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针对影响脑部的大型原发性肿瘤的两阶段放射外科治疗。

Two-Session Radiosurgery for Large Primary Tumors Affecting the Brain.

作者信息

Lovo Eduardo E, Barahona Kaory C, Campos Fidel, Caceros Victor, Tobar Carlos, Reyes William A

机构信息

Radiosurgery, International Cancer Center, Diagnostic Hospital, San Salvador, SLV.

Radiation Oncology, International Cancer Center, Diagnostic Hospital, San Salvador, SLV.

出版信息

Cureus. 2020 Apr 27;12(4):e7850. doi: 10.7759/cureus.7850.

Abstract

Introduction Surgery is an option for patients with large, symptomatic primary tumors affecting the brain. However, surgery might not be suitable for all tumors, especially those located in sensitive areas such as the pineal region and the hypothalamus. Single-session stereotactic radiosurgery (SRS) might not provide an adequate dose for long-term local control due to the initial tumor volume and the involvement of radiation sensitive organs at risk (OARs). Two-session radiosurgery has been described as a feasible strategy for dose escalation in large secondary brain tumors. This report describes a series of patients treated upfront with two-session radiosurgery for primary tumors affecting the brain. Materials and methods From May 2017 to January 2020, eight patients with primary tumors affecting the brain were treated with two-session radiosurgery due to either an initial large tumor volume or tumor localization and the involvement of OARs. The response was assessed by imaging and clinical evaluations. Results A total of eight patients were treated, nine tumors were treated with two-session radiosurgery, four patients had tumors in the pineal region (50%), and the rest were in the hypothalamic region (25%) or elsewhere. The mean tumor volume for the first SRS session was 15 mL (range 5.2 to 51.6 mL), the mean prescription dose was 13 Gy, and the timespan between both sessions was 30 days (range, 30 to 42 days). During the second session, tumor volume was reduced to 73.6% (range, -20% to 98.7%) of the original dimension, mean tumor volume was 5 mL (range, 0.1 to 17.8 ml), mean prescription dose for the second session was 16.2 Gy estimated by time, dose, and fractionation and by bioequivalent dose under alpha-beta values often to be equivalent to a single dose of 15.8 Gy. Doses to the OARs for the optic pathway were equivalent to a single maximum dose of 9.75 Gy (range, 7.12 to 10.92), and to the brainstem, the equivalent was a maximum dose of 12.3 Gy (range, 5.6 to 15.07). At last follow-up, at a mean of 336.5 days (range, 65 to 962 days), seven patients were alive, five tumors had a partial response (PR), and three had stable disease in accordance to Response Evaluation Criteria in Solid Tumors (RECIST) criteria. One patient died 435 days after treatment, the Karnofsky Performance Status (KPS) was 90 at the first session, 90 at the second session, and was maintained at last follow-up. No adverse radiation effects were reported. Conclusions Two-stage SRS proved to be a safe method to escalate dose in proportionately large volume primary brain tumors whose histology is expected to have a quick biological response to radiation. Longer follow-up is needed to determine the long-term effectiveness by tumor subtypes of two-stage SRS in the same manner as it has been proven in single session SRS series in smaller tumor volumes.

摘要

引言

手术是患有影响大脑的大型、有症状原发性肿瘤患者的一种选择。然而,手术可能并不适用于所有肿瘤,尤其是那些位于松果体区和下丘脑等敏感区域的肿瘤。由于初始肿瘤体积以及辐射敏感危及器官(OARs)的累及,单次立体定向放射外科手术(SRS)可能无法提供足够的剂量以实现长期局部控制。两阶段放射外科手术已被描述为大型继发性脑肿瘤剂量递增的一种可行策略。本报告描述了一系列因原发性脑肿瘤而接受两阶段放射外科手术的患者。

材料与方法

2017年5月至2020年1月,8例患有影响大脑的原发性肿瘤的患者因初始肿瘤体积较大或肿瘤位置以及OARs的累及而接受了两阶段放射外科手术。通过影像学和临床评估来评估反应情况。

结果

共治疗了8例患者,9个肿瘤接受了两阶段放射外科手术,4例患者的肿瘤位于松果体区(50%),其余位于下丘脑区(25%)或其他部位。第一次SRS治疗时的平均肿瘤体积为15毫升(范围5.2至51.6毫升),平均处方剂量为13 Gy,两次治疗之间的时间间隔为30天(范围30至42天)。在第二次治疗时,肿瘤体积缩小至原始尺寸的73.6%(范围 -20%至98.7%),平均肿瘤体积为5毫升(范围0.1至17.8毫升),第二次治疗的平均处方剂量根据时间、剂量和分次以及α-β值下的生物等效剂量估计相当于单次剂量15.8 Gy。视路的OARs剂量相当于单次最大剂量9.75 Gy(范围7.12至10.92),脑干的等效最大剂量为12.3 Gy(范围5.6至15.07)。在最后一次随访时,平均随访时间为336.5天(范围65至962天),7例患者存活,按照实体瘤疗效评价标准(RECIST)标准,5个肿瘤有部分缓解(PR),3个病情稳定。1例患者在治疗后435天死亡,卡氏功能状态评分(KPS)在第一次治疗时为90,第二次治疗时为90,在最后一次随访时保持不变。未报告不良放射效应。

结论

两阶段SRS被证明是一种安全的方法,可在组织学预期对辐射有快速生物学反应的较大体积原发性脑肿瘤中按比例递增剂量。需要更长时间的随访,以与在较小肿瘤体积的单次SRS系列中已得到证实的方式一样,确定两阶段SRS在不同肿瘤亚型中的长期有效性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3a86/7255071/966c77d690aa/cureus-0012-00000007850-i01.jpg

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