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首页> 外文期刊>Cancer biotherapy and radiopharmaceuticals >Biodistribution of 131I-, 186Re-, 177Lu-, and 88Y-labeled hLL2 (Epratuzumab) in nude mice with CD22-positive lymphoma.
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Biodistribution of 131I-, 186Re-, 177Lu-, and 88Y-labeled hLL2 (Epratuzumab) in nude mice with CD22-positive lymphoma.

机译:131I,186Re,177Lu和88Y标记的hLL2(依普妥珠单抗)在CD22阳性淋巴瘤裸鼠中的生物分布。

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摘要

Radioimmunotherapy (RIT) is a new and effective treatment modality in patients with non-Hodgkin's lymphoma. The monoclonal antibody (mAb) hLL2 (epratuzumab), a humanized mAb directed against the CD22 antigen, and which internalizes, can be labeled with various radionuclides. The biodistribution of hLL2 labeled with (131)I, (186)Re, (177)Lu, and (88)Y was studied in nude mice with subcutaneous human lymphoma xenografts in order to determine the most suitable of these four radionuclides for RIT with hLL2. METHODS: Human Ramos lymphoma xenografts were transplanted in cyclophosphamide-pretreated athymic BALB/c mice. Four groups of mice were injected intravenously with (131)I-, (186)Re-, (88)Y-, or (177)Lu-labeled hLL2, respectively. To determine the nonspecific tumor uptake, two groups of mice received (88)Y-labeled or (131)I-labeled control antibody, cG250. The biodistribution of the radiolabel was determined 1, 3, and 7 days postinjection (p.i.). RESULTS: Radiolabeled hLL2 had a higher tumor uptake than the nonspecific mAb at all time-points, irrespective of the radiolabel used. Tumor accretion of (88)Y- and (177)Lu-hLL2 was higher than tumor uptake of (131)I- and (186)Re-hLL2. Activity in the bone, represented by the femur without bone marrow, was higher for (177)Lu- and (88)Y-hLL2 than for (131)I- and (186)Re-hLL2 on day 7 p.i. CONCLUSION: The use of the residualizing radiolabels (88)Y and (177)Lu in combination with a mAb directed against an internalizing antigen resulted in higher uptake and better retention of the radiolabel in the tumor.
机译:放射免疫疗法(RIT)是非霍奇金淋巴瘤患者的一种新型有效治疗方法。单克隆抗体(mAb)hLL2(依帕珠单抗)是针对CD22抗原的人源化单克隆抗体,它可以内在化,可以用各种放射性核素标记。在具有皮下人淋巴瘤异种移植物的裸鼠中研究了用(131)I,(186)Re,(177)Lu和(88)Y标记的hLL2的生物分布,以确定这四种放射性核素最适合RIT hLL2。方法:将人类Ramos淋巴瘤异种移植物移植到环磷酰胺预处理的无胸腺BALB / c小鼠中。四组小鼠分别静脉注射(131)I-,(186)Re-,(88)Y-或(177)Lu标记的hLL2。为了确定非特异性肿瘤摄取,两组小鼠接受(88)Y标记的或(131)I标记的对照抗体cG250。在注射后1、3和7天(p.i.)确定放射性标记的生物分布。结果:放射性标记的hLL2在所有时间点均比非特异性mAb吸收更高的肿瘤,而与所使用的放射性标记无关。 (88)Y-和(177)Lu-hLL2的肿瘤积聚高于(131)I-和(186)Re-hLL2的肿瘤吸收。 (177)Lu-和(88)Y-hLL2在第7天p.i时比(131)I-和(186)Re-hLL2的骨活性更高。结论:将残留的放射性标记(88)Y和(177)Lu与针对内在化抗原的mAb结合使用可导致放射性标记在肿瘤中的吸收和保留更高。

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