一种在人神经母细胞瘤细胞中具有延长滞留时间的4-甲基取代间碘苄胍类似物。

A 4-methyl-substituted meta-iodobenzylguanidine analogue with prolonged retention in human neuroblastoma cells.

作者信息

Vaidyanathan Ganesan, Welsh Philip C, Vitorello Katia C, Snyder Stacey, Friedman Henry S, Zalutsky Michael R

机构信息

Department of Radiology, Duke University Medical Center, Durham, NC 27710, USA.

出版信息

Eur J Nucl Med Mol Imaging. 2004 Oct;31(10):1362-70. doi: 10.1007/s00259-004-1596-8. Epub 2004 Jun 16.

DOI:10.1007/s00259-004-1596-8

PMID:15205923

Abstract

PURPOSE

As a part of our efforts to develop a meta-iodobenzylguanidine (MIBG) analogue with improved characteristics for the diagnosis and treatment of neuroendocrine tumours, 3-[131I]iodo-4-methyl-benzylguanidine ([131I]MeIBG) has been developed. The purpose of this study was to evaluate [131I]MeIBG in vitro using the uptake-1 positive SK-N-SH neuroblastoma cell line and in vivo in normal mice and mice bearing human neuroblastoma xenografts.

METHODS

The ability of SK-N-SH human neuroblastoma cells to retain [131I]MeIBG in vitro over a period of 4 days, in comparison to [125I]MIBG, was determined by a paired-label assay. Paired-label biodistributions of [131I]MeIBG and [125I]MIBG were performed in normal mice as well as in athymic mice bearing SK-N-SH and IMR-32 human neuroblastoma xenografts.

RESULTS

Retention of [131I]MeIBG by SK-N-SH cells in vitro was increased by factors of 1.2, 1.5, 2.0, 2.5 and 3.1 compared with [125I]MIBG at 8, 24, 48, 72 and 96 h, respectively. In normal mice, the uptake of [131I]MeIBG in the heart was similar to that of [125I]MIBG at 1 and 4 h; in contrast, myocardial uptake of [131I]MeIBG was 1.6-fold higher than that of [125I]MIBG (p<0.05) at 24 h. When mice were pre-treated with the uptake-1 inhibitor desipramine (DMI), the heart uptake of both tracers was reduced to about half that in untreated controls at 1 h post injection (p<0.05). The hepatic uptake of [131I]MeIBG was two- to threefold lower than that of [125I]MIBG. On the other hand, blood levels of [131I]MeIBG were substantially higher (up to sixfold), especially at early time points. Uptake of [131I]MeIBG in heart and tumour at 1 h in the murine SK-N-SH model was specific and comparable to that of [125I]MIBG. However, [131I]MeIBG uptake was 1.6- to 1.7-fold lower than that of [125I]MIBG over 4-48 h. While the uptake of both tracers in IMR32 xenografts was similar, it was not uptake-1 mediated.

CONCLUSION

Introduction of a methyl group at the 4-position of MIBG seems to be advantageous in terms of higher tumour retention in vitro and lower hepatic uptake in vivo. However, the slower blood clearance of MeIBG may be problematic for some applications.

摘要

目的

作为我们开发一种具有改进特性的间碘苄胍（MIBG）类似物用于神经内分泌肿瘤诊断和治疗工作的一部分，已研发出3 - [¹³¹I]碘 - 4 - 甲基苄胍（[¹³¹I]MeIBG）。本研究的目的是使用摄取 - 1阳性的SK - N - SH神经母细胞瘤细胞系在体外以及在正常小鼠和携带人神经母细胞瘤异种移植瘤的小鼠体内评估[¹³¹I]MeIBG。

方法

通过配对标记试验确定SK - N - SH人神经母细胞瘤细胞在体外4天内与[¹²⁵I]MIBG相比保留[¹³¹I]MeIBG的能力。在正常小鼠以及携带SK - N - SH和IMR - 32人神经母细胞瘤异种移植瘤的无胸腺小鼠中进行了[¹³¹I]MeIBG和[¹²⁵I]MIBG的配对标记生物分布研究。

结果

与[¹²⁵I]MIBG相比，SK - N - SH细胞在体外对[¹³¹I]MeIBG的保留在8、24、48、72和96小时分别增加了1.2、1.5、2.0、2.5和3.1倍。在正常小鼠中，[¹³¹I]MeIBG在心脏中的摄取在1小时和4小时时与[¹²⁵I]MIBG相似；相比之下，[¹³¹I]MeIBG在24小时时心肌摄取比[¹²⁵I]MIBG高1.6倍（p<0.05）。当小鼠用摄取 - 1抑制剂地昔帕明（DMI）预处理时，两种示踪剂在心脏中的摄取在注射后1小时降至未处理对照组的约一半（p<0.05）。[¹³¹I]MeIBG的肝脏摄取比[¹²⁵I]MIBG低两到三倍。另一方面，[¹³¹I]MeIBG的血药浓度显著更高（高达六倍），尤其是在早期时间点。在小鼠SK - N - SH模型中，[¹³¹I]MeIBG在1小时时在心脏和肿瘤中的摄取具有特异性且与[¹²⁵I]MIBG相当。然而，在4 - 48小时内，[¹³¹I]MeIBG的摄取比[¹²⁵I]MIBG低1.6 - 1.7倍。虽然两种示踪剂在IMR32异种移植瘤中的摄取相似，但不是由摄取 - 1介导的。