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靶向动脉内抗血管内皮生长因子治疗脑内难治性放射性坏死

Targeted intraarterial anti-VEGF therapy for medically refractory radiation necrosis in the brain.

作者信息

Dashti Shervin R, Spalding Aaron, Kadner Rob J, Yao Tom, Kumar Arooshi, Sun David A, LaRocca Renato

机构信息

Norton Neuroscience Institute and.

出版信息

J Neurosurg Pediatr. 2015 Jan;15(1):20-5. doi: 10.3171/2014.9.PEDS14198.

Abstract

Radiation necrosis (RN) is a serious complication that can occur in up to 10% of brain radiotherapy cases, with the incidence dependent on both dose and brain location. Available medical treatment for RN includes steroids, vitamin E, pentoxifylline, and hyperbaric oxygen. In a significant number of patients, however, RN is medically refractory and the patients experience progressive neurological decline, disabling headaches, and decreased quality of life. Vascular endothelial growth factor (VEGF) is a known mediator of cerebral edema in RN. Recent reports have shown successful treatment of RN with intravenous bevacizumab, a monoclonal antibody for VEGF. Bevacizumab, however, is associated with significant systemic complications including sinus thrombosis, pulmonary embolus, gastrointestinal tract perforation, wound dehiscence, and severe hypertension. Using lower drug doses may decrease systemic exposure and reduce complication rates. By using an intraarterial route for drug administration following blood-brain barrier disruption (BBBD), the authors aim to lower the bevacizumab dose while increasing target delivery. In the present report, the authors present the cases of 2 pediatric patients with cerebral arteriovenous malformations, who presented with medically intractable RN following stereotactic radiosurgery. They received a single intraarterial infusion of 2.5 mg/kg bevacizumab after hyperosmotic BBBD. At mean follow-up duration of 8.5 months, the patients had significant and durable clinical and radiographic response. Both patients experienced resolution of their previously intractable headaches and reversal of cushingoid features as they were successfully weaned off steroids. One of the patients regained significant motor strength. There was an associated greater than 70% reduction in cerebral edema. Intraarterial administration of a single low dose of bevacizumab after BBBD was safe and resulted in durable clinical and radiographic improvements at concentrations well below those required for the typical systemic intravenous route. Advantages over the intravenous route may include higher concentration of drug delivery to the affected brain, decreased systemic toxicity, and a significantly lower cost.

摘要

放射性坏死(RN)是一种严重的并发症,在高达10%的脑部放射治疗病例中可能发生,其发生率取决于剂量和脑部位置。现有的针对RN的医学治疗方法包括类固醇、维生素E、己酮可可碱和高压氧。然而,在相当数量的患者中,RN对药物治疗无效,患者会出现进行性神经功能衰退、致残性头痛和生活质量下降。血管内皮生长因子(VEGF)是RN中脑水肿的已知介质。最近的报告显示,使用静脉注射贝伐单抗(一种针对VEGF的单克隆抗体)成功治疗了RN。然而,贝伐单抗与包括鼻窦血栓形成、肺栓塞、胃肠道穿孔、伤口裂开和严重高血压在内的显著全身并发症有关。使用较低的药物剂量可能会减少全身暴露并降低并发症发生率。通过在血脑屏障破坏(BBBD)后采用动脉内给药途径,作者旨在降低贝伐单抗剂量,同时增加靶向递送。在本报告中,作者介绍了2例患有脑动静脉畸形的儿科患者的病例,这些患者在立体定向放射外科手术后出现了药物难治性RN。在渗透性BBBD后,他们接受了一次2.5mg/kg贝伐单抗的动脉内输注。平均随访8.5个月时,患者有显著且持久的临床和影像学反应。两名患者之前难治性的头痛均得到缓解,随着成功停用类固醇,库欣样特征也得到逆转。其中一名患者恢复了显著的运动力量。脑水肿减少了70%以上。BBBD后单次低剂量动脉内注射贝伐单抗是安全的,并且在远低于典型全身静脉途径所需浓度的情况下,产生了持久的临床和影像学改善。与静脉途径相比,其优势可能包括更高浓度的药物递送至受影响的脑部、降低全身毒性以及显著更低的成本。

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