Nataniel Mandelberg, Tiffany R Hodges, Tony J C Wang, Tresa McGranahan, Jeffrey J Olson, Daniel A Orringer
{"title":"神经外科医师大会对WHOⅱ级弥漫性神经胶质瘤的系统评价和循证神经病理学指南:更新。","authors":"Nataniel Mandelberg, Tiffany R Hodges, Tony J C Wang, Tresa McGranahan, Jeffrey J Olson, Daniel A Orringer","doi":"10.1007/s11060-024-04898-7","DOIUrl":null,"url":null,"abstract":"<p><p>QUESTIONS AND RECOMMENDATIONS FROM THE PRIOR VERSION OF THESE GUIDELINES WITHOUT CHANGE: TARGET POPULATION: Adult patients (age ≥ 18 years) who have suspected low-grade diffuse glioma.</p><p><strong>Question: </strong>What are the optimal neuropathological techniques to diagnose low-grade diffuse glioma in the adult?</p><p><strong>Recommendation: </strong>Level I Histopathological analysis of a representative surgical sample of the lesion should be used to provide the diagnosis of low-grade diffuse glioma. Level III Both frozen section and cytopathologic/smear evaluation should be used to aid the intra-operative assessment of low-grade diffuse glioma diagnosis. A resection specimen is preferred over a biopsy specimen, to minimize the potential for sampling error issues.</p><p><strong>Target population: </strong>Patients with histologically-proven WHO grade II diffuse glioma.</p><p><strong>Question: </strong>In adult patients (age ≥ 18 years) with histologically-proven WHO grade II diffuse glioma, is testing for IDH1 mutation (R132H and/or others) warranted? If so, is there a preferred method?</p><p><strong>Recommendation: </strong>Level II IDH gene mutation assessment, via IDH1 R132H antibody and/or IDH1/2 mutation hotspot sequencing, is highly-specific for low-grade diffuse glioma, and is recommended as an additional test for classification and prognosis.</p><p><strong>Target population: </strong>Patients with histologically-proven WHO grade II diffuse glioma.</p><p><strong>Question: </strong>In adult patients (age ≥ 18 years) with histologically-proven WHO grade II diffuse glioma, is testing for 1p/19q loss warranted? If so, is there a preferred method?</p><p><strong>Recommendation: </strong>Level III 1p/19q loss-of-heterozygosity testing, by FISH, array-CGH or PCR, is recommended as an additional test in oligodendroglial cases for prognosis and potential treatment planning.</p><p><strong>Target population: </strong>Patients with histologically proven WHO grade II diffuse glioma.</p><p><strong>Question: </strong>In adult patients (age > 18 years) with histologically-proven WHO grade II diffuse glioma, is methyl-guanine methyl-transferase (MGMT) promoter methylation testing warranted? If so, is there a preferred method?</p><p><strong>Recommendation: </strong>There is insufficient evidence to recommend MGMT promoter methylation testing as a routine for low-grade diffuse gliomas. It is recommended that patients be enrolled in properly designed clinical trials to assess the value of this and related markers for this target population.</p><p><strong>Target population: </strong>Patients with histologically-proven WHO grade II diffuse glioma.</p><p><strong>Question: </strong>In adult patients (age ≥ 18 years) with histologically proven WHO grade II diffuse glioma, is Ki-67/MIB1 immunohistochemistry warranted? If so, is there a preferred method to quantitate results?</p><p><strong>Recommendation: </strong>Level III Ki67/MIB1 immunohistochemistry is recommended as an option for prognostic assessment.</p><p><strong>New recommendation: </strong>TARGET POPULATION: Adult patients (age ≥ 18 years) who have suspected WHO grade II diffuse glioma.</p><p><strong>Question: </strong>Is testing for ATRX mutations helpful for predicting survival and making treatment recommendations?</p><p><strong>Recommendation: </strong>There is insufficient evidence to recommend ATRX mutation testing as a means of predicting survival or making treatment recommendations.</p><p><strong>Target population: </strong>Adult patients (age ≥ 18 years) who have suspected WHO grade II diffuse glioma.</p><p><strong>Question: </strong>Does the addition of intraoperative optical histologic methods provide accuracy beyond the use of conventional histologic methods in diagnosis and management?</p><p><strong>Recommendation: </strong>There is insufficient evidence at this time to suggest that intraoperative optical histologic methods offer increased diagnostic accuracy when compared to conventional techniques.</p>","PeriodicalId":16425,"journal":{"name":"Journal of Neuro-Oncology","volume":" ","pages":""},"PeriodicalIF":3.2000,"publicationDate":"2025-01-02","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Congress of Neurological Surgeons systematic review and evidence based guideline on neuropathology for WHO grade II diffuse glioma: update.\",\"authors\":\"Nataniel Mandelberg, Tiffany R Hodges, Tony J C Wang, Tresa McGranahan, Jeffrey J Olson, Daniel A Orringer\",\"doi\":\"10.1007/s11060-024-04898-7\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>QUESTIONS AND RECOMMENDATIONS FROM THE PRIOR VERSION OF THESE GUIDELINES WITHOUT CHANGE: TARGET POPULATION: Adult patients (age ≥ 18 years) who have suspected low-grade diffuse glioma.</p><p><strong>Question: </strong>What are the optimal neuropathological techniques to diagnose low-grade diffuse glioma in the adult?</p><p><strong>Recommendation: </strong>Level I Histopathological analysis of a representative surgical sample of the lesion should be used to provide the diagnosis of low-grade diffuse glioma. 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If so, is there a preferred method?</p><p><strong>Recommendation: </strong>Level II IDH gene mutation assessment, via IDH1 R132H antibody and/or IDH1/2 mutation hotspot sequencing, is highly-specific for low-grade diffuse glioma, and is recommended as an additional test for classification and prognosis.</p><p><strong>Target population: </strong>Patients with histologically-proven WHO grade II diffuse glioma.</p><p><strong>Question: </strong>In adult patients (age ≥ 18 years) with histologically-proven WHO grade II diffuse glioma, is testing for 1p/19q loss warranted? If so, is there a preferred method?</p><p><strong>Recommendation: </strong>Level III 1p/19q loss-of-heterozygosity testing, by FISH, array-CGH or PCR, is recommended as an additional test in oligodendroglial cases for prognosis and potential treatment planning.</p><p><strong>Target population: </strong>Patients with histologically proven WHO grade II diffuse glioma.</p><p><strong>Question: </strong>In adult patients (age > 18 years) with histologically-proven WHO grade II diffuse glioma, is methyl-guanine methyl-transferase (MGMT) promoter methylation testing warranted? If so, is there a preferred method?</p><p><strong>Recommendation: </strong>There is insufficient evidence to recommend MGMT promoter methylation testing as a routine for low-grade diffuse gliomas. 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Congress of Neurological Surgeons systematic review and evidence based guideline on neuropathology for WHO grade II diffuse glioma: update.
QUESTIONS AND RECOMMENDATIONS FROM THE PRIOR VERSION OF THESE GUIDELINES WITHOUT CHANGE: TARGET POPULATION: Adult patients (age ≥ 18 years) who have suspected low-grade diffuse glioma.
Question: What are the optimal neuropathological techniques to diagnose low-grade diffuse glioma in the adult?
Recommendation: Level I Histopathological analysis of a representative surgical sample of the lesion should be used to provide the diagnosis of low-grade diffuse glioma. Level III Both frozen section and cytopathologic/smear evaluation should be used to aid the intra-operative assessment of low-grade diffuse glioma diagnosis. A resection specimen is preferred over a biopsy specimen, to minimize the potential for sampling error issues.
Target population: Patients with histologically-proven WHO grade II diffuse glioma.
Question: In adult patients (age ≥ 18 years) with histologically-proven WHO grade II diffuse glioma, is testing for IDH1 mutation (R132H and/or others) warranted? If so, is there a preferred method?
Recommendation: Level II IDH gene mutation assessment, via IDH1 R132H antibody and/or IDH1/2 mutation hotspot sequencing, is highly-specific for low-grade diffuse glioma, and is recommended as an additional test for classification and prognosis.
Target population: Patients with histologically-proven WHO grade II diffuse glioma.
Question: In adult patients (age ≥ 18 years) with histologically-proven WHO grade II diffuse glioma, is testing for 1p/19q loss warranted? If so, is there a preferred method?
Recommendation: Level III 1p/19q loss-of-heterozygosity testing, by FISH, array-CGH or PCR, is recommended as an additional test in oligodendroglial cases for prognosis and potential treatment planning.
Target population: Patients with histologically proven WHO grade II diffuse glioma.
Question: In adult patients (age > 18 years) with histologically-proven WHO grade II diffuse glioma, is methyl-guanine methyl-transferase (MGMT) promoter methylation testing warranted? If so, is there a preferred method?
Recommendation: There is insufficient evidence to recommend MGMT promoter methylation testing as a routine for low-grade diffuse gliomas. It is recommended that patients be enrolled in properly designed clinical trials to assess the value of this and related markers for this target population.
Target population: Patients with histologically-proven WHO grade II diffuse glioma.
Question: In adult patients (age ≥ 18 years) with histologically proven WHO grade II diffuse glioma, is Ki-67/MIB1 immunohistochemistry warranted? If so, is there a preferred method to quantitate results?
Recommendation: Level III Ki67/MIB1 immunohistochemistry is recommended as an option for prognostic assessment.
New recommendation: TARGET POPULATION: Adult patients (age ≥ 18 years) who have suspected WHO grade II diffuse glioma.
Question: Is testing for ATRX mutations helpful for predicting survival and making treatment recommendations?
Recommendation: There is insufficient evidence to recommend ATRX mutation testing as a means of predicting survival or making treatment recommendations.
Target population: Adult patients (age ≥ 18 years) who have suspected WHO grade II diffuse glioma.
Question: Does the addition of intraoperative optical histologic methods provide accuracy beyond the use of conventional histologic methods in diagnosis and management?
Recommendation: There is insufficient evidence at this time to suggest that intraoperative optical histologic methods offer increased diagnostic accuracy when compared to conventional techniques.
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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