Malignant glioma as a secondary malignant neoplasm after radiation therapy for craniopharyngioma - Report of a case and review of reported cases

被引:40
|
作者
Kranzinger, M
Jones, N
Rittinger, O
Pilz, P
Piotrowski, WP
Manzl, M
Galvan, G
Kogelnik, HD
机构
[1] Landeskliniken Salzburg, St Johanns Spital, Inst Radiotherapie & Radioonkol, A-5020 Salzburg, Austria
[2] Landeskliniken Salzburg, St Johanns Spital, Abt Kinderheilkunde, A-5020 Salzburg, Austria
[3] Landeskliniken Salzburg, St Johanns Spital, Inst Neuropathol, A-5020 Salzburg, Austria
[4] Landeskliniken Salzburg, Christian Doppler Klin, Abt Neurochirurg, Salzburg, Austria
来源
ONKOLOGIE | 2001年 / 24卷 / 01期
关键词
secondary malignant neoplasm; craniopharyngioma; growth hormone; late effects;
D O I
10.1159/000050285
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background: The development of a secondary neoplasm in childhood cancer survivors attains growing importance due to the reported excellent survival and therefore the long exposure to potentially carcinogenic effects of treatment. Case Report: We report a 14-year-old girl in whom a large craniopharyngioma (CP) was diagnosed. After surgery, radiation therapy (RT) was given for residual tumour. Discrete progression necessitated further surgery, resulting in permanent tumour control. Soon after the second surgery hypothalamic-pituitary dysfunction developed together with obesity. Supportive hormone therapy was initiated. Growth hormone (GH) therapy was also given for 15 months. Four years after the diagnosis, a cerebropontine anaplastic astrocytoma WHO grade III was detected, with the main lesion being at the dorsal edge of the irradiated area. The girl died 1 month later from this secondary presumably radiation-induced tumour. Only recently a second child with RT for a CP was diagnosed with malignant glioma in our hospital. Case Reports in the Literature: 12 other cases of malignant glioma have been reported after RT for CP. Including our present cases, the mean latency period was 10.7 years (median 9.6 years). However, the shortest latency periods were found in patients who had received GH therapy. In numerous cases, the secondary tumour was seen at the edge of the irradiated volume, and not in the region with the highest absorbed dose. Conclusions:Therapy-induced secondary gliomas after treatment of CP or other intracranial tumours are rare but dramatic late events with a very poor prognosis. Including our own 2 patients, we reviewed 14 cases of CP with occurrence of a secondary, probably radiation-induced malignant glioma. The short latency periods for patients treated with GH is remarkable. We therefore suspect that GH therapy may accelerate the development of a secondary brain tumour. We are reluctant to recommend GH therapy in conventionally irradiated CP patients. In order to seriously answer the questions about therapy-induced secondary neoplasms, a lifelong follow-up is mandatory for all patients who are survivors of childhood cancer.
引用
收藏
页码:66 / 72
页数:7
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