dural tumors

  • 文章类型: Journal Article
    未经批准:难治性脑膜瘤的全身疗法有限,没有FDA批准的疗法。血管内皮生长因子(VEGF)是一种与新生血管形成相关的信号蛋白,瘤周水肿,和脑膜瘤的肿瘤发生。
    未经评估:这项II期研究调查了贝伐单抗(BEV)的疗效,VEGF结合单克隆抗体,在进行性I级(G1M)患者中,二级(G2M),III级(G3M)脑膜瘤,和其他非实质肿瘤,包括前庭神经鞘瘤(n=4)和血管外皮细胞瘤(n=4),主要终点为6个月无进展生存率(PFS-6)。非脑膜瘤包括在分析中的相应脑膜瘤等级。次要终点包括中位总生存期(mOS)和缓解率。
    未经评估:50名患者(26名女性;平均年龄54岁;范围23-81),治疗42例进行性脑膜瘤:10G1M,20G2M,12G3M先前的治疗包括手术切除(41例),放射外科(24名患者),外束放疗(28例),和化疗(14例)。中位输注次数为16次(范围,2-68).使用麦克唐纳的标准对反应进行分级。PFS-6,中位数PFS,MOS为87%,22个月,G1M为35个月;77%,23个月,G2M为41个月;46%,8个月,12个月为G3M。最佳放射学应答包括疾病稳定(G1M:100%;G2M:85%;G3M:82%);部分应答(G1M:0%;G2M:5%;G3M:0%)和疾病进展(G1M:0%;G2M:10%;G3M:18%)。最常见的毒性是高血压(n=19,42.2%),蛋白尿(n=16,35.6%),和疲劳(n=14,31.1%)。
    UNASSIGNED:这项研究表明,BEV具有良好的耐受性,似乎是复发性和难治性脑膜瘤患者的一种有希望的全身治疗选择。
    UNASSIGNED: Systemic therapies for refractory meningiomas are limited with no FDA-approved therapeutics. Vascular endothelial growth factor (VEGF) is a signaling protein associated with neovascularization, peritumoral edema, and meningioma tumorigenesis.
    UNASSIGNED: This phase II study investigates the efficacy of bevacizumab (BEV), a VEGF binding monoclonal antibody, in patients with progressive Grade I (G1M), Grade II (G2M), Grade III (G3M) meningioma, and other non-parenchymal tumors including vestibular schwannoma (n = 4) and hemangiopericytoma (n = 4) with the primary endpoint of progression-free survival rate at 6-months (PFS-6). Non-meningiomas were included with the respective meningioma grade in the analysis. Secondary endpoints include median overall survival (mOS) and response rate.
    UNASSIGNED: Fifty Patients (26 women; median age 54 years; range 23-81), 42 with progressive meningioma were treated: 10 G1M, 20 G2M, and 12 G3M. Prior treatments include surgical resection (41 patients), radiosurgery (24 patients), external beam radiotherapy (28 patients), and chemotherapy (14 patients). Median infusions administered were 16 (range, 2-68). Response was graded using the Macdonald\'s criteria. PFS-6, median PFS, and mOS were 87%, 22 months, 35 months for G1M; 77%, 23 months, 41 months for G2M; and 46%, 8 months, 12 months for G3M. Best radiographic responses include stable disease (G1M: 100%; G2M: 85%; G3M: 82%); partial response (G1M: 0%; G2M: 5%; G3M: 0%) and progressive disease (G1M: 0%; G2M: 10%; G3M:18%). The most common toxicities were hypertension (n = 19, 42.2%), proteinuria (n = 16, 35.6%), and fatigue (n = 14, 31.1%).
    UNASSIGNED: This study showed BEV is well tolerated and appears to be a promising systemic treatment option for patients with recurrent and refractory meningiomas.
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  • 文章类型: Case Reports
    BACKGROUND: It is challenging for neurosurgeons to remove huge tumors involving the skull that may possibly invade the dura or intracranial neural tissue. In this situation, excision of the tumor may cause profound blood loss, unexpected opening of the dura, or neurological injury. We describe a technique of craniotomy in a pediatric patient to avoid surgical complications.
    METHODS: A 15-year-old boy had a huge metastatic calvarial Ewing\'s sarcoma. We removed the tumor successfully with modified concentric craniotomy. First, two oval burr holes are made on both sides of the tumor. The inner craniotomy uses the internal margin of the oval holes, while the outer cut uses the outer margins. The skull bone in between the two craniotomies is removed easily in two pieces and the dura surrounding the tumor can be exposed early in the procedure. In this way, the huge skull tumor can be removed en bloc under direct vision to avoid unwanted complications. Minimal blood and bone loss can be achieved.
    RESULTS: Blood transfusion was not necessary during the surgery. The patient did not have new neurological symptoms and signs after surgery.
    CONCLUSIONS: The goal of the modified concentric craniotomy is to develop an accessible margin of the dura surrounding the bulky tumor in the early phase of surgery. Blood and bone loss can be reduced significantly.
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