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通过动态光学成像量化αvβ3整合素靶向光学造影剂的分子特异性。

Quantifying molecular specificity of alphavbeta3 integrin-targeted optical contrast agents with dynamic optical imaging.

作者信息

Gurfinkel Michael, Ke Shi, Wang Wei, Li Chun, Sevick-Muraca Eva M

机构信息

Texas A&M University, Photon Migration Laboratories, College Station, Texas 77843-3012, USA.

出版信息

J Biomed Opt. 2005 May-Jun;10(3):034019. doi: 10.1117/1.1924696.

Abstract

Dynamic fluorescence images were obtained from a subcutaneous human Kaposi's sarcoma tumor (KS1767) model immediately following the intravenous injection of an integrin-targeting cyanine dye conjugate, Cy5.5-c(KRGDf). The fluorescence images, acquired via an intensified charge-coupled device detection system, were used in conjunction with a pharmacokinetic (PK) model to determine kinetic properties of target binding in the presence and absence of a competitive ligand, free c(KRGDf). The results indicate that the conjugate dye behaves similarly in normal tissue to the free Cy5.5 dye while it possesses increased uptake in tumor tissue. The change in pharmacokinetic parameters obtained from dynamic imaging of Cy5.5-c(KRGDf) after administration of c(KRGDf) as a competitive ligand to the integrin receptor suggests that (i) the increased uptake of Cy5.5-c(KRGDf) is molecularly specific and that (ii) receptor turnover occurs within 24 h. In addition, PK analysis enables quantification of an in vivo c(KRGDf) binding constant attributable to integrin binding. In vivo pharmacokinetic analysis based on rapid and dynamic optical imaging may be potentially useful for evaluating the presence and turnover rate of disease markers that are potential targets of molecular medicine.

摘要

在静脉注射整合素靶向花菁染料偶联物Cy5.5-c(KRGDf)后,立即从皮下人卡波西肉瘤肿瘤(KS1767)模型获取动态荧光图像。通过增强型电荷耦合器件检测系统采集的荧光图像,与药代动力学(PK)模型结合使用,以确定在存在和不存在竞争性配体游离c(KRGDf)的情况下靶点结合的动力学特性。结果表明,偶联染料在正常组织中的行为与游离Cy5.5染料相似,而在肿瘤组织中的摄取增加。在给整合素受体施用c(KRGDf)作为竞争性配体后,从Cy5.5-c(KRGDf)的动态成像获得的药代动力学参数变化表明:(i) Cy5.5-c(KRGDf)摄取增加具有分子特异性;(ii) 受体周转在24小时内发生。此外,PK分析能够量化归因于整合素结合的体内c(KRGDf)结合常数。基于快速动态光学成像的体内药代动力学分析可能对评估作为分子医学潜在靶点的疾病标志物的存在和周转率具有潜在用途。

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