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Pharmacokinetic and Biodistribution Assessment of a Near Infrared-Labeled PSMA-Specific Small Molecule in Tumor-Bearing Mice

机译:近红外标记的PSMA特异性小分子在荷瘤小鼠中的药代动力学和生物分布评估

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摘要

Prostate cancer is the most frequently diagnosed cancer in men and often requires surgery. Use of near infrared (NIR) technologies to perform image-guided surgery may improve accurate delineation of tumor margins. To facilitate preclinical testing of such outcomes, here we developed and characterized a PSMA-targeted small molecule, YC-27. IRDye 800CW was conjugated to YC-27 or an anti-PSMA antibody used for reference. Human 22Rv1, PC3M-LN4, and/or LNCaP prostate tumor cells were exposed to the labeled compounds. In vivo targeting and clearance properties were determined in tumor-bearing mice. Organs and tumors were excised and imaged to assess probe localization. YC-27 exhibited a dose dependent increase in signal upon binding. Binding specificity and internalization were visualized by microscopy. In vitro and in vivo blocking studies confirmed YC-27 specificity. In vivo, YC-27 showed good tumor delineation and tissue contrast at doses as low as 0.25 nmole. YC-27 was cleared via the kidneys but bound the proximal tubules of the renal cortex and epididymis. Since PSMA is also broadly expressed on the neovasculature of most tumors, we expect YC-27 will have clinical utility for image-guided surgery and tumor resections.
机译:前列腺癌是男性中最常被诊断出的癌症,通常需要手术治疗。使用近红外(NIR)技术执行图像引导的手术可能会改善肿瘤边缘的精确描绘。为了促进此类结果的临床前测试,在这里我们开发并表征了靶向PSMA的小分子YC-27。将IRDye 800CW与YC-27或用于参考的抗PSMA抗体偶联。将人22Rv1,PC3M-LN4和/或LNCaP前列腺肿瘤细胞暴露于标记的化合物。在荷瘤小鼠中确定体内靶向和清除特性。切除器官和肿瘤并成像以评估探针定位。 YC-27在结合后显示出剂量依赖性的信号增加。结合特异性和内在化通过显微镜观察。体外和体内阻断研究证实了YC-27的特异性。在体内,YC-27在低至0.25μmol的剂量下显示出良好的肿瘤轮廓和组织对比。 YC-27通过肾脏清除,但束缚了肾皮质和附睾的近端小管。由于PSMA在大多数肿瘤的新血管系统中也广泛表达,因此我们希望YC-27在图像引导手术和肿瘤切除方面具有临床应用价值。

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