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用于荧光引导肿瘤切除和光动力治疗的氨基乙酰丙酸光学葡萄糖类似物。

Optical glucose analogs of aminolevulinic acid for fluorescence-guided tumor resection and photodynamic therapy.

作者信息

Moriyama Eduardo H, Cao Weiguo, Liu Tracy W, Wang Han Lin, Kim Peter D, Chen Juan, Zheng Gang, Wilson Brian C

机构信息

Ontario Cancer Institute, University Heath Network, Toronto, Ontario, Canada,

出版信息

Mol Imaging Biol. 2014 Aug;16(4):495-503. doi: 10.1007/s11307-013-0687-y.

Abstract

PURPOSE

We have developed and tested a novel conjugation of the clinically used prodrug aminolevulinic acid with 2-deoxyglucosamine as a novel probe (ALA-2DG) for fluorescence imaging and photodynamic therapy.

PROCEDURES

ALA-2DG was successfully synthesized, and the mechanisms of probe uptake, PpIX synthesis, and photodynamic therapy efficacy were evaluated in vitro and in vivo.

RESULTS

ALA-2DG led to PpIX synthesis in tumor cells in vitro and in tumor in vivo. Competitive and inhibitory assays in vitro showed a reduction of this PpIX synthesis that was not observed when cells were incubated with ALA itself, indicating that intracellular uptake of ALA-2DG occurs by GLUT-mediated active transport. Initial photodynamic therapy studies confirmed the efficacy of ALA-2DG as a photodynamic sensitizer.

CONCLUSIONS

The in vitro assays suggest that ALA-2DG is taken up by cells via glucose transporters. Initial studies in oral cancer demonstrated the applicability of ALA-2DG for in vivo imaging and its potential as an alternative to ALA-PpIX-based fluorescence diagnostics and photodynamic therapy, providing higher tumor specificity.

摘要

目的

我们研发并测试了一种临床上使用的前药氨基乙酰丙酸与2-脱氧葡萄糖胺的新型缀合物,作为一种用于荧光成像和光动力疗法的新型探针(ALA-2DG)。

程序

成功合成了ALA-2DG,并在体外和体内评估了探针摄取、原卟啉IX(PpIX)合成及光动力疗法疗效的机制。

结果

ALA-2DG在体外肿瘤细胞和体内肿瘤中均能导致PpIX合成。体外竞争和抑制试验表明,这种PpIX合成减少,而细胞与ALA本身孵育时未观察到这种情况,这表明ALA-2DG的细胞内摄取是通过葡萄糖转运蛋白介导的主动转运发生的。初步的光动力疗法研究证实了ALA-2DG作为光动力敏化剂的疗效。

结论

体外试验表明,ALA-2DG通过葡萄糖转运蛋白被细胞摄取。口腔癌的初步研究证明了ALA-2DG在体内成像中的适用性及其作为基于ALA-PpIX的荧光诊断和光动力疗法替代方案的潜力,具有更高的肿瘤特异性。

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