Jostel Andreas, Mukherjee Annice, Hulse Paul A, Shalet Stephen M
Department of Endocrinology, Christie Hospital, Wilmslow Road, Manchester, M20 4BX, UK.
Clin Endocrinol (Oxf). 2005 Jun;62(6):698-705. doi: 10.1111/j.1365-2265.2005.02282.x.
Systematic collections of neuroimaging data are nonexistent in brain tumour survivors treated with adult growth hormone replacement therapy (AGHRT). We present our surveillance data.
In 1993, our unit implemented a policy of performing brain scans on every brain tumour survivor before starting AGHRT, with repeat neuroimaging at least once after 12-18 months' treatment. Reports for baseline scans and most recent scans were analysed for this retrospective study.
All brain tumour survivors who received AGHRT (60 patients) were included in the analysis.
Evidence and extent of residual tumour, tumour progression, tumour recurrence, and secondary neoplasms (SN) on baseline scan and latest follow-up scan.
All patients had baseline scans performed. Follow-up scans were available in 41/45 (91%) patients who received AGHRT for more than 1 year (mean duration +/- SD of GHRT was 6.7 +/- 3.6 years). Sixteen patients had residual tumours, and SNs (all meningiomas) were demonstrated in three patients on baseline scans. Appearances remained stable in 34 (83%) patients during follow-up (extending to 17.4 +/- 8.3 years after tumour diagnosis). Of the 16 residual primary tumours, an incurable ependymoma continued to grow, and one meningioma progressed slightly in size over 7.7 years. Follow-up scans also revealed continued growth of the SNs detected at baseline, and five additional meningiomas (two in patients with a previous SN, confirming an excess risk in this subgroup, P = 0.02). All SNs occurred on average 22.8 (range 17-37) years after radiotherapy.
Our data do not suggest an increased rate of recurrence or progression of childhood brain tumours during AGHRT. Nonetheless, vigilance and long-term surveillance are needed in these patients in order to detect and monitor SNs, in particular in patients with a previous history of a SN. We endorse a proactive neuroimaging policy, preferably as part of a larger, controlled trial in the future.
接受成人生长激素替代疗法(AGHRT)治疗的脑肿瘤幸存者中不存在神经影像学数据的系统收集情况。我们展示我们的监测数据。
1993年,我们科室实施了一项政策,即在开始AGHRT之前对每位脑肿瘤幸存者进行脑部扫描,并在治疗12 - 18个月后至少重复进行一次神经影像学检查。对基线扫描和最近扫描的报告进行分析以开展这项回顾性研究。
所有接受AGHRT的脑肿瘤幸存者(60例患者)均纳入分析。
基线扫描和最新随访扫描时残留肿瘤的证据和范围、肿瘤进展、肿瘤复发及继发性肿瘤(SN)情况。
所有患者均进行了基线扫描。45例接受AGHRT超过1年的患者中有41例(91%)有随访扫描结果(生长激素替代疗法的平均持续时间±标准差为6.7±3.6年)。16例患者有残留肿瘤,3例患者在基线扫描时发现有继发性肿瘤(均为脑膜瘤)。34例(83%)患者在随访期间(肿瘤诊断后长达17.4±8.3年)病情保持稳定。16例残留的原发性肿瘤中,一例无法治愈的室管膜瘤持续生长,一例脑膜瘤在7.7年中体积略有增大。随访扫描还显示基线时检测到的继发性肿瘤持续生长,另外还有5例脑膜瘤(2例在既往有继发性肿瘤的患者中,证实该亚组存在额外风险,P = 0.02)。所有继发性肿瘤平均在放疗后22.8年(范围17 - 37年)出现。
我们的数据未提示AGHRT期间儿童脑肿瘤的复发或进展率增加。尽管如此,这些患者仍需要保持警惕并进行长期监测,以便检测和监测继发性肿瘤,特别是既往有继发性肿瘤病史的患者。我们支持积极的神经影像学检查政策,最好作为未来一项更大规模对照试验的一部分。
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