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载脂蛋白E基因敲除小鼠实验性动脉粥样硬化病变的成像:用Z2D3-抗二乙三胺五乙酸双特异性抗体和99mTc标记的带负电荷聚合物增强靶向作用。

Imaging experimental atherosclerotic lesions in ApoE knockout mice: enhanced targeting with Z2D3-anti-DTPA bispecific antibody and 99mTc-labeled negatively charged polymers.

作者信息

Khaw Ban-An, Tekabe Yared, Johnson Lynne L

机构信息

Center for Cardiovascular Targeting, School of Pharmacy, Bouve College of Health Sciences, Northeastern University, Boston, MA 02115, USA.

出版信息

J Nucl Med. 2006 May;47(5):868-76.

PMID:16644758
Abstract

UNLABELLED

In vivo molecular imaging may be improved if specific radioactivity at the target site could be increased while maintaining low background activity. Bispecific antibody complexes and (99m)Tc-labeled negatively charged chelating polymers that react specifically with the capture arm of the bispecific antibody complex were used to demonstrate the feasibility of imaging very small atherosclerotic lesions in ApoE knockout mice.

METHODS

Left femoral artery denudation in ApoE(-/-) mice on a hyperlipidemic diet was used to induce accelerated atherosclerotic lesions. Approximately 40 microg of bispecific antibodies were injected intravenously after 2 wk of endothelial denudation. The next day, approximately 15.0 MBq (99m)Tc-DTPA-succinyl-polylysine (2 microg; DTPA is diethylenetriaminepentaacetic acid) were injected intravenously.

RESULTS

In vivo gamma-images showed that lesions were observed unequivocally by 2-3 h. Sham-operated right femoral regions showed no radiotracer accumulation. Ex vivo gamma-scintillation counting corrected for sham-operated nonspecific activity and lesion mass showed that the mean lesion activity was 10.10 +/- 6.76 %ID/g (percentage injected dose per gram), whereas nonspecific human IgG bispecific control (NSB control) also corrected similarly was 0.939 +/- 0.877 %ID/g (P < 0.03). Atherosclerotic lesions were confirmed by immunohistochemical staining. Computer planimetry of immunohistograms showed the mean lesion size to be 2.64 +/- 2.46 mg.

CONCLUSION

Use of bispecific antibody complexes and (99m)Tc-DTPA-succinyl-polylysine enabled in vivo visualization of very small atherosclerotic lesions in ApoE knockout mice.

摘要

未标记

如果在保持低本底活性的同时能够提高靶位点的比放射性,那么体内分子成像可能会得到改善。双特异性抗体复合物以及与双特异性抗体复合物的捕获臂特异性反应的(99m)Tc标记的带负电荷螯合聚合物,被用于证明在载脂蛋白E基因敲除小鼠中对非常小的动脉粥样硬化病变进行成像的可行性。

方法

对高脂饮食的载脂蛋白E(-/-)小鼠进行左股动脉剥脱术,以诱导加速动脉粥样硬化病变。在内皮剥脱2周后静脉注射约40微克双特异性抗体。第二天,静脉注射约15.0兆贝可(99m)Tc-DTPA-琥珀酰聚赖氨酸(2微克;DTPA为二乙三胺五乙酸)。

结果

体内γ图像显示,在2至3小时时可明确观察到病变。假手术的右股区域未显示放射性示踪剂积聚。针对假手术非特异性活性和病变质量校正后的体外γ闪烁计数显示,平均病变活性为10.10±6.76%ID/g(每克注射剂量的百分比),而同样校正后的非特异性人IgG双特异性对照(NSB对照)为0.939±0.877%ID/g(P<0.03)。通过免疫组织化学染色确认动脉粥样硬化病变。免疫组织化学图谱的计算机平面测量显示,平均病变大小为2.64±2.46毫克。

结论

使用双特异性抗体复合物和(99m)Tc-DTPA-琥珀酰聚赖氨酸能够在载脂蛋白E基因敲除小鼠体内可视化非常小的动脉粥样硬化病变。

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