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光谱特征良好的 RGD 光学探针是寿命门控肿瘤成像的前提。

Spectroscopically well-characterized RGD optical probe as a prerequisite for lifetime-gated tumor imaging.

机构信息

Department of Molecular Biology of Neuronal Signals, Max-Planck-Institute for Experimental Medicine, Göttingen, Germany.

出版信息

Mol Imaging. 2011 Dec;10(6):469-80.

PMID:22201538
Abstract

Labeling of RGD peptides with near-infrared fluorophores yields optical probes for noninvasive imaging of tumors overexpressing ανβ3 integrins. An important prerequisite for optimum detection sensitivity in vivo is strongly absorbing and highly emissive probes with a known fluorescence lifetime. The RGD-Cy5.5 optical probe was derived by coupling Cy5.5 to a cyclic arginine-glycine-aspartic acid-d-phenylalanine-lysine (RGDfK) peptide via an aminohexanoic acid spacer. Spectroscopic properties of the probe were studied in different matrices in comparison to Cy5.5. For in vivo imaging, human glioblastoma cells were subcutaneously implanted into nude mice, and in vivo fluorescence intensity and lifetime were measured. The fluorescence quantum yield and lifetime of Cy5.5 were found to be barely affected on RGD conjugation but dramatically changed in the presence of proteins. By time domain fluorescence imaging, we demonstrated specific binding of RGD-Cy5.5 to glioblastoma xenografts in nude mice. Discrimination of unspecific fluorescence by lifetime-gated analysis further enhanced the detection sensitivity of RGD-Cy5.5-derived signals. We characterized RGD-Cy5.5 as a strongly emissive and stable probe adequate for selective targeting of ανβ3 integrins. The specificity and thus the overall detection sensitivity in vivo were optimized with lifetime gating, based on the previous determination of the probes fluorescence lifetime under application-relevant conditions.

摘要

通过将近红外荧光团标记 RGD 肽,得到了用于过表达 ανβ3 整合素的肿瘤的非侵入性成像的光学探针。在体内获得最佳检测灵敏度的一个重要前提是具有已知荧光寿命的强吸收和高发射探针。RGD-Cy5.5 光学探针是通过将 Cy5.5 通过氨己酸间隔臂偶联到环状精氨酸-甘氨酸-天冬氨酸-d-苯丙氨酸-赖氨酸(RGDfK)肽上来衍生的。与 Cy5.5 相比,在不同基质中研究了探针的光谱性质。对于体内成像,将人胶质母细胞瘤细胞皮下植入裸鼠中,并测量体内荧光强度和寿命。发现 Cy5.5 的荧光量子产率和寿命在 RGD 缀合后几乎没有受到影响,但在存在蛋白质的情况下会发生剧烈变化。通过时域荧光成像,我们证明了 RGD-Cy5.5 特异性结合裸鼠中的胶质母细胞瘤异种移植物。通过寿命门控分析对非特异性荧光进行区分,进一步提高了 RGD-Cy5.5 衍生信号的检测灵敏度。我们将 RGD-Cy5.5 表征为一种强发射和稳定的探针,适用于选择性靶向 ανβ3 整合素。基于先前在应用相关条件下确定的探针荧光寿命,通过寿命门控,优化了探针的特异性和因此体内的整体检测灵敏度。

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