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具有罕见BRAF V600D突变的促纤维增生性婴儿星形细胞瘤/节细胞胶质瘤

Desmoplastic infantile astrocytoma/ganglioglioma with rare BRAF V600D mutation.

作者信息

Greer Ashley, Foreman Nicholas K, Donson Andrew, Davies Kurtis D, Kleinschmidt-DeMasters B K

机构信息

Department of Pathology, The University of Colorado School of Medicine, Aurora, Colorado.

Department of Pediatrics, Children's Hospital Colorado, Aurora, CO.

出版信息

Pediatr Blood Cancer. 2017 Jun;64(6). doi: 10.1002/pbc.26350. Epub 2016 Nov 10.

Abstract

BACKGROUND

Desmoplastic infantile astrocytoma (DIA) and desmoplastic infantile gangliogliomas (DIGs) are rare, massive, cystic and solid tumors of infants usually found in superficial cerebral hemispheres. They manifest prominent desmoplastic stroma, admixed neoplastic astrocytes, primitive-appearing small cells, and additional neoplastic ganglion cells in the case of DIGs. While v-Raf murine sarcoma viral oncogene homolog B (BRAF) mutation is found in up to 50% of pediatric gangliogliomas, two recent studies found that it was rare in DIA/DIGs; we sought to assess BRAF status in DIA/DIGs from our institution.

PROCEDURE

Departmental files from 2000 to 2016 were reviewed to identify cases. Clinical, neuroimaging, histological, and immunohistochemistry (IHC) features were assessed; the latter included IHC for astrocytic and neuronal markers and BRAF VE1. BRAF mutational assessment by Sanger and next-generation sequencing was attempted in all cases.

RESULTS

All six identified cases (four males-two females; three DIA-three DIG) occurred in children <1-year old, were large, cerebral-hemispheric, cystic and solid, and enhancing tumors. Only one case, a DIG with prominent aggregates of neoplastic ganglion cells, showed either BRAF VE1 IHC positivity or mutation by Sanger and next-generation sequencing (rare c. 1799_1800delinsAT; p. V600D). Four of six archival cases were BRAF VE1 IHC negative, but failed mutational sequencing.

CONCLUSION

Five of six classic DIA/DIGs were negative for BRAF mutation; previous series have identified BRAF mutation in two of 18 and one of 14 cases, although all were the more common BRAF V600E. We were unable to find other examples of glial tumors in public databases with this rare BRAF V600D mutation. Identification of BRAF mutational opens the possibility of BRAF-targeted therapies for the subset of DIA/DIG that clinically progress postresection.

摘要

背景

促纤维增生性婴儿星形细胞瘤(DIA)和促纤维增生性婴儿节细胞胶质瘤(DIG)是罕见的、巨大的、囊性和实性肿瘤,通常发生于婴儿大脑浅表半球。它们表现为显著的促纤维增生性基质,混合性肿瘤性星形胶质细胞、外观原始的小细胞,在DIG病例中还存在额外的肿瘤性神经节细胞。虽然高达50%的儿童节细胞胶质瘤中发现有v-Raf鼠肉瘤病毒癌基因同源物B(BRAF)突变,但最近两项研究发现其在DIA/DIG中罕见;我们试图评估本机构DIA/DIG中的BRAF状态。

方法

回顾2000年至2016年的科室档案以确定病例。评估临床、神经影像学、组织学和免疫组化(IHC)特征;后者包括星形细胞和神经元标志物以及BRAF VE1的IHC。所有病例均尝试通过桑格测序和二代测序进行BRAF突变评估。

结果

所有6例确诊病例(4例男性-2例女性;3例DIA-3例DIG)均发生于1岁以下儿童,为大脑半球的、巨大的、囊性和实性的强化肿瘤。仅1例有显著肿瘤性神经节细胞聚集的DIG显示BRAF VE1 IHC阳性或通过桑格测序和二代测序检测到突变(罕见的c.1799_1800delinsAT;p.V600D)。6例存档病例中有4例BRAF VE1 IHC阴性,但突变测序失败。

结论

6例经典DIA/DIG中有5例BRAF突变阴性;既往系列研究在18例中的2例和14例中的1例中发现BRAF突变,尽管均为更常见的BRAF V600E。我们在公共数据库中未能找到其他具有这种罕见BRAF V600D突变的胶质肿瘤实例。BRAF突变的鉴定为术后临床进展的DIA/DIG亚组提供了BRAF靶向治疗的可能性。

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