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采用优化的染料/光源/相机组合进行实时近红外荧光成像,用于前列腺癌手术引导。

Real-time, near-infrared fluorescence imaging with an optimized dye/light source/camera combination for surgical guidance of prostate cancer.

作者信息

Neuman Brian P, Eifler John B, Castanares Mark, Chowdhury Wasim H, Chen Ying, Mease Ronnie C, Ma Rong, Mukherjee Amarnath, Lupold Shawn E, Pomper Martin G, Rodriguez Ronald

机构信息

James Buchanan Brady Urological Institute and Department of Urology, The Johns Hopkins School of Medicine, Baltimore, Maryland.

The Russell H. Morgan Department of Radiology and Radiological Science, The Johns Hopkins Hospital, Baltimore, Maryland.

出版信息

Clin Cancer Res. 2015 Feb 15;21(4):771-80. doi: 10.1158/1078-0432.CCR-14-0891. Epub 2014 Dec 12.

Abstract

PURPOSE

The prostate-specific membrane antigen (PSMA) is a surface glycoprotein overexpressed on malignant prostate cells, as well as in the neovasculature of many tumors. Recent efforts to target PSMA for imaging prostate cancer rely on suitably functionalized low-molecular-weight agents. YC-27 is a low-molecular-weight, urea-based agent that enables near-infrared (NIR) imaging of PSMA in vivo.

EXPERIMENTAL DESIGN

We have developed and validated a laparoscopic imaging system (including an optimized light source, LumiNIR) that is capable of imaging small tumor burdens with minimal background fluorescence in real-time laparoscopic extirpative surgery of small prostate tumor xenografts in murine and porcine models.

RESULTS

In a mouse model, we demonstrate the feasibility of using real-time NIR laparoscopic imaging to detect and surgically remove PSMA-positive xenografts. We then validate the use of our laparoscopic real-time NIR imaging system in a large animal model. Our novel light source, which is optimized for YC-27, is capable of detecting as little as 12.4 pg/mL of the compound (2.48-pg YC-27 in 200-μL agarose). Finally, in a mouse xenograft model, we demonstrate that the use of real-time NIR imaging can reduce positive surgical margins (PSM).

CONCLUSIONS

These data indicate that a NIR-emitting fluorophore targeted to PSMA may allow improved surgical treatment of human prostate cancer, reduce the rate of PSMs, and alleviate the need for adjuvant radiotherapy postoperatively.

摘要

目的

前列腺特异性膜抗原(PSMA)是一种在恶性前列腺细胞以及许多肿瘤的新生血管中过度表达的表面糖蛋白。近期针对PSMA进行前列腺癌成像的研究依赖于功能适当的低分子量试剂。YC-27是一种低分子量的基于尿素的试剂,能够在体内对PSMA进行近红外(NIR)成像。

实验设计

我们开发并验证了一种腹腔镜成像系统(包括优化的光源LumiNIR),该系统能够在小鼠和猪模型中小前列腺肿瘤异种移植的实时腹腔镜切除手术中,以最小的背景荧光对小肿瘤负荷进行成像。

结果

在小鼠模型中,我们证明了使用实时近红外腹腔镜成像检测并手术切除PSMA阳性异种移植瘤的可行性。然后我们在大型动物模型中验证了腹腔镜实时近红外成像系统的应用。我们针对YC-27优化的新型光源能够检测低至12.4 pg/mL的该化合物(200 μL琼脂糖中含2.48 pg YC-27)。最后,在小鼠异种移植模型中,我们证明了使用实时近红外成像可减少手术切缘阳性(PSM)。

结论

这些数据表明,靶向PSMA的近红外发射荧光团可能会改善人类前列腺癌的手术治疗,降低手术切缘阳性率,并减少术后辅助放疗的需求。

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