如何治疗复发性小儿高级别胶质瘤(pHGG):一项全欧范围的调查研究。
How I treat recurrent pediatric high-grade glioma (pHGG): a Europe-wide survey study.
机构信息
Division of Pediatric Hemato-Oncology, Department of Pediatrics and Adolescent Medicine, Medical University of Graz, Auenbruggerplatz 34/2, 8036, Graz, Austria.
Department of Pediatrics, Obstetrics and Gynecology, Division of Pediatric Hematology and Oncology, University Hospital of Geneva, Geneva, Switzerland.
出版信息
J Neurooncol. 2023 Feb;161(3):525-538. doi: 10.1007/s11060-023-04241-6. Epub 2023 Feb 1.
PURPOSE
As there is no standard of care treatment for recurrent/progressing pediatric high-grade gliomas (pHGG), we aimed to gain an overview of different treatment strategies.
METHODS
In a web-based questionnaire, members of the SIOPE-BTG and the GPOH were surveyed on therapeutic options in four case scenarios (children/adolescents with recurrent/progressing HGG).
RESULTS
139 clinicians with experience in pediatric neuro-oncology from 22 European countries participated in the survey. Most respondents preferred further oncological treatment in three out of four cases and chose palliative care in one case with marked symptoms. Depending on the case, 8-92% would initiate a re-resection (preferably hemispheric pHGG), combined with molecular diagnostics. Throughout all case scenarios, 55-77% recommended (re-)irradiation, preferably local radiotherapy > 20 Gy. Most respondents would participate in clinical trials and use targeted therapy (79-99%), depending on molecular genetic findings (BRAF alterations: BRAF/MEK inhibitor, 64-88%; EGFR overexpression: anti-EGFR treatment, 46%; CDKN2A deletion: CDK inhibitor, 18%; SMARCB1 deletion: EZH2 inhibitor, 12%). 31-72% would administer chemotherapy (CCNU, 17%; PCV, 8%; temozolomide, 19%; oral etoposide/trofosfamide, 8%), and 20-69% proposed immunotherapy (checkpoint inhibitors, 30%; tumor vaccines, 16%). Depending on the individual case, respondents would also include bevacizumab (6-18%), HDAC inhibitors (4-15%), tumor-treating fields (1-26%), and intraventricular chemotherapy (4-24%).
CONCLUSION
In each case, experts would combine conventional multimodal treatment concepts, including re-irradiation, with targeted therapy based on molecular genetic findings. International cooperative trials combining a (chemo-)therapy backbone with targeted therapy approaches for defined subgroups may help to gain valid clinical data and improve treatment in pediatric patients with recurrent/progressing HGG.
目的
由于目前尚无复发性/进展性小儿高级别胶质瘤(pHGG)的标准治疗方法,我们旨在全面了解不同的治疗策略。
方法
在一个基于网络的问卷中,SIOPE-BTG 和 GPOH 的成员针对四个病例场景(患有复发性/进展性 HGG 的儿童/青少年)中的治疗选择进行了调查。
结果
来自 22 个欧洲国家的 139 名具有小儿神经肿瘤学经验的临床医生参与了这项调查。在四个病例中的三个中,大多数受访者倾向于进一步进行肿瘤治疗,而在一个有明显症状的病例中则选择姑息治疗。根据病例的不同,8-92%的受访者会进行再次切除(最好是半球 pHGG),并结合分子诊断。在所有病例场景中,55-77%的受访者建议(重新)放疗,最好是局部放疗>20Gy。大多数受访者将根据分子遗传学发现(BRAF 改变:BRAF/MEK 抑制剂,64-88%;EGFR 过表达:抗 EGFR 治疗,46%;CDKN2A 缺失:CDK 抑制剂,18%;SMARCB1 缺失:EZH2 抑制剂,12%)参加临床试验并使用靶向治疗(79-99%)。31-72%的受访者会进行化疗(卡莫司汀,17%;PCV,8%;替莫唑胺,19%;口服依托泊苷/替罗福新,8%),20-69%的受访者会建议免疫治疗(检查点抑制剂,30%;肿瘤疫苗,16%)。根据具体病例,受访者还会包括贝伐单抗(6-18%)、HDAC 抑制剂(4-15%)、肿瘤治疗场(1-26%)和脑室化疗(4-24%)。
结论
在每种情况下,专家们都会将常规的多模式治疗概念与基于分子遗传学发现的靶向治疗相结合。国际合作试验将(化疗)基础与针对特定亚组的靶向治疗方法相结合,可能有助于获得有效的临床数据,并改善复发性/进展性 HGG 患儿的治疗效果。
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