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用于前列腺特异性膜抗原体内成像的高亲和力近红外荧光小分子造影剂。

High-affinity near-infrared fluorescent small-molecule contrast agents for in vivo imaging of prostate-specific membrane antigen.

作者信息

Humblet Valerie, Lapidus Rena, Williams Larry R, Tsukamoto Takashi, Rojas Camilo, Majer Pavel, Hin Bunda, Ohnishi Shunsuke, De Grand Alec M, Zaheer Atif, Renze Jürgen T, Nakayama Akira, Slusher Barbara S, Frangioni John V

机构信息

Beth Israel Deaconess Medical Center, Boston, MA 02215, USA.

出版信息

Mol Imaging. 2005 Oct-Dec;4(4):448-62. doi: 10.2310/7290.2005.05163.

Abstract

Surgical resection remains a definitive treatment for prostate cancer. Yet, prostate cancer surgery is performed without image guidance for tumor margin, extension beyond the capsule and lymph node positivity, and without verification of other occult metastases in the surgical field. Recently, several imaging systems have been described that exploit near-infrared (NIR) fluorescent light for sensitive, real-time detection of disease pathology intraoperatively. In this study, we describe a high-affinity (9 nM), single nucleophile-containing, small molecule specific for the active site of the enzyme PSMA. We demonstrate production of a tetra-sulfonated heptamethine indocyanine NIR fluorescent derivative of this molecule using a high-yield LC/MS purification strategy. Interestingly, NIR fluorophore conjugation improves affinity over 20-fold, and we provide mechanistic insight into this observation. We describe the preparative production of enzymatically active PSMA using a baculovirus expression system and an adenovirus that co-expresses PSMA and GFP. We demonstrate sensitive and specific in vitro imaging of endogenous and ectopically expressed PSMA in human cells and in vivo imaging of xenograft tumors. We also discuss chemical strategies for improving performance even further. Taken together, this study describes nearly complete preclinical development of an optically based small-molecule contrast agent for image-guided surgery.

摘要

手术切除仍然是前列腺癌的一种确定性治疗方法。然而,前列腺癌手术在没有图像引导的情况下进行,无法确定肿瘤边缘、包膜外扩展和淋巴结阳性情况,也无法在手术视野中验证其他隐匿性转移。最近,已经描述了几种利用近红外(NIR)荧光进行术中疾病病理敏感、实时检测的成像系统。在本研究中,我们描述了一种对酶PSMA活性位点具有高亲和力(9 nM)、含单亲核试剂的小分子。我们展示了使用高产率液相色谱/质谱纯化策略制备该分子的四磺化七甲川吲哚菁NIR荧光衍生物。有趣的是,NIR荧光团共轭使亲和力提高了20倍以上,我们对这一观察结果提供了机理见解。我们描述了使用杆状病毒表达系统和共表达PSMA和GFP的腺病毒制备具有酶活性的PSMA。我们展示了在人细胞中对内源性和异位表达的PSMA进行灵敏且特异的体外成像以及对异种移植肿瘤进行体内成像。我们还讨论了进一步提高性能的化学策略。综上所述,本研究描述了一种用于图像引导手术的基于光学的小分子造影剂几乎完整的临床前开发。

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