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治疗相关的恶性脑胶质瘤患者淋巴细胞减少症的病因:模拟辐射剂量对循环淋巴细胞的影响可解释临床观察结果,并提出了改变辐射对免疫细胞影响的方法。

The etiology of treatment-related lymphopenia in patients with malignant gliomas: modeling radiation dose to circulating lymphocytes explains clinical observations and suggests methods of modifying the impact of radiation on immune cells.

机构信息

Department of Radiation Oncology, Johns Hopkins University School of Medicine, Baltimore, MD, USA

出版信息

Cancer Invest. 2013 Feb;31(2):140-4. doi: 10.3109/07357907.2012.762780.

Abstract

PURPOSE

Severe treatment-related lymphopenia (TRL) occurs in 40% of patients with high grade gliomas (HGG) receiving glucocorticoids, temozolomide, and radiation. This occurs following radiation, persists for months, and is associated with reduced survival. As all three treatment modalities are lymphotoxic, this study was conducted to estimate the radiation dose that lymphocytes receive passing through the radiation field and if this could explain the observed TRL.

MATERIALS AND METHODS

A typical glioblastoma plan (8-cm tumor, 60 Gy/30 fractions) was constructed using the Pinnacle™ radiation planning system. Radiation doses to circulating cells (DCC) were analyzed using MatLab™. The primary endpoints were mean DCC and percent of circulating cells receiving ≥0.5 Gy. The model was also used to study how changes in target volumes (PTV), dose rates, and delivery techniques affect DCC.

RESULTS

The modeling determined that while a single radiation fraction delivered 0.5 Gy to 5% of circulating cells, after 30 fractions 99% of circulating blood had received ≥0.5 Gy. The mean DCC was 2.2 Gy and was similar for IMRT, 3D-conformal techniques, and different dose rates. Major changes in PTV size affected mean DCC and percent of circulating cells receiving ≥0.5 Gy.

CONCLUSIONS

Standard treatment plans for brain tumors deliver potentially lymphotoxic radiation doses to the entire circulating blood pool. Altering dose rates or delivery techniques are unlikely to significantly affect DCC by the end of treatment. Novel approaches are needed to limit radiation to circulating lymphocytes given the association of lymphopenia with poorer survival in patients with HGG.

摘要

目的

接受糖皮质激素、替莫唑胺和放疗的高级别神经胶质瘤(HGG)患者中有 40%发生严重的治疗相关淋巴细胞减少症(TRL)。这种情况发生在放疗后,持续数月,并与生存率降低有关。由于这三种治疗方式均具有淋巴细胞毒性,因此进行了这项研究,以评估淋巴细胞在穿过放射野时所接受的放射剂量,以及这是否可以解释观察到的 TRL。

材料和方法

使用 Pinnacle™ 放射规划系统构建典型的胶质母细胞瘤计划(8 厘米肿瘤,60 Gy/30 个分次)。使用 MatLab™ 分析循环细胞(DCC)的放射剂量。主要终点是平均 DCC 和接受≥0.5 Gy 的循环细胞百分比。该模型还用于研究靶区(PTV)、剂量率和递送技术的变化如何影响 DCC。

结果

模型确定,单次放射分次可使 5%的循环细胞接受 0.5 Gy 的剂量,而在 30 个分次后,99%的循环血液接受了≥0.5 Gy 的剂量。平均 DCC 为 2.2 Gy,适用于调强放疗、三维适形技术和不同的剂量率。PTV 大小的主要变化会影响平均 DCC 和接受≥0.5 Gy 的循环细胞百分比。

结论

标准的脑肿瘤治疗方案会向整个循环血液池输送潜在的具有淋巴细胞毒性的放射剂量。改变剂量率或递送技术不太可能在治疗结束时显著影响 DCC。鉴于淋巴细胞减少症与 HGG 患者的生存率降低有关,需要采取新的方法来限制对循环淋巴细胞的放射。

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