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首页> 外文期刊>Journal of neuro-oncology. >Increased expression of tumor-associated antigens in pediatric and adult ependymomas: implication for vaccine therapy.
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Increased expression of tumor-associated antigens in pediatric and adult ependymomas: implication for vaccine therapy.

机译:儿科和成人室管膜瘤中肿瘤相关抗原的表达增加:对疫苗治疗的意义。

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Despite surgery and radiotherapy, as many as 50 % of children with ependymomas will suffer from tumor recurrences that will ultimately lead to death. Our group's initial peptide-based glioma vaccine targeting EphA2, IL-13Rα2, and Survivin, which are overexpressed in pediatric gliomas, has shown promise in its initial phase of testing. We therefore investigated whether EphA2, IL-13Rα2, Survivin, and, additionally, Wilms' Tumor 1 (WT1), are overexpressed in pediatric ependymomas to determine if a similar immunotherapy approach could be applicable. Immunohistochemistry was performed using antibodies specific for EphA2, IL-13Rα2, Survivin, and WT1 on paraffin-embedded specimens from 19 pediatric and 13 adult ependymomas. Normal brain and ependyma were used for background staining controls. Negative staining was defined as no staining or staining equaling the background intensity in normal brain tissues. In the 19 pediatric cases, 18 (95 %) demonstrated positive staining for EphA2, 16 (84 %) for IL-13Rα2, 18 (95 %) for Survivin, and only 7 (37 %) for WT1. Only 3 of 19 cases were positive for two or fewer tumor-associated antigens (TAAs); 16 of 19 cases were positive for three or more TAAs. In the 13 adult cases, all 13 demonstrated positive staining for EphA2, IL-13Rα2, and Survivin. Only 2 of 13 cases (15 %) demonstrated positive staining for WT1. All adult specimens were positive for three or more TAAs. Some ependymomas showed patchy variability in intensity. Pediatric and adult ependymomas frequently express EphA2, IL-13Rα2, and Survivin. This provides the basis for the utilization of an established multiple peptide vaccine for ependymoma in a clinical trial setting.
机译:尽管进行了手术和放疗,但仍有多达50%的室间隔瘤儿童患有肿瘤复发,最终导致死亡。我们小组针对EphA2,IL-13Rα2和Survivin的最初基于肽的神经胶质瘤疫苗在儿童神经胶质瘤中过度表达,在其初始测试阶段已显示出希望。因此,我们调查了EphA2,IL-13Rα2,Survivin,以及Wilms肿瘤1(WT1)在小儿室管膜瘤中是否过表达,以确定是否可以采用类似的免疫疗法。在19个儿科和13个成人室管膜瘤的石蜡包埋标本上,使用对EphA2,IL-13Rα2,Survivin和WT1特异的抗体进行免疫组织化学。正常脑和室管膜被用作背景染色对照。阴性染色被定义为在正常脑组织中没有染色或没有与背景强度相等的染色。在19例儿科病例中,有18例(95%)EphA2阳性染色,IL-13Rα2阳性16例(84%),Survivin阳性18例(95%),WT1仅7例(37%)。在19例病例中,只有3例具有两个或更少的肿瘤相关抗原(TAA)阳性。 19例病例中有16例三个或三个以上TAA呈阳性。在13例成人病例中,所有13例均显示EphA2,IL-13Rα2和Survivin呈阳性染色。 13例中只有2例(15%)表现出WT1阳性染色。所有成人标本中三个或三个以上的TAA均为阳性。一些室管膜瘤的强度表现出斑驳的变异性。小儿和成人室管膜瘤经常表达EphA2,IL-13Rα2和Survivin。这为在临床试验中将建立的多肽疫苗用于室管膜瘤提供了基础。

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