神经外科医师大会关于化疗在新诊断的 WHO II 级成人弥漫性胶质瘤中的作用的系统回顾和循证指南:更新版。

IF 3.2 2区 医学 Q2 CLINICAL NEUROLOGY
Mateo Ziu, Lia M Halasz, Priya U Kumthekar, Tresa M McGranahan, Simon S Lo, Jeffrey J Olson
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引用次数: 0

摘要

目标人群新诊断为世界卫生组织(WHO)II级胶质瘤(少突胶质细胞瘤、星形细胞瘤、混合型少突胶质细胞瘤)的成人患者(18岁以上)。问题化疗是否可作为新诊断为低级别胶质瘤患者的首选辅助治疗?建议III级:推荐化疗作为一种治疗选择,以推迟放疗的使用,减缓肿瘤生长,改善新诊断低级别胶质瘤成人患者的无进展生存期(PFS)、总生存期(OS)和临床症状。问题哪些新诊断低级别胶质瘤患者从化疗中获益最多? 建议III级:推荐化疗作为一种可选的组成部分,单独使用或与放疗联合使用,作为所有无法接受新诊断低级别胶质瘤大体全切除术(GTR)患者的初始辅助治疗。术后 MRI 检查残留肿瘤大于 1 cm、肿瘤直径大于 4 cm 或年龄大于 40 岁的患者也应考虑接受辅助治疗。此外,建议将替莫唑胺(TMZ)作为一种治疗选择,以减缓携带1p/19q共缺失的患者的肿瘤生长。问题一旦确诊为LGG,应在多长时间内开始化疗?建议目前还没有足够的证据对手术/病理诊断为LGG后开始化疗的时间做出明确的建议。不过,建议将12周作为开始辅助化疗的最晚时限。建议将患者纳入设计合理的临床试验,以评估该目标人群确诊后开始化疗的时机。问题新确诊的 LGG 应使用何种化疗药物?建议招募受试者参加设计合理的试验,比较这些药物或其他药物的疗效,以确定哪种方案更优。问题作为LGG的初始治疗,化疗的最佳持续时间和剂量是多少?建议将受试者纳入设计合理的临床研究,以评估该疗法的最佳疗程。问题作为LGG的初始疗法,化疗应单独使用还是与RT联合使用? 建议目前尚无足够证据就此提出建议。问题新确诊的LGG患者在接受其他类型的辅助治疗的同时,是否还应该接受化疗?建议II级:建议对LGG病情不乐观的患者在接受RT治疗的同时进行化疗,以改善患者的无进展生存期。本指南上一版本的更新问题和建议问题经病理证实为WHO II级弥漫性胶质瘤的成年患者,与单纯放疗相比,单纯化疗、联合放疗或放疗后化疗是否能获得更好的总生存期、无进展生存期、局部控制、更少的并发症、神经认知保护和生活质量?建议Ⅰ级:建议对所有新确诊的高危WHOⅡ级弥漫性胶质瘤患者(小于40岁无法进行全切和大于40岁无论切除程度如何的患者)在放疗(RT)的基础上加用化疗(PCV),以提高总生存率:建议所有新确诊的高危WHO II级弥漫性胶质瘤患者在放疗的基础上加用化疗(替莫唑胺),以改善无进展生存期和总生存期:新问题与建议目标人群本建议适用于诊断为WHO II级弥漫性胶质瘤的成年患者。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Congress of Neurological Surgeons systematic review and evidence-based guidelines for the role of chemotherapy in newly diagnosed WHO Grade II diffuse glioma in adults: update.

Questions and recommendations from the prior version of these guidelines without changeTarget populationAdult patients (older than 18 years of age) with newly diagnosed World Health Organization (WHO) Grade II gliomas (Oligodendroglioma, astrocytoma, mixed oligoastrocytoma).QuestionIs there a role for chemotherapy as adjuvant therapy of choice in treatment of patients with newly diagnosed low-grade gliomas?RecommendationLevel III: Chemotherapy is recommended as a treatment option to postpone the use of radiotherapy, to slow tumor growth and to improve progression free survival (PFS), overall survival (OS) and clinical symptoms in adult patients with newly diagnosed LGG.QuestionWho are the patients with newly diagnosed LGG that would benefit the most from chemotherapy?RecommendationLevel III: Chemotherapy is recommended as an optional component alone or in combination with radiation as the initial adjuvant therapy for all patients who cannot undergo gross total resection (GTR) of a newly diagnosed LGG. Patients with residual tumor >1 cm on post-operative MRI, presenting diameter of 4 cm or older than 40 years of age should be considered for adjuvant therapy as well.QuestionAre there tumor markers that can predict which patients can benefit the most from initial treatment with chemotherapy?RecommendationLevel III: The addition of chemotherapy to standard RT is recommended in LGG patients that carry IDH mutation. In addition, temozolomide (TMZ) is recommended as a treatment option to slow tumor growth in patients who harbor the 1p/19q co-deletion.QuestionHow soon should the chemotherapy be started once the diagnosis of LGG is confirmed?RecommendationThere is insufficient evidence to make a definitive recommendation on the timing of starting chemotherapy after surgical/pathological diagnosis of LGG has been made. However, using the 12 weeks mark as the latest timeframe to start adjuvant chemotherapy is suggested. It is recommended that patients be enrolled in properly designed clinical trials to assess the timing of chemotherapy initiation once diagnosis is confirmed for this target population.QuestionWhat chemotherapeutic agents should be used for treatment of newly diagnosed LGG?RecommendationThere is insufficient evidence to make a recommendation of one particular regimen. Enrollment of subjects in properly designed trials comparing the efficacy of these or other agents is recommended so as to determine which of these regimens is superior.QuestionWhat is the optimal duration and dosing of chemotherapy as initial treatment for LGG?RecommendationInsufficient evidence exists regarding the duration of any specific cytotoxic drug regimen for treatment of newly diagnosed LGG. Enrollment of subjects in properly designed clinical investigations assessing the optimal duration of this therapy is recommended.QuestionShould chemotherapy be given alone or in conjunction with RT as initial therapy for LGG?RecommendationInsufficient evidence exists to make recommendations in this regard. Hence, enrollment of patients in properly designed clinical trials assessing the difference between chemotherapy alone, RT alone or a combination of them is recommended.QuestionShould chemotherapy be given in addition to other type of adjuvant therapy to patients with newly diagnosed LGG?RecommendationLevel II: It is recommended that chemotherapy be added to the RT in patients with unfavorable LGG to improve their progression free survival.Updated Question and Recommendations from the Prior Version of These GuidelinesQuestionIn adult patients with pathologically confirmed WHO Grade II diffuse glioma does chemotherapy alone, combined with radiation therapy or after radiation therapy compared to radiotherapy alone result in better overall survival, progression free survival, local control, fewer complications, neurocognitive preservation, and quality of life?RecommendationLevel I: It is recommended that chemotherapy (PCV) be added to radiation therapy (RT) in all patients with newly diagnosed high-risk WHO Grade II diffuse glioma (Patients younger than 40 unable to get gross total resection and older than 40 regardless of the degree of resection) to improve their overall survival.

Level ii: It is recommended that chemotherapy be added to radiation therapy in all patients with newly diagnosed high-risk WHO Grade II diffuse glioma to improve overall survival without a decline in neurocognitive function.

Level iii: It is suggested that chemotherapy (temozolomide) be added to RT in all patients with newly diagnosed high-risk WHO Grade II diffuse glioma to improve progression free survival and overall survival.

Level iii: It is suggested that chemotherapy alone should be considered in patients with newly diagnosed WHO Grade II diffuse glioma in cases with 1p/19q co-deletion.New questions and recommendationsTarget populationThese recommendations apply to adult patients diagnosed with WHO Grade II diffuse glioma.QuestionIn adult patients with newly diagnosed WHO grade II diffuse glioma does administration of chemotherapy prior to surgical resection improve extent of resection, provide longer progression free survival and overall survival when compared to chemotherapy alone?RecommendationLevel III: Neo-adjuvant temozolomide may be used in patients with WHO Grade II diffuse gliomas deemed unsafe for resection due to infiltration of eloquent areas or with large contralateral extension as an initial step to improve the extent of resection.There is insufficient evidence to support a recommendation regarding the ability of chemotherapy provided prior to surgical resection to improve progression free survival (PFS) and overall survival (OS).QuestionIn adult patients with newly diagnosed WHO grade II diffuse glioma does the administration of temozolomide increase the rate of malignant transformation when compared to no chemotherapy or other chemotherapy regimens?RecommendationThere is insufficient evidence to support a recommendation against the use of temozolomide for WHO Grade II diffuse gliomas due to concern over increasing the rate of malignant transformation.QuestionIn adult patients with newly diagnosed WHO grade II diffuse glioma does administration of multi-agent chemotherapy improve progression free survival and overall survival when compared to administration of single-agent chemotherapy?RecommendationThere is insufficient evidence to support a recommendation for or against the use of multi-agent chemotherapy to improve progression free survival and overall survival when compared to administration of single-agent chemotherapy in patients with newly diagnosed WHO Grade II diffuse glioma.

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来源期刊
Journal of Neuro-Oncology
Journal of Neuro-Oncology 医学-临床神经学
CiteScore
6.60
自引率
7.70%
发文量
277
审稿时长
3.3 months
期刊介绍: The Journal of Neuro-Oncology is a multi-disciplinary journal encompassing basic, applied, and clinical investigations in all research areas as they relate to cancer and the central nervous system. It provides a single forum for communication among neurologists, neurosurgeons, radiotherapists, medical oncologists, neuropathologists, neurodiagnosticians, and laboratory-based oncologists conducting relevant research. The Journal of Neuro-Oncology does not seek to isolate the field, but rather to focus the efforts of many disciplines in one publication through a format which pulls together these diverse interests. More than any other field of oncology, cancer of the central nervous system requires multi-disciplinary approaches. To alleviate having to scan dozens of journals of cell biology, pathology, laboratory and clinical endeavours, JNO is a periodical in which current, high-quality, relevant research in all aspects of neuro-oncology may be found.
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