与 AVM 的发病机制有关。进一步了解 AVM 发病的分子机制将有助于开发新的疗法和治疗模式。考虑到儿童的预期寿命,儿科患者终生累积出血风险之高令人难以接受。动静脉畸形的治疗策略取决于动静脉畸形的等级、提供者的偏好和机构资源。虽然开放显微外科手术是治疗某些动静脉畸形的主要方法,但放射外科手术和辅助性血管内栓塞也被广泛用于最终治疗。越来越多的证据表明,这三种治疗方式在小儿视网膜血管瘤的治疗中发挥着重要且可能协同增效的作用。本综述旨在报告目前对小儿动静脉畸形遗传和分子机制的认识,回顾临床诊断和分类标准,并详细介绍小儿动静脉畸形患者的治疗方案和后续疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of neurosurgery. Pediatrics
Journal of neurosurgery. Pediatrics 医学-临床神经学
CiteScore
3.40
自引率
10.50%
发文量
307
审稿时长
2 months
期刊介绍: Information not localiced
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