Yi Zhu, Darin D Carabenciov, Derek R Johnson, Jorge A Trejo-Lopez, Aivi T Nguyen, Aditya Raghunathan, Giuseppe Lanzino, Cristiane M Ida, Cinthya J Zepeda-Mendoza, Surendra Dasari, Emilie Russler-Germain, Sonika Dahiya, Martha Quezado, Kenneth Aldape, Caterina Giannini
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Leptomeningeal biopsy was diagnostic in five (of six) cases, revealing infiltration by an astrocytic glioma with mitotic activity, lacking microvascular proliferation or necrosis. One case was diagnosed at autopsy. All tumors were IDH-wildtype, with five harboring TERT promoter mutations. Additional mutations identified were PTEN in one case, TP53 in two cases, and NF1 in two cases. A chromosome profile with +7/-10 was found in four cases, whereas the remaining two showed either chromosome 7 or 7p gain only. Four cases showed chromosome 9p loss with CDKN2A/B homozygous deletion, one case showed hemizygous CDKN2A/B loss, and one case showed intact chromosome 9 and CDK4/GLI1 amplification. DNA methylation profiling was performed in four cases and revealed a match to glioblastoma (GBM) family and mesenchymal typical class with high confidence scores in two cases; the other two cases showed only suggestive combined scores for GBM family and mesenchymal atypical class. The molecular profile of all cases closely aligned with that of adult-type GBM, IDH-wildtype, CNS WHO grade 4. All patients succumbed to the disease. In five cases with extensive leptomeningeal disease at diagnosis, the course was rapid, with median survival of 24 days following palliative care. Only one case, with relatively localized disease at diagnosis, received chemoradiation therapy and survived 535 days, raising the possibility that early diagnosis and timely treatment could improve outcome. 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引用次数: 0
摘要
成人原发性脑轻脑膜胶质瘤病(PLG)是一种罕见的、进展迅速且致命的疾病,其特征是脑轻脑膜被明显的胶质肿瘤浸润而没有可识别的实质肿块。成人PLG的分子特征尚未得到很好的表征。我们报告6例成年PLG患者的临床、病理和分子表现(5男1女),中位年龄58岁。所有病例均表现为病理性脑轻脑膜增强。6例中有5例是轻脑膜活检,显示星形细胞胶质瘤浸润,具有有丝分裂活性,缺乏微血管增生或坏死。1例在尸检时确诊。所有肿瘤均为idh野生型,其中5个携带TERT启动子突变。发现的其他突变有一例为PTEN,两例为TP53,两例为NF1。在4例中发现了+7/-10染色体谱,而其余2例仅显示了7号或7p染色体增益。4例9p染色体缺失伴CDKN2A/B纯合子缺失,1例CDKN2A/B半合子缺失,1例9号染色体完整伴CDK4/GLI1扩增。4例进行了DNA甲基化分析,结果显示与胶质母细胞瘤(GBM)家族和间充质典型类相匹配,其中2例具有高置信度;另外两例仅显示GBM家族和间充质非典型分类的综合评分。所有病例的分子特征与成人型GBM, idh -野生型,CNS WHO 4级密切相关。所有的病人都死于这种疾病。在5例诊断时患有广泛性脑脊膜疾病的病例中,病程迅速,姑息治疗后的中位生存期为24天。只有1例在诊断时疾病相对局限,接受了放化疗并存活了535天,这提高了早期诊断和及时治疗可以改善预后的可能性。补充表中提供了以前报告病例的详细清单。
Molecular profile of adult primary leptomeningeal gliomatosis aligns with glioblastoma, IDH-wildtype.
Adult primary leptomeningeal gliomatosis (PLG) is a rare, rapidly progressive and fatal disease characterized by prominent leptomeningeal infiltration by a glial tumor without an identifiable parenchymal mass. The molecular profile of adult PLG has not been well-characterized. We report the clinical, pathological, and molecular findings of six adult PLG patients (five males and one female), median age 58 years. All cases exhibited pathological leptomeningeal enhancement at presentation. Leptomeningeal biopsy was diagnostic in five (of six) cases, revealing infiltration by an astrocytic glioma with mitotic activity, lacking microvascular proliferation or necrosis. One case was diagnosed at autopsy. All tumors were IDH-wildtype, with five harboring TERT promoter mutations. Additional mutations identified were PTEN in one case, TP53 in two cases, and NF1 in two cases. A chromosome profile with +7/-10 was found in four cases, whereas the remaining two showed either chromosome 7 or 7p gain only. Four cases showed chromosome 9p loss with CDKN2A/B homozygous deletion, one case showed hemizygous CDKN2A/B loss, and one case showed intact chromosome 9 and CDK4/GLI1 amplification. DNA methylation profiling was performed in four cases and revealed a match to glioblastoma (GBM) family and mesenchymal typical class with high confidence scores in two cases; the other two cases showed only suggestive combined scores for GBM family and mesenchymal atypical class. The molecular profile of all cases closely aligned with that of adult-type GBM, IDH-wildtype, CNS WHO grade 4. All patients succumbed to the disease. In five cases with extensive leptomeningeal disease at diagnosis, the course was rapid, with median survival of 24 days following palliative care. Only one case, with relatively localized disease at diagnosis, received chemoradiation therapy and survived 535 days, raising the possibility that early diagnosis and timely treatment could improve outcome. A detailed list of previously reported cases is provided in a supplementary table.
期刊介绍:
Brain Pathology is the journal of choice for biomedical scientists investigating diseases of the nervous system. The official journal of the International Society of Neuropathology, Brain Pathology is a peer-reviewed quarterly publication that includes original research, review articles and symposia focuses on the pathogenesis of neurological disease.
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