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B7-H3,一个潜在的治疗靶点,在弥漫性内在脑桥神经胶质瘤中表达。

B7-H3, a potential therapeutic target, is expressed in diffuse intrinsic pontine glioma.

机构信息

Department of Neurological Surgery, Weill Medical College of Cornell University, 1300 York Ave, Box 99, New York, NY 10065, USA.

出版信息

J Neurooncol. 2013 Feb;111(3):257-64. doi: 10.1007/s11060-012-1021-2. Epub 2012 Dec 12.

Abstract

Diffuse intrinsic pontine glioma (DIPG) is a brain cancer with a median survival of only 1 year. Lack of molecular characterization of this tumor impedes the development of novel therapies. Membrane protein B7-H3, aka CD276, involved in interactions with host defenses in certain cancers, has been shown to be over-expressed in the majority of malignant neuroectodermal tumors including adult high-grade glioma. Targeting B7-H3 with a monoclonal antibody has demonstrated safety and efficacy in the salvage treatment of stage IV childhood neuroblastoma, another neuroectodermal tumor. It thus stands to reason that B7-H3 might serve as a therapeutic target in DIPG. B7-H3 immunoreactivity was determined in DIPG and non-diffuse brainstem glioma specimens with immunohistochemistry. In addition, B7-H3 mRNA expression was evaluated with microarrays in another set of specimens. All of the nine (100 %) DIPG specimens were shown to be B7-H3 immunoreactive. In the non-diffuse brainstem glioma group, none of the eight WHO grade I specimens showed B7-H3 immunoreactivity and nine of the 24 WHO grade II specimens (37.5 %) showed B7-H3 immunoreactivity. The association between histological grade and B7-H3 immunoreactivity was statistically highly significant. B7-H3 mRNA expression was also significantly higher in DIPG samples than in normal brain and juvenile pilocytic astrocytoma (WHO grade I) specimens. In summary, B7-H3 is over-expressed in DIPG. Given the need for novel treatment in this disease, antibody-based immunotherapy against B7-H3 in DIPG warrants further investigation.

摘要

弥漫性内在脑桥神经胶质瘤(DIPG)是一种脑癌,中位生存期仅为 1 年。由于这种肿瘤缺乏分子特征,阻碍了新疗法的开发。膜蛋白 B7-H3(也称为 CD276)参与某些癌症中宿主防御的相互作用,已被证明在大多数恶性神经外胚层肿瘤中过度表达,包括成人高级别胶质瘤。用单克隆抗体靶向 B7-H3 已被证明在挽救性治疗 IV 期儿童神经母细胞瘤(另一种神经外胚层肿瘤)中是安全有效的。因此,B7-H3 可能是 DIPG 的治疗靶点。通过免疫组织化学法确定 DIPG 和非弥漫性脑桥胶质瘤标本中的 B7-H3 免疫反应性。此外,还通过微阵列评估了另一组标本中的 B7-H3 mRNA 表达。所有 9 例(100%)DIPG 标本均显示 B7-H3 免疫反应性。在非弥漫性脑桥胶质瘤组中,8 例 WHO 1 级标本中无一例显示 B7-H3 免疫反应性,24 例 WHO 2 级标本中有 9 例(37.5%)显示 B7-H3 免疫反应性。组织学分级与 B7-H3 免疫反应性之间存在显著关联。与正常脑组织和青少年毛细胞星形细胞瘤(WHO 1 级)标本相比,DIPG 样本中的 B7-H3 mRNA 表达也明显更高。总之,B7-H3 在 DIPG 中过度表达。鉴于该疾病需要新的治疗方法,针对 DIPG 中 B7-H3 的抗体免疫疗法值得进一步研究。

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