Intraoperative rapid molecular diagnosis aids glioma subtyping and guides precise surgical resection

Author:

Li Jia123,Han Zhe123,Ma Caizhi123,Chi Huizhong123,Jia Deze1,Zhang Kailiang1,Feng Zichao1,Han Bo45,Qi Mei45,Li Gang123ORCID,Li Xueen1,Xue Hao123

Affiliation:

1. Department of Neurosurgery, Qilu Hospital, Cheeloo College of Medicine Shandong University Jinan Shandong China

2. Institute of Brain and Brain‐Inspired Science Shandong University Jinan Shandong China

3. Shandong Key Laboratory of Brain Function Remodeling Jinan Shandong China

4. Department of Pathology Shandong University Qilu Hospital Jinan Shandong China

5. Department of Pathology Shandong University School of Basic Medical Sciences Jinan Shandong China

Abstract

AbstractObjectiveThe molecular era of glioma diagnosis and treatment has arrived, and a single rapid histopathology is no longer sufficient for surgery. This study sought to present an automatic integrated gene detection system (AIGS), which enables rapid intraoperative detection of IDH/TERTp mutations.MethodsA total of 78 patients with gliomas were included in this study. IDH/TERTp mutations were detected intraoperatively using AIGS in 41 of these patients, and they were guided to surgical resection (AIGS detection group). The remaining 37 underwent histopathology‐guided conventional surgical resection (non‐AIGS detection group). The clinical utility of this technique was evaluated by comparing the accuracy of glioma subtype diagnosis before and after TERTp mutation results were obtained by pathologists and the extent of resection (EOR) and patient prognosis for molecular pathology‐guided glioma surgery.ResultsWith NGS/Sanger sequencing and chromosome detection as the gold standard, the accuracy of AIGS results was 100%. And the timing was well matched to the intraoperative rapid pathology report. After obtaining the TERTp mutation detection results, the accuracy of the glioma subtype diagnosis made by the pathologists increased by 19.51%. Molecular pathology‐guided surgical resection of gliomas significantly increased EOR (99.06% vs. 93.73%, p < 0.0001) and also improved median OS (26.77 vs. 13.47 months, p = 0.0289) and median PFS (15.90 vs. 10.57 months, p = 0.0181) in patients with glioblastoma.InterpretationUsing AIGS intraoperatively to detect IDH/TERTp mutations to accurately diagnose glioma subtypes can help achieve maximum safe resection of gliomas, which in turn improves the survival prognosis of patients.

Publisher

Wiley

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