Division of Nuclear Medicine, European Institute of Oncology, Via Ripamonti, 435-20141 Milan, Italy.
Eur J Nucl Med Mol Imaging. 2011 Dec;38(12):2125-35. doi: 10.1007/s00259-011-1902-1. Epub 2011 Sep 3.
Peptide receptor radionuclide therapy (PRRT) is used in tumours expressing type 2 somatostatin receptors (sst(2)), mainly neuroendocrine. The aim of this prospective phase I-II study was to evaluate the toxicity and efficacy of (177)Lu-DOTATATE in multiple cycles.
Fifty-one consecutive patients with unresectable/metastatic sst(2)-positive tumours, divided into two groups, received escalating activities (3.7-5.18 GBq/cycle, group 1; 5.18-7.4 GBq/cycle, group 2) of (177)Lu-DOTATATE. Cumulative activities ranged from 3.7 to 29.2 GBq (median 26.4 GBq in median 6 cycles, group 1, 21 patients) and 5.55 to 28.9 GBq (median 25.2 GBq in 4 cycles, group 2, 30 patients), based on dosimetry.
No major acute or delayed renal or haematological toxicity occurred (one grade 3 leukopenia and thrombocytopenia). Cumulative renal absorbed doses were 8-37 Gy (9-41 Gy bioeffective doses). A median decrease of creatinine clearance of 21.7% 6 months after PRRT, 23.9% after 1 year and 27.6% after 2 years was observed. Higher losses (>20%) occurred in patients with risk factors for renal toxicity, particularly hypertension and diabetes. Cumulative bone marrow doses were <1.5 Gy. Blood elements showed a progressive mild drop during cycles and recovered during follow-up (median 30 months). Thirty-nine patients were progressive at enrolment. Partial and complete responses occurred in 15 of 46 (32.6%) assessable patients. The median time to progression was 36 months. Overall survival was 68% at 36 months. Non-responders and patients with extensive tumour involvement had lower survival.
(177)Lu-DOTATATE was well tolerated up to 29 GBq cumulative activity (up to 7.4 GBq/cycle). The maximum tolerated dose/cycle was not reached. However, considering the individual bone marrow function and the presence of risk factors for kidney toxicity, it seems safer to divide cumulative activities into lower activity cycles.
肽受体放射性核素疗法(PRRT)用于表达 2 型生长抑素受体(sst(2))的肿瘤,主要是神经内分泌肿瘤。本前瞻性 I- II 期研究的目的是评估多次(177)Lu-DOTATATE 治疗的毒性和疗效。
51 例不可切除/转移性 sst(2)阳性肿瘤患者分为两组,接受递增剂量(3.7-5.18GBq/周期,组 1;5.18-7.4GBq/周期,组 2)的(177)Lu-DOTATATE。累积活度范围为 3.7-29.2GBq(中位数 26.4GBq,中位数 6 个周期,组 1,21 例)和 5.55-28.9GBq(中位数 25.2GBq,中位数 4 个周期,组 2,30 例),基于剂量学。
无严重急性或迟发性肾或血液学毒性(1 例 3 级白细胞减少和血小板减少)。累积肾吸收剂量为 8-37Gy(9-41Gy 生物有效剂量)。PRRT 后 6 个月、1 年后和 2 年后观察到肌酐清除率中位数分别下降 21.7%、23.9%和 27.6%。有肾毒性危险因素的患者(尤其是高血压和糖尿病)发生较高的损失(>20%)。累积骨髓剂量<1.5Gy。血液元素在周期中逐渐轻微下降,并在随访中恢复(中位数 30 个月)。39 名患者在入组时进展。46 名可评估患者中有 15 名(32.6%)出现部分和完全缓解。中位进展时间为 36 个月。36 个月时总生存率为 68%。无反应者和广泛肿瘤受累者的生存率较低。
(177)Lu-DOTATATE 累积活度高达 29GBq(高达 7.4GBq/周期)时耐受性良好。未达到最大耐受剂量/周期。然而,考虑到个体骨髓功能和肾毒性危险因素的存在,将累积活度分为较低的活性周期似乎更安全。
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