Adult-type diffuse glioma

成人型弥漫性神经胶质瘤
  • 文章类型: Journal Article
    化学交换饱和转移(CEST)是一种使用特定的非共振饱和脉冲来使目标物质预饱和的技术。这个过程影响自由水的信号强度,从而间接提供关于预饱和物质的信息。在CEST的临床应用中,酰胺质子转移(APT)是目前最成熟的。APT可用于胶质瘤的术前分级。具有较高APTw信号的肿瘤通常表明较高的恶性肿瘤可能性。在预测术前分子分型时,在具有良好分子表型的肿瘤中,APTw值通常较低,如异柠檬酸脱氢酶(IDH)突变,与IDH野生型肿瘤相比。为了鉴别诊断,脑膜瘤的平均APTw值显著低于高级别胶质瘤.各种APTw测量指标有助于区分具有相似影像学特征的中枢神经系统病变,如进行性多灶性白质脑病,中枢神经系统淋巴瘤,孤立性脑转移瘤,和胶质母细胞瘤.关于预后,APT有效区分肿瘤复发和治疗效果,并且还具有总生存期(OS)和无进展生存期(PFS)的预测能力。
    Chemical Exchange Saturation Transfer (CEST) is a technique that uses specific off-resonance saturation pulses to pre-saturate targeted substances. This process influences the signal intensity of free water, thereby indirectly providing information about the pre-saturated substance. Among the clinical applications of CEST, Amide Proton Transfer (APT) is currently the most well-established. APT can be utilized for the preoperative grading of gliomas. Tumors with higher APTw signals generally indicate a higher likelihood of malignancy. In predicting preoperative molecular typing, APTw values are typically lower in tumors with favorable molecular phenotypes, such as isocitrate dehydrogenase (IDH) mutations, compared to IDH wild-type tumors. For differential diagnosis, the average APTw values of meningiomas are significantly lower than those of high-grade gliomas. Various APTw measurement indices assist in distinguishing central nervous system lesions with similar imaging features, such as progressive multifocal leukoencephalopathy, central nervous system lymphoma, solitary brain metastases, and glioblastoma. Regarding prognosis, APT effectively differentiates between tumor recurrence and treatment effects, and also possesses predictive capabilities for overall survival (OS) and progression-free survival (PFS).
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  • 文章类型: Journal Article
    2021年,世界卫生组织发布了针对中枢神经系统肿瘤的新分类系统。本研究将成人弥漫性胶质瘤(ADG)重新分类为星形细胞瘤,少突胶质细胞瘤,根据新的肿瘤分类和胶质母细胞瘤(GBM)。
    TERT启动子(pTERT)突变的关联,MGMT甲基化,和CD47/TIGIT表达与患者预后的关系进行了研究。
    免疫组化分析表明,肿瘤组织中CD47和TIGIT的表达水平明显高于正常脑组织。GBM和4级星形细胞瘤组织中CD47水平较高。GBM患者的TIGIT表达也较高。CD47、TIGIT、CD47/TIGIT与MGMT未甲基化呈正相关,但与pTERT突变无关。此外,MGMT未甲基化与星形细胞瘤总体生存率低相关。高CD47,TIGIT,CD47/TIGIT水平与ADG和GBM患者生存率显著降低相关。GBM,MGMT非甲基化,CD47高表达是ADG患者总生存期的独立预后因素。
    集体,这些结果表明MGMT的非甲基化和高水平的CD47和TIGIT与ADG的不良预后相关。具有高CD47和TIGIT表达的患者可受益于抗CD47和TIGIT免疫疗法。
    In 2021, the World Health Organization published a new classification system for central nervous system tumors. This study reclassified the adult diffuse glioma (ADG) into astrocytoma, oligodendroglioma, and glioblastoma (GBM) according to the new tumor classification.
    The association of TERT promoter (pTERT) mutation, MGMT methylation, and CD47/TIGIT expression with patient prognosis was investigated.
    Immunohistochemical analysis showed that the expression levels of CD47 and TIGIT in tumor tissues were significantly higher than those in normal brain tissues. CD47 levels were higher in GBM and grade 4 astrocytoma tissues. TIGIT expression was also higher in patients with GBM. The high expressions of CD47, TIGIT, and CD47/TIGIT were positively correlated with MGMT unmethylation but not pTERT mutation. Moreover, MGMT unmethylation was associated with poor overall survival in astrocytoma. High CD47, TIGIT, and CD47/TIGIT levels were associated with significantly reduced survival in ADG and GBM. GBM, MGMT unmethylation, and high CD47 expression were independent prognostic factors for overall survival in ADG.
    Collectively, these results showed that the MGMT unmethylation and high levels of CD47 and TIGIT are associated with a poor prognosis in ADG. Patients with high CD47 and TIGIT expression may benefit from anti-CD47 and TIGIT immunotherapy.
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  • 文章类型: Journal Article
    目的:准确的成人弥漫性神经胶质瘤术前影像学分期对于有效的预后分层和选择适当的治疗干预措施至关重要。这项研究的目的是比较从超高b值扩散加权成像(DWI)生成的表观扩散系数(ADC)图对分子分级的有效性和对成人型弥漫性神经胶质瘤的组织学分级的有效性。并评估这些ADC图与分子和组织学生物标志物之间的相关性。
    方法:本研究回顾性纳入了40例成人型弥漫性神经胶质瘤患者,使用2021年WHO分类标准诊断。术前影像数据,包括多b值DWI和常规磁共振成像,被收集。使用组织学和分子标准对肿瘤进行分级。进行直方图分析以产生每个肿瘤的14个参数。受试者工作特征曲线和曲线下面积(AUC)用于评估肿瘤分级和分子状态分化。通过计算连续变量和分层变量的Pearson和Spearman相关系数来分析组织学生物标志物,分别。
    结果:对于WHO4级(WHO4)成人型弥漫性神经胶质瘤的鉴定,分子分级的强度相关参数优于组织学分级。两种分级系统的AUC随着b值的增加而增加,基于ADC8000的直方图参数显示最佳结果(分子分级,平方根:AUC=0.897;组织学分级,中位数:AUC=0.737)。强度相关参数还可以区分分子WHO4胶质瘤与组织学上较低级别的胶质瘤(基于ADC8000的平方根:AUC=0.919),在分子和组织学WHO4胶质瘤之间观察到基于ADC8000的峰度不同(AUC=0.833)。Ki-67指数与IDH的分子状态预测之间存在显著相关性,CDKN2A,和EGFR也被证明。
    结论:发现从高b值ADC图得出的直方图参数对于区分WHO4成人型弥漫性神经胶质瘤的分子等级比区分组织学等级更有效。
    OBJECTIVE: Accurate preoperative radiological staging of adult-type diffuse glioma is crucial for effective prognostic stratification and selection of appropriate therapeutic interventions. The purpose of this study was to compare the effectiveness of apparent diffusion coefficient (ADC) maps generated from ultrahigh b-value diffusion-weighted imaging (DWI) for molecular grading with that for histological grading of adult-type diffuse glioma, and to evaluate the correlation between these ADC maps and molecular and histological biomarkers.
    METHODS: This study retrospectively enrolled forty adult-type diffuse glioma patients, diagnosed using the 2021 WHO classification criteria. Preoperative imaging data, including multiple b-value DWI and conventional magnetic resonance imaging, were collected. Tumors were graded using both histological and molecular criteria. Histogram analysis was conducted to generate 14 parameters for each tumor. Receiver operating characteristic curves and the area under the curve (AUC) were used to evaluate tumor grading and molecular status differentiation. Analysis of histological biomarkers was performed by calculating the Pearson and Spearman correlation coefficients of continuous and hierarchical variables, respectively.
    RESULTS: The intensity-related parameters for molecular grading were found to be superior to those for histological grading for the identification of WHO grade 4 (WHO4) adult-type diffuse glioma. The AUC of both grading systems increased with increasing b-values, with ADC8000-based histogram parameters showing the best results (molecular grading, square root: AUC = 0.897; histological grading, median: AUC = 0.737). The intensity-related parameters could also differentiate molecular WHO4 gliomas from histologically lower-grade gliomas (ADC8000-based square root: AUC = 0.919), and different ADC8000-based kurtosis was observed between molecular and histological WHO4 gliomas (AUC = 0.833). Significant correlations between the Ki-67 index and molecular status prediction for IDH, CDKN2A, and EGFR were also demonstrated.
    CONCLUSIONS: The histogram parameters derived from high b-value ADC maps were found to be more effective for differentiating molecular grades of WHO4 adult-type diffuse glioma than for differentiating histological grades.
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