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在结肠癌异种移植模型中,大剂量推注与持续注射CC49单克隆抗体的剂量学比较。

Dosimetric comparison of bolus and continuous injections of CC49 monoclonal antibody in a colon cancer xenograft model.

作者信息

Roberson P L, Dudek S, Buchsbaum D J

机构信息

The University of Michigan Medical Center, Ann Arbor 48109-0010, USA.

出版信息

Cancer. 1997 Dec 15;80(12 Suppl):2567-75. doi: 10.1002/(sici)1097-0142(19971215)80:12+<2567::aid-cncr32>3.3.co;2-4.

Abstract

BACKGROUND

Improved understanding of dose and effective dose calculations may contribute to the optimization of fractionated radioimmunotherapy.

METHODS

Comparison three-dimensional tumor dosimetry was performed on athymic nude mice bearing established LS174T human colon carcinoma xenografts. Mice were given bolus intraperitoneal injections of 300 microCi 131I-labeled CC49 monoclonal antibody once (Day 0) or three times (Days 0, 3, and 7) or continuous intraperitoneal infusion with miniosmotic pumps over 7 days. Serial section autoradiography was used to reconstruct tumor activity density distributions for Days 3, 4, 7, 10, and 11 (single injection); Days 3, 4, 7, 8, and 11 (3 injections); and Days 4, 7, 10, and 13 (pump). At least three tumors were reconstructed at each time point. Uptakes in blood and tumor were measured up to 14 days (single injection), 11 days (3 injections), or 16 days (pump) after injection.

RESULTS

Average dose values calculated from total activity uptake data only (assuming no energy loss external to the tumor) yielded 102 Gy (single injection), 158 Gy (three injections), and 47 Gy (pump). Average doses using three-dimensional dose calculations were 88 Gy, 139 Gy, and 40 Gy, respectively. The nonuniformity of dose deposition affects treatment outcome, because cell loss is an exponential function of dose. Using the linear quadratic model with fractional cell survival to define an effective dose, D(eff) were calculated to be 20 Gy, 23 Gy, and 14 Gy, respectively. Cell proliferation affects outcome for variable dose-rate treatments. With cell proliferation parameters set to reproduce single-fraction 60Co recurrence results, D(eff) (for local control endpoint) were 8.9 Gy, 12.8 Gy, and 3.9 Gy, respectively. Three bolus injections compared with a single bolus injection were relatively less efficient in tumor uptake. However, three bolus injections resulted in a more uniform dose rate over a longer period, resulting in a 50% improvement in D(eff). The slower dose delivery for pump infusion resulted in a significantly lower D(eff), although dose-rate distributions were more uniform compared with the single bolus injection.

CONCLUSIONS

Improvement in dose-rate nonuniformities was observed for fractionated and continuous radiolabeled monoclonal antibody injections. Fractionated injections produced superior dosimetric results compared with single bolus or continuous injections.

摘要

背景

更好地理解剂量和有效剂量计算可能有助于优化分次放射免疫治疗。

方法

对携带已建立的LS174T人结肠癌异种移植瘤的无胸腺裸鼠进行三维肿瘤剂量测定比较。小鼠在第0天接受一次300微居里131I标记的CC49单克隆抗体的腹腔推注,或在第0、3和7天接受三次推注,或通过微型渗透泵连续腹腔输注7天。使用连续切片放射自显影术重建第3、4、7、10和11天(单次注射);第3、4、7、8和11天(三次注射);以及第4、7、10和13天(泵注)的肿瘤活性密度分布。每个时间点至少重建三个肿瘤。在注射后14天(单次注射)、11天(三次注射)或16天(泵注)测量血液和肿瘤中的摄取量。

结果

仅根据总活性摄取数据计算的平均剂量值(假设肿瘤外部无能量损失)分别为102 Gy(单次注射)、158 Gy(三次注射)和47 Gy(泵注)。使用三维剂量计算的平均剂量分别为88 Gy、139 Gy和40 Gy。剂量沉积的不均匀性会影响治疗结果,因为细胞损失是剂量的指数函数。使用具有分数细胞存活的线性二次模型来定义有效剂量,计算得出的D(eff)分别为20 Gy、23 Gy和14 Gy。细胞增殖会影响可变剂量率治疗的结果。将细胞增殖参数设置为重现单次分割60Co复发结果时,(局部控制终点的)D(eff)分别为8.9 Gy、12.8 Gy和3.9 Gy。与单次推注相比,三次推注在肿瘤摄取方面效率相对较低。然而,三次推注在更长时间内导致更均匀的剂量率,使D(eff)提高了50%。泵注的较慢剂量递送导致D(eff)显著降低,尽管与单次推注相比剂量率分布更均匀。

结论

对于分次和连续放射性标记单克隆抗体注射,观察到剂量率不均匀性有所改善。与单次推注或连续注射相比

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