Clinical management and survival outcomes of patients withdifferent molecular subtypes of diffuse gliomas in China(2011–2017):a multicenter retrospective study from CGGA

Objective:We aimed to summarize the clinicopathological characteristics and prognostic features of various molecular subtypes of diffuse gliomas(DGs)in the Chinese population.Methods:In total,1,418 patients diagnosed with DG between 2011 and 2017 were classified into 5 molecular subtypes according to the 2016 WHO classification of central nervous system tumors.The IDH mutation status was determined by immunohistochemistry and/or DNA sequencing,and 1p/19q codeletion was detected with fluorescence in situ hybridization.The median clinical follow-up time was 1,076 days.T-tests and chi-square tests were used to compare clinicopathological characteristics.Kaplan‒Meier and Cox regression methods were used to evaluate prognostic factors.Results:Our cohort included 15.5%lower-grade gliomas,IDH-mutant and 1p/19q-codeleted(LGG-IDHm-1p/19q);18.1%lowergrade gliomas,IDH-mutant(LGG-IDHm);13.1%lower-grade gliomas,IDH-wildtype(LGG-IDHwt);36.1%glioblastoma,IDHwildtype(GBM-IDHwt);and 17.2%glioblastoma,IDH-mutant(GBM-IDHm).Approximately 63.3%of the enrolled primary gliomas,and the median overall survival times for LGG-IDHm,LGG-IDHwt,GBM-IDHwt,and GBM-IDHm subtypes were 75.97,34.47,11.57,and 15.17 months,respectively.The 5-year survival rate of LGG-IDHm-1p/19q was 76.54%.We observed a significant association between high resection rate and favorable survival outcomes across all subtypes of primary tumors.We also observed a significant role of chemotherapy in prolonging overall survival for GBM-IDHwt and GBM-IDHm,and in prolonging post-relapse survival for the 2 recurrent GBM subtypes.Conclusions:By controlling for molecular subtypes,we found that resection rate and chemotherapy were 2 prognostic factors associated with survival outcomes in a Chinese cohort with DG.

Genomic profiling of lower-grade gliomas uncovers cohesive disease groups:implications for diagnosis and treatment

Lower-grade gliomas(including low-and intermediate-grade gliomas,World Health Organization grades II and III)are diffusely infiltrative neoplasms that arise most often in the cerebral hemispheres of adults and have traditionally been classified based on their presumed histogenesis as astrocytomas,oligodendrogliomas,or oligoastrocytomas.Although the histopathologic classification of lower-grade glioma has been the accepted standard for nearly a century,it suffers from high intra-and inter-observer variability and does not adequately predict clinical outcomes.Based on integrated analysis of multiplatform genomic data from The Cancer Genome Atlas,lower-grade gliomas have been found to segregate into three cohesive,clinically relevant molecular classes.Molecular classes were closely aligned with the status of isocitrate dehydrogenase(IDH)mutations,tumor protein 53 mutations and the co-deletion of chromosome arms 1 p and 19q,but were not closely aligned with histologic classes.These findings emphasize the potential for improved definition of clinically relevant disease subsets using integrated molecular approaches and highlight the importance of biomarkers for brain tumor classification.

A Phase II Study of Antineoplastons A10 and AS2-1 in Patients with Brainstem Gliomas. The Report on Non-Diffuse Intrinsic Pontine Glioma (Protocol BT-11)

Inoperable brainstem gliomas (BSG) are among the most difficult to treat malignancies. In the intent-to-treat (ITT) population of the BT-11 study for BSG, forty patients (median age 11.2 years old) were enrolled. Antineoplastons A10 and AS2-1 (ANP) were administered intravenously daily. The median daily dose of A10 was 8.70 g/kg/day and AS2-1 was 0.32 g/kg/day. Efficacy analyses were conducted in two subgroups: recurrent pediatric diffuse intrinsic pontine glioma (RPDIPG, N?= 17) and non-diffuse intrinsic pontine glioma (NDIPG, N?= 11). This paper reports the results of the study of the efficacy and safety of ANP in patients with NDIPG. The results in the RPDIPG group were reported before;complete response (CR) was 6%, partial response (PR) 23.5%, and stable disease (SD) 17.6%. One year overall survival (OS) was 29.4%, 2 years 11.8%, and 5, 10, and 15 years 6%. In the NDIPG group, there were 36% CR and 27.5% SD. OS at 1, 5, 10, and 15 years was 82%, 73%, 62%, and 50% correspondingly. There was only one serious adverse event (9%) reported in NDIPG represented by hypokalemia, Grade 4. The results suggest that ANP shows efficacy and an acceptable tolerability profile in patients with RPDIPG and NDIPG.

ERBB1 Is Amplified and Overexpressed in High-grade Diffusely Infiltrative Pediatric Brain Stem Glioma

PURPOSE:This study was conducted to investigate the incidence of ERBB1 amplification and overexpression in samples of diffusely infiltrative (WHO grades Ⅱ-Ⅳ) pediatric brain stem glioma (BSG) and determine the relationship of these abnormalities to expression and mutation of TP53 and tumor grade. Experimental Design: After central pathology review, the incidence of ERBB1 amplification and overexpression was determined in 28 samples (18 surgical biopsy and 10 postmortem specimens) of BSG using quantitative PCR and immunohistochemistry,

Diffusive modelling of glioma evolution: a review

Gliomas, the most aggressive form of brain cancer, are known for their widespread invasion into the tissue near the tumor lesion. Exponential models, which have been widely used in other types of cancers, cannot be used for the simulation of tumor growth, due to the diffusive behavior of glioma. Diffusive models that have been proposed in the last two decades seem to better approximate the expansion of gliomas. This paper covers the history of glioma diffusive modelling, starting from the simplified initial model in 90s and describing how this have been enriched to take into account heterogenous brain tissue, anisotropic migration of glioma cells and adjustable proliferation rates. Especially, adjustable proliferation rates are very important for modelling therapy plans and personalising therapy to different patients.

Exploratory therapy for brainstem gliomas

Brainstem gliomas comprise both slow-growing and highly aggressive tumors,the latter carrying a dismal prognosis of approximately 10 months in children.Given their common locations along the brainstem,they are often not amenable to surgical resection.There are currently a host of exploratory therapies under investigation ranging from immunotherapy,small molecular inhibitors,epigenetic-modifying agents,and radiation protocols to combat these difficult-to-treat tumors.Recent discoveries highlighting the role of H3 histone mutations in diffuse midline glioma oncogenesis have yielded a variety of new targetable antigens and aberrant signaling pathways.Although many of these studies have shown promise in terms of inhibiting tumor growth and disease progression,results to date have been modest in their ability to translate into meaningful clinical benefit.This review will serve as an updated report on the current state of literature concerning pre-clinical and clinical therapies being investigated for brainstem glioma.In addition,this review will serve as a guide for clinicians as we review the evolving nomenclature of brainstem gliomas,commonly presenting symptoms,diagnostic tools,and standard therapies.

磁共振FSE/MDME序列联合DWI预测胶质瘤病理组织学分级及增殖活性的研究

目的:探讨快速自旋回波(FSE)/多延迟饱和多回波(MDME)联合弥散加权成像(diffusion-weighted imaging,DWI)预测胶质瘤病理组织学分级,并进一步分析与增殖活性的关系,旨在为早期识别高级别及高增殖活性人群提供更多有价值信息。方法:回顾性纳入2018年01月至2023年01月于我院行手术治疗并经病理组织学检查证实为胶质瘤患者137例,根据病理组织学分级情况分为高级别组(82例)和低级别组(55例);比较两组基线临床资料及磁共振影像学定量分析指标,FSE/MDME联合DWI磁共振用于胶质瘤病理组织学分级预测临床效能分析。结果:两组基线临床资料比较差异无统计学意义(P>0.05);低级别组T1值和质子密度均显著低于高级别组(P<0.05);低级别组表观弥散系数显著高于高级别组(P<0.05);两组T2值比较差异无统计学意义(P>0.05)。T1值、质子密度及表观弥散系数均可用于胶质瘤病理组织学分级预测,单一指标中表观弥散系数预测AUC显著高于T1值及质子密度,同时三者联合预测效能优于三者单用(P<0.05)。胶质瘤患者表观弥散系数与Ki-67阳性细胞比例呈负相关,而T1值和质子密度与Ki-67阳性细胞比例呈正相关(P<0.05),但T2值则与Ki-67阳性细胞比例无相关性(P>0.05)。结论:FSE/MDME联合DWI磁共振可用于胶质瘤病理组织学分级预测,且T1值、质子密度及表观弥散系数三者联合预测效能最佳;同时上述磁共振定量分析指标与胶质瘤组织细胞增殖活性有关。

多模态MRI影像组学及深度学习在胶质瘤诊疗中的研究进展

弥漫性胶质瘤是最常见的颅脑原发恶性肿瘤,术前精准分级、分子分型预测等对于制订适当的治疗策略和预测生存率具有至关重要的作用。影像组学使用高级特征分析从医学图像中提取数据并构建预测模型,捕捉病变微小的变化,从而提高临床诊断、评估预后和预测治疗反应的准确性。深度学习(deep learning, DL)可以从大量原始数据中自动学习和提取多层特征,而不是手工提取的浅层特征,由于DL已被充分证明能够准确地找到非常深入和抽象的特征,这使其成为医学图像分析领域中广泛研究的课题。随着计算能力的进步,基于DL的人工智能已经彻底改变了各个领域。本研究基于多模态MRI影像组学与DL在胶质瘤术前分级、分子分型、生存预测及治疗评价中的最新研究进行综述,以期为胶质瘤患者提供精准诊疗。

弥漫内生型脑桥胶质瘤放化疗及靶向治疗单中心研究

目的探索弥漫内生型脑桥胶质瘤(DIPG)的有效治疗方法及生存影响因素。方法回顾分析2021年4月至2024年1月首都医科大学附属北京天坛医院采用放射治疗联合替莫唑胺和尼妥珠单抗化疗或放射治疗联合ACT001化疗的14例儿童DIPG患者的临床和影像学信息及生存资料,采用Kaplan⁃Meier生存曲线计算中位无进展生存期和总生存期,多变量Cox比例风险回归分析各项因素对无进展生存期和总生存期的影响。结果共14例患儿的客观缓解率为10/14,中位无进展生存期7.83个月,中位总生存期8.30个月。基线影像学无强化是无进展生存期延长的保护因素(RR=0.052,95%CI:0.006~0.416;P=0.005);男性(RR=0.085,95%CI:0.009~0.764;P=0.028)、年龄较大(RR=0.631,95%CI:0.423~0.942;P=0.024)、无脑神经受累表现(RR=0.116,95%CI:0.017~0.781;P=0.027)和基线影像学无强化(RR=0.046,95%CI:0.005~0.413;P=0.006)是总生存期延长的保护因素。结论女性、诊断时年龄较小、发病时脑神经受累、基线影像学强化是影响DIPG患儿生存的危险因素。

弥漫性胶质瘤瘤周水肿组织BMAL1的表达及其临床意义

目的探讨弥漫性胶质瘤瘤周水肿组织脑和肌肉ARNT样蛋白1(BMAL1)的表达及其临床意义。方法选取2021年6月至2023年1月手术切除的64例弥漫性胶质瘤瘤周水肿组织,免疫组化法检测瘤周水肿组织BMAL1表达;术前进行脑MRI检查,计算水肿指数评估瘤周水肿程度。结果64例均伴有瘤周水肿,其中轻度水肿20例,中度水肿9例,重度水肿35例;瘤周水肿组织BMAL1高表达39例,低表达25例。瘤周水肿组织BMAL1免疫组化染色评分与水肿指数呈明显正相关(r=0.408;95%CI 0.179~0.594;P<0.001)。多因素logistic回归分析显示,BMAL1高表达是弥漫性胶质瘤并发重度瘤周水肿的独立影响因素(OR=5.558;95%CI 1.897~8.467;P<0.001)。结论弥漫性胶质瘤瘤周水肿组织BMAL1表达水平与瘤周水肿程度呈正相关,提示BMAL1可能参与弥漫性胶质瘤瘤周水肿的发生、进展。

DKI及DTI在鉴别诊断低级别胶质瘤与脑炎中的价值

目的评估MR扩散峰度成像(diffusion kurtosis imaging,DKI)及扩散张量成像(diffusion-tensor imaging,DTI)在鉴别低级别胶质瘤与脑炎中的价值。材料与方法回顾性分析58例低级别胶质瘤或脑炎患者的影像学资料,所有患者在术前或保守治疗前均行MRI常规序列及DKI序列扫描。用NeuDiLab软件处理DKI图像,获得基于DKI模型的平均峰度(mean kurtosis,MK)、轴向扩散峰度(axial kurtosis,AK)和径向扩散峰度(radial kurtosis,RK)以及基于DTI模型的平均扩散系数(mean diffusivity,MD)、轴向扩散系数(axial diffusivity,AD)、径向扩散系数(radial diffusivity,RD)和各向异性分数(fractional anisotropy,FA)参数图及b=0 s/mm2的扩散图像(B0)。用ITK-SNAP软件在B0图像上手动勾画肿瘤的感兴趣容积(volume of interest,VOI),将其配准到其他参数图上。用FAE软件提取各参数图的平均值。根据病理检查或脑脊液检查结果将患者分为胶质瘤组和脑炎组。采用卡方检验、独立样本t检验及Mann-Whitney U检验比较两组患者的一般资料、常规MRI表现及扩散参数的差异。计算Cohen’s d值评估各扩散参数的效应量。绘制受试者工作特征(receiver operating characteristic,ROC)曲线,计算曲线下面积(area under the curve,AUC)、敏感度、特异度和准确度,并用De Long检验比较各参数的鉴别诊断效能。结果共51例患者被纳入研究,包括29例低级别胶质瘤患者、22例脑炎病变患者。RK鉴别诊断脑炎组低级别胶质瘤的表现最好,AUC为0.878,当阈值取0.662时,其敏感度为72.7%,特异度为89.7%。De Long检验显示DKI模型的诊断表现显著优于DTI模型。结论DKI序列有助于鉴别诊断低级别胶质瘤与脑炎。

儿童弥漫性中线胶质瘤伴H3K27变异型102例临床病理特征

目的 探讨儿童弥漫性中线胶质瘤(diffuse midline gliomas, DMG)伴H3K27变异型的临床病理特点和分子学特征。方法 收集102例DMG伴H3K27变异型患者临床资料,采用HE、免疫组化EnVision两步法染色,应用Sanger测序法行分子检测,分析其临床病理特征并复习相关文献。结果 患者发病年龄1~14岁,中位年龄7岁。发病部位:脑干83例(81.4%),非脑干如丘脑、基底节和松果体等19例(18.6%)。临床表现主要为头晕、头痛和步态不稳等。MRI示T1低信号或等信号,T2高信号。组织学示高级别64例(62.7%),低级别38例(37.3%)。免疫表型:H3K27me3表达降低或缺失(100%,81/81),表达H3K27M(98%,100/102)、EZHIP(2%,2/102)、BRAF V600E(2.2%,2/89);p53突变型占53.6%(52/97);ATRX失表达(19.1%,18/94);IDH1不表达(100%,89/89)。分子检测示BRAF突变占1.7%(1/59);EGFR突变占9.1%(1/11)。结论 儿童DMG伴H3K27变异型好发于脑干,组织学以高级别为主,H3K27me3染色呈不同程度表达缺失,分子变异包括H3K27M突变、EZHIP过表达和EGFR突变。

多模态MRI功能成像在脑胶质瘤术后复发与治疗后反应评估中的价值

目的比较MR扩散加权成像(DWI)、三维动脉自旋标记成像(3D ASL)在鉴别脑胶质瘤术后复发与治疗后反应的诊断价值,为临床精准治疗提供客观依据。方法回顾分析我院2019年1月-2023年7月间行脑胶质瘤手术,术后放化疗1月以上,随访过程中首次出现异常强化病灶者47例,进行MRI平扫、DWI、3D ASL、增强扫描检查,分别测量DWI的表观扩散系数(ADC)值和相对ADC(rADC)值、3D ASL的血流动力学参数CBF值和相对CBF(rCBF)值。利用两样本t检验、受试者工作特征曲线(ROC)分析来评估研究参数在鉴别治疗后反应方面的诊断与胶质瘤术后复发效能。结果47例患者中,30例为脑胶质瘤复发,17例为治疗后反应,1.脑胶质瘤复发强化区CBF值为(119.16±18.58)mL/100g/1min,治疗后反应区的CBF值为(72.06±22.77)mL/100g/1min,差异有统计学意义(P<0.05);脑胶质瘤复发强化区rCBF值为3.56±1.13,放射损伤区的rCBF值为1.18±0.39,差异有统计学意义(P<0.05);2.ADC在脑胶质瘤复发和治疗后反应之间没有明显差异(P=0.235);rADC(P<0.05)在脑胶质瘤复发和治疗后反应之间差异有统计学意义;3.3D ASL(rCBF)诊断脑胶质瘤复发曲线下面积约0.971,ADC诊断脑胶质瘤复发曲线下面积约为0.675。结论与DWI序列相比,3D ASL成像技术在鉴别胶质瘤复发和治疗后反应方面显示出更好的诊断效能。

MRI用于胶质瘤神经重塑的研究进展

胶质瘤是成人最常见的恶性脑肿瘤,复发率高且预后极差。神经重塑是大脑在胶质瘤生长中发生的复杂而精密的适应性反应,深入理解大脑的神经重塑对于改善胶质瘤病人生活质量,延长病人生存期具有重要意义。利用高分辨三维T1加权成像(3D T1WI)、扩散张量成像(DTI)及血氧水平依赖功能MRI(BOLD-fMRI)等技术,同时结合先进的影像分析方法可以探索胶质瘤病人结构和功能方面的可塑性及其相关机制。就不同MRI技术对胶质瘤病人结构和功能重塑的研究进行综述,并展望未来的研究方向。

基于DWI的分形维数评价3D打印技术对胶质瘤术后临床疗效的价值

目的使用基于弥散加权成像(diffusion weighted imaging,DWI)的分形维数(fractal dimension,FD)评价个性化3D打印技术是否可以提高手术治疗胶质瘤患者的临床疗效。材料与方法回顾性分析2018年1月至2023年1月我院经病理证实的136例胶质瘤患者病例,其中32例为试验组,术前使用了个性化3D打印技术;其余患者为对照组,进行常规开颅手术。在术后一周DWI图上手动勾画术区周围边界,绘制二值图后测量FD。使用FD中位数对对照组进行分组,比较对照组中高FD和低FD患者的手术情况、疼痛程度、神经缺损程度、预后、日常生活能力是否存在差异;探究个性化3D打印技术是否会影响水肿创面的FD,以及是否会进一步提高患者临床疗效。结果高FD组的疼痛程度(t=−13.228,P<0.001)、神经缺损程度(t=−2.627,P=0.008)高于低FD组,日常生活能力(t=4.821,P<0.001)及预后(t=−3.058,P=0.003)较低FD组差。受试者工作特征(receiver operating characteristic,ROC)曲线结果显示FD能对患者上述四项评分的高低进行有效区分,术前使用个性化3D打印技术可使得患者水肿带FD下降,减轻神经缺损程度并提高日常生活能力,但对改善预后及术区疼痛效果不明显。结论个性化3D打印技术可以有效降低患者术区创面水肿带的FD,减轻神经损伤,值得临床应用。

胶质瘤侵犯中央前回对大脑半球激活斑的影响:一项任务态磁共振研究

【目的】探讨在术前任务态功能磁共振(T-fMRI)中,胶质瘤侵犯中央前回对双侧大脑半球激活斑的影响。【方法】将56例接受了术前任务态磁共振扫描的胶质瘤患者分为中央前回侵犯组(PGI,n=21)和中央前回无侵犯组(PGNI,n=35)。我们设定了三个不同的体素水平上的统计阈值(P值:P1,10^(-4);P2,10^(-6);P3,10^(-8)),并获得相应统计水平的大脑激活图(V1,V2和V3)。分别计算双侧大脑半球间(瘤侧/对侧:IAVR)和双侧中央前回间的激活斑体积比值(瘤侧/对侧:PAVR)。计算位于不同统计阈值区间的激活斑体积(△V1=V1-V2;△V2=V2-V3),并进一步比较它们在双侧大脑半球间的比值[△Vn(瘤侧)/△Vn'(对侧),n=1,2]。此外,我们还分析了肿瘤特征与IAVR和PAVR间的关系。【结果】在相对较低的统计阈值水平中(P1和P2),相较于PGNI组,PGI组的IAVR和PAVR明显减低(P<0.05),但在较严格的统计阈值中(P3),这两组间则无明显差异。相比PGNI组,PGI组的△V1/△V1’明显减低(P=0.02),但△V2/△V2’在两组间没有差异。此外,在PGI组,PAVR与肿瘤大小呈负相关(P=0.043),并且肿瘤距手节区的距离与IAVR和PAVR呈正相关(P<0.05)。【结论】相比胶质瘤未侵犯功能区,在T-fMRI中,侵犯功能区会更容易影响肿瘤同侧脑半球中较低统计阈值的激活斑,造成双侧大脑半球间激活斑不对称性,但这种影响在更严格的统计阈值中没有出现。选取多个统计阈值来分析胶质瘤术前T-fMRI的激活斑结果是十分必要的。

成人弥漫性内生型脑桥胶质瘤伴椎管内播散一例并文献复习

本研究遵守《赫尔辛基宣言》,经兰州大学第二医院伦理委员会审核批准,免除受试者知情同意,批准文号:2023A-782。患者男,25岁,因“持续性头晕3个月”于2020年8月24日收入兰州大学第二医院神经内科,患者自述3个月前无明显诱因出现持续性头部昏沉感,自觉头重脚轻,走路脚踩棉花感,站立步态不稳,间歇性视物水平重影,每次持续数秒,上述症状于3个月内逐渐加重。专科检查:双眼水平眼震,右视时为著.

磁共振灌注加权成像联合扩散加权成像鉴别脑胶质瘤分级的效能分析

【目的】探讨磁共振灌注加权成像(PWI)联合扩散加权成像(DWI)鉴别脑胶质瘤分级的效能。【方法】回顾性分析2021年10月至2022年10月两院收治的经手术病理确诊的脑胶质瘤患者70例(低级别脑胶质瘤40例,高级别脑胶质瘤30例),比较肿瘤实质区、瘤周水肿区与对侧相应正常脑实质的局部脑血流量(rCBF)和表观扩散系数(ADC),比较不同级别脑胶质瘤患者肿瘤实质区和瘤周水肿区相对rCBF(rrCBF)和相对ADC(rADC)。绘制受试者工作特征(ROC)曲线评价rrCBF、rADC单独及联合鉴别脑胶质瘤分级的效能。【结果】肿瘤实质区rCBF高于瘤周水肿区和正常脑实质(P<0.05),ADC低于瘤周水肿区和正常脑实质(P<0.05);瘤周水肿区rCBF高于正常脑实质(P<0.05),ADC低于正常脑实质(P<0.05)。低级别脑胶质瘤患者肿瘤实质区rrCBF低于高级别脑胶质瘤患者(P<0.05),rADC高于高级别脑胶质瘤患者(P<0.05)。低级别脑胶质瘤患者瘤周水肿区rrCBF低于高级别脑胶质瘤患者(P<0.05),rADC与高级别脑胶质瘤患者比较,差异无统计学意义(P>0.05)。ROC曲线分析结果显示:rrCBF、rADC对脑胶质瘤分级均有一定鉴别效能,曲线下面积分别为0.898、0.870,敏感度分别为0.867、0.900,特异度分别为0.800、0.775;两项联合鉴别脑胶质瘤分级的曲线下面积为0.954,敏感度为0.933,特异度为0.975。【结论】PWI、DWI对脑胶质瘤分级均有一定鉴别效能,两者联合鉴别效能更高,值得临床积极推广。

APT-联合DCE-MRI术前预测成人型弥漫性胶质瘤病理分级及IDH基因突变型

目的:探讨氨基质子转移(APT)成像联合DCE-MRI对成人型弥漫性胶质瘤病理分级和IDH基因型的术前预测价值。方法:将2020年10月-2023年10月在本院诊治且经病理证实的78例脑胶质瘤患者纳入本研究。患者手术前均进行APT成像和DCE-MRI检查。依据肿瘤的组织病理学分级将患者分为2组:低级别组(Ⅱ~Ⅲ级)36例,高级别组(Ⅳ级)42例;依据患者IDH基因表达情况将患者分为2组:IDH野生型组31例,IDH突变型组47例。比较高、低病理分级组及不同IDH分型组之间病灶的APT图像信号等级(分为1~5级)和DCE-MRI参数(K_(trans)、V_(e)、rCBV、V_(p)、K_(ep)和rCBF)值的差异,对组间差异有统计学意义的指标,采用ROC曲线分析其诊断效能。结果:IDH突变型和野生型组之间年龄、性别、主诉、神经系统体征差异均无统计学意义(P>0.05);高级别组和低级别组之间年龄、性别、主诉、神经系统体征差异均无统计学意义(P>0.05),但是高级别组中IDH野生型占比更高(P<0.05)。78例病灶的APT信号分级:1级有19例,2级3例,3级14例,4级6例,5级36例。高级别组APT图像上肿瘤的信号等级高于低级别组,IDH野生型组患者APT图像等级高于突变型组,差异有统计学意义(P<0.05)。DCE-MRI参数的组间比较结果显示,高级别组与低级别组之间,以及IDH突变型与IDH野生型之间,K_(trans)、V_(e)和rCBV值的差异均有统计学意义(P<0.05)。APT信号等级鉴别高、低级别胶质瘤及IDH状态的AUC分别为0.782和0.714,K_(trans)、V_(e)和rCBV鉴别高、低级别胶质瘤的AUC分别为0.982、0.793和0.898,鉴别IDH状态的AUC分别为0.963、0.803和0.873。结论:APT成像联合DCE-MRI定量参数能在术前较准确地预测成人型弥漫性胶质瘤的病理分级和IDH基因分型。

儿童弥散内生型脑干胶质瘤的研究进展

儿童弥散内生型脑干胶质瘤(DIPG)的发病机制是肿瘤基因H3.3K27M起始突变和肿瘤微环境改变导致的共同结果,最新研究发现磷酸肌醇3-激酶/蛋白激酶B(PI3K/Akt)、血小板衍生生长因子受体(PDGFRA)扩增等机制也参与肿瘤调控,从而对DIPG的病理特征、基因突变、靶向治疗、免疫治疗等有了新的认识,该文就DIPG的最新研究进展作综述。