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长期存活的低级别胶质瘤中增殖与凋亡和放疗的关系

Proliferation and apoptosis in long-term surviving low grade gliomas in relation to radiotherapy.

作者信息

Heesters Mart A A M, Koudstaal Jan, Go K Gwan, Molenaar Willemina M

机构信息

Department of Radiotherapy, University Hospital, Groningen, The Netherlands.

出版信息

J Neurooncol. 2002 Jun;58(2):157-65. doi: 10.1023/a:1016046125698.

Abstract

Identification of patients with a low grade glioma with a long-term recurrence-free survival is of clinical value as radiotherapy can be postponed until recurrence. The recurring glioma may increase in malignancy compared to the original tumor, which is possibly related to radiotherapy. We studied proliferation by counting mitotic figures and by MIB-1 labeling, apoptosis by TUNEL and expression of proteins related to cell cycle regulation by immunohistochemical analysis of p53, p21, bcl-2 and bax expression in 48 low grade gliomas. Astrocytomas (A, n = 14) and oligodendrogliomas (O, n = 4) with a recurrence-free survival of more than 9 years after surgery had a signficantly lower p53 index compared to A (n = 18) and O (n = 12) with a histopathologically documented recurrence. Additionally, the recurrence-free A had a higher p21 index. No significant differences were observed in MIB-LI, TUNEL-LI, bcl-2 and bax expression. Initially low grade gliomas and their corresponding recurrences were compared (n = 30). In the gliomas without radiotherapy (n = 15), no differences in mitotic rate, TUNEL-LI, p53, p21, bcl-2 and bax expression were found between primary tumors and their recurrences. Only MIB-LI was higher in the recurrent tumors. In the gliomas with radiotherapy (n = 15) no differences were detected in these parameters between the original tumor and the recurrent tumor except for a higher number of mitoses in the recurrent tumors. We conclude that low grade gliomas with a long-term recurrence-free survival were characterized by a low p53 protein expression and, in the case of A, a higher p21 index. We found no evidence that radiotherapy is involved in changes of proliferation, apoptosis or expression of proteins related to cell cycle regulation in recurring gliomas.

摘要

识别长期无复发生存的低级别胶质瘤患者具有临床价值,因为放疗可推迟至复发时进行。与原始肿瘤相比,复发性胶质瘤的恶性程度可能增加,这可能与放疗有关。我们通过计数有丝分裂象和进行MIB-1标记来研究增殖,通过TUNEL检测凋亡,并通过免疫组织化学分析p53、p21、bcl-2和bax的表达来研究与细胞周期调控相关的蛋白质在48例低级别胶质瘤中的表达。术后无复发生存超过9年的星形细胞瘤(A,n = 14)和少突胶质细胞瘤(O,n = 4)与组织病理学记录有复发的A(n = 18)和O(n = 12)相比,p53指数显著更低。此外,无复发生存的A的p21指数更高。在MIB-LI、TUNEL-LI、bcl-2和bax表达方面未观察到显著差异。最初比较了低级别胶质瘤及其相应的复发瘤(n = 30)。在未接受放疗的胶质瘤(n = 15)中,原发肿瘤与其复发瘤在有丝分裂率、TUNEL-LI、p53、p21、bcl-2和bax表达方面未发现差异。仅复发瘤中的MIB-LI更高。在接受放疗的胶质瘤(n = 15)中,除了复发瘤中有丝分裂数量更多外,在这些参数方面原始肿瘤与复发瘤之间未检测到差异。我们得出结论,长期无复发生存的低级别胶质瘤的特征是p53蛋白表达低,对于星形细胞瘤而言,p21指数更高。我们没有发现证据表明放疗与复发性胶质瘤的增殖、凋亡或与细胞周期调控相关的蛋白质表达变化有关。

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