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基于 DOTA-金属的 PSMA 靶向成像剂的模块化合成用于前列腺癌的 MRI 和 PET 成像。

Modular Synthesis of DOTA-Metal-Based PSMA-Targeted Imaging Agents for MRI and PET of Prostate Cancer.

机构信息

School of Chemistry and Materials Science, Rochester Institute of Technology, Rochester, NY, 14623, USA.

Golisano School of Life Sciences, Rochester Institute of Technology, Rochester, NY, 14623, USA.

出版信息

Chemistry. 2019 Nov 4;25(61):13848-13854. doi: 10.1002/chem.201903390. Epub 2019 Sep 24.

Abstract

A practical, convergent synthesis of prostate-specific membrane antigen (PSMA) targeted imaging agents for MRI, PET, and SPECT of prostate cancer has been developed. In this approach, metals chelated to 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (DOTA) were placed on the side chains of lysine early in the synthesis to form imaging modules. These are coupled to targeting modules, in this case consisting of the PSMA-binding urea DCL, bonded to an activated linker. The modular approach to targeted molecular imaging agents (TMIAs) offers distinct advantages. By chelating the MRI contrast metal Gd early, it doubles as a protecting group for DOTA. Standard coupling and deprotection steps may be utilized to assemble the modules into peptides, and the need for tri-tert-butyl protection of DOTA requiring removal by strong acid is averted. This enables mild conjugation of the imaging module to a wide variety of targeting agents in the final step. It was further discovered that two labile metals, La or Ce , can be used as placeholders in DOTA during the synthesis, then transmetalated in mild acid by Cu , Ga , In , and Y , metals used in PET/SPECT. This enables the efficient synthesis of nonradioactive analogues of targeted molecular imaging agents that may be transported or stored until needed. A simple and mild two-step transmetalation, involving de-metalation in dilute acid, followed by rapid chelation of the radioactive metal, may be conveniently performed later at the clinic to provide the TMIAs for PET or SPECT.

摘要

已经开发出一种用于 MRI、PET 和 SPECT 前列腺癌成像的前列腺特异性膜抗原(PSMA)靶向成像剂的实用、会聚合成方法。在这种方法中,金属螯合到 1,4,7,10-四氮杂环十二烷-1,4,7,10-四乙酸(DOTA)的侧链上,在早期合成中形成成像模块。这些成像模块与靶向模块结合,在这种情况下,靶向模块由与活化的连接子结合的 PSMA 结合脲 DCL 组成。靶向分子成像剂(TMIAs)的模块化方法具有明显的优势。通过早期螯合 MRI 对比金属 Gd,它还可以作为 DOTA 的保护基团。可以利用标准的偶联和脱保护步骤将模块组装成肽,并且避免了需要用强酸去除三-叔丁基保护的 DOTA 的需要。这使得可以在最后一步温和地将成像模块与各种靶向剂偶联。进一步发现,两种不稳定金属 La 或 Ce 可以在 DOTA 合成期间用作 DOTA 中的占位剂,然后通过 Cu、Ga、In 和 Y(用于 PET/SPECT 的金属)在弱酸中进行转金属化。这可以有效地合成靶向分子成像剂的非放射性类似物,这些类似物可以在需要时进行运输或储存。可以在以后的临床中方便地进行简单温和的两步转金属化,涉及在稀酸中脱金属化,然后快速螯合放射性金属,以便为 PET 或 SPECT 提供 TMIAs。

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