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与绿脓杆菌外毒素结合的白细胞介素13的实时、图像引导、对流增强递送

Real-time, image-guided, convection-enhanced delivery of interleukin 13 bound to pseudomonas exotoxin.

作者信息

Murad Gregory J A, Walbridge Stuart, Morrison Paul F, Garmestani Kayhan, Degen Jeffrey W, Brechbiel Martin W, Oldfield Edward H, Lonser Russell R

机构信息

Surgical Neurology Branch, National Institute of Neurological Disorders and Stroke, NIH, Bethesda, Maryland 20892-1414, USA.

出版信息

Clin Cancer Res. 2006 May 15;12(10):3145-51. doi: 10.1158/1078-0432.CCR-05-2583.

Abstract

PURPOSE

To determine if the tumor-targeted cytotoxin interleukin 13 bound to Pseudomonas exotoxin (IL13-PE) could be delivered to the brainstem safely at therapeutic doses while monitoring its distribution in real-time using a surrogate magnetic resonance imaging tracer, we used convection-enhanced delivery to perfuse rat and primate brainstems with IL13-PE and gadolinium-bound albumin (Gd-albumin).

EXPERIMENTAL DESIGN

Thirty rats underwent convective brainstem perfusion of IL13-PE (0.25, 0.5, or 10 microg/mL) or vehicle. Twelve primates underwent convective brainstem perfusion of either IL13-PE (0.25, 0.5, or 10 microg/mL; n = 8), co-infusion of 125I-IL13-PE and Gd-albumin (n = 2), or co-infusion of IL13-PE (0.5 microg/mL) and Gd-albumin (n = 2). The animals were permitted to survive for up to 28 days before sacrifice and histologic assessment.

RESULTS

Rats showed no evidence of toxicity at all doses. Primates showed no toxicity at 0.25 or 0.5 microg/mL but showed clinical and histologic toxicity at 10 microg/mL. Quantitative autoradiography confirmed that Gd-albumin precisely tracked IL13-PE anatomic distribution and accurately showed the volume of distribution.

CONCLUSIONS

IL13-PE can be delivered safely and effectively to the primate brainstem at therapeutic concentrations and over clinically relevant volumes using convection-enhanced delivery. Moreover, the distribution of IL13-PE can be accurately tracked by co-infusion of Gd-albumin using real-time magnetic resonance imaging.

摘要

目的

为了确定与绿脓杆菌外毒素结合的肿瘤靶向细胞毒素白细胞介素13(IL13 - PE)能否在治疗剂量下安全地递送至脑干,同时使用替代磁共振成像示踪剂实时监测其分布情况,我们采用对流增强递送技术,用IL13 - PE和钆结合白蛋白(钆 - 白蛋白)灌注大鼠和灵长类动物的脑干。

实验设计

30只大鼠接受了IL13 - PE(0.25、0.5或10微克/毫升)或赋形剂的对流脑干灌注。12只灵长类动物接受了IL13 - PE(0.25、0.5或10微克/毫升;n = 8)的对流脑干灌注、125I - IL13 - PE与钆 - 白蛋白的联合输注(n = 2)或IL13 - PE(0.5微克/毫升)与钆 - 白蛋白的联合输注(n = 2)。在处死和组织学评估前,允许动物存活长达28天。

结果

所有剂量的大鼠均未显示出毒性迹象。灵长类动物在0.25或0.5微克/毫升时未显示出毒性,但在10微克/毫升时显示出临床和组织学毒性。定量放射自显影证实,钆 - 白蛋白精确追踪了IL13 - PE的解剖分布,并准确显示了分布体积。

结论

使用对流增强递送技术,IL13 - PE能够以治疗浓度并在临床相关体积范围内安全有效地递送至灵长类动物脑干。此外,通过实时磁共振成像联合输注钆 - 白蛋白可以准确追踪IL13 - PE的分布情况。

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