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Expression of pERK and pAKT in human astrocytomas: correlation with IDH1-R132H presence, vascular endothelial growth factor, microvascular characteristics and clinical outcome

机译:pERK和pAKT在人星形细胞瘤中的表达:与IDH1-R132H存在,血管内皮生长因子,微血管特征和临床结局的相关性

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Although pERK and pAKT are reportedly activated in various neoplasms, little information is available about their significance in astrocytomas. Paraffin-embedded tissue from 82 patients with diffuse infiltrating astrocytomas (grades II to IV) was investigated for the association of pERK and pAKT activation with clinicopathological features, vascular endothelial growth factor (VEGF), isocitrate dehydrogenase 1 and microvascular parameters. Nuclear pERK labelling index (LI) increased with increasing cytoplasmic pERK LI and nuclear and cytoplasmic pAKT LI (p = 0.0019, p = 0.0260 and p = 0.0012, respectively). Accordingly, cytoplasmic pERK increased with increasing levels of nuclear (p = 0.0001) and marginally with cytoplasmic pAKT LI (p = 0.0526). Nuclear and cytoplasmic pERK LI and nuclear pAKT LI were positively correlated with tumour histological grade (p = 0.0040, p = 0.0238 for pERK and p = 0.0004 for pAKT, respectively). VEGF expression was correlated with nuclear pERK (p = 0.0099) and nuclear pAKT LI (p = 0.0002). Interestingly, pERK cytoplasmic LI increased with microvessel calibre (p = 0.0287), whereas pAKT nuclear LI was marginally related to microvessel density (p = 0.0685). The presence of IDH1-R132H was related only to histological grade and lower microvessel calibre. Multivariate survival analysis in the entire cohort selected cytoplasmic pAKT LI (p = 0.045), histological grade, microvessel calibre (p = 0.028), patients' age, gender and surgical excision as independent predictors of survival. Moreover, in glioblastomas, pERK nuclear LI emerged as a favourable prognosticator in the presence of IDH1-R132H. pERK and pAKT in astrocytomas are interrelated and associated with tumour grade and angiogenesis. Moreover, the importance of cytoplasmic pAKT immunoexpression in patients' prognosis and nuclear pERK immunoexpression in glioblastomas is confirmed.
机译:尽管据报道pERK和pAKT在多种肿瘤中被激活,但是关于它们在星形细胞瘤中的重要性的信息很少。研究了82例弥漫性浸润性星形细胞瘤患者的石蜡包埋组织(II至IV级)与pERK和pAKT活化与临床病理特征,血管内皮生长因子(VEGF),异柠檬酸脱氢酶1和微血管参数之间的关系。核pERK标记指数(LI)随细胞质pERK LI和核及细胞质pAKT LI的增加而增加(分别为p = 0.0019,p = 0.0260和p = 0.0012)。因此,细胞质pERK随着核水平的增加而增加(p = 0.0001),而随着细胞质pAKT LI的增加而略有增加(p = 0.0526)。核和细胞质pERK LI和核pAKT LI与肿瘤组织学分级呈正相关(pERK分别为p = 0.0040,p = 0.0238和pAKT为p = 0.0004)。 VEGF表达与核pERK(p = 0.0099)和核pAKT LI(p = 0.0002)相关。有趣的是,pERK细胞质LI随微血管口径而增加(p = 0.0287),而pAKT核LI与微血管密度微相关(p = 0.0685)。 IDH1-R132H的存在仅与组织学等级和较低的微血管口径有关。整个队列的多变量生存分析选择了细胞质pAKT LI(p = 0.045),组织学等级,微血管口径(p = 0.028),患者的年龄,性别和手术切除作为生存的独立预测因子。此外,在成胶质细胞瘤中,在存在IDH1-R132H的情况下,pERK核LI成为一种有利的预后指标。星形细胞瘤中的pERK和pAKT是相互关联的,并与肿瘤的分级和血管生成有关。此外,证实了细胞质pAKT免疫表达在胶质母细胞瘤患者的预后和核pERK免疫表达中的重要性。

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