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本文引用的文献

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A phosphoramidate-based prostate-specific membrane antigen-targeted SPECT agent.基于膦酰胺的前列腺特异性膜抗原靶向 SPECT 探针。
Prostate. 2012 Jun 1;72(8):904-12. doi: 10.1002/pros.21493.
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Click-functionalized compact quantum dots protected by multidentate-imidazole ligands: conjugation-ready nanotags for living-virus labeling and imaging.点击功能化的多齿咪唑配体保护的紧凑型量子点:用于活病毒标记和成像的即用型纳米标签。
J Am Chem Soc. 2012 May 23;134(20):8388-91. doi: 10.1021/ja302367s. Epub 2012 May 11.
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Strain-promoted copper-free "click" chemistry for 18F radiolabeling of bombesin.用于蛙皮素18F放射性标记的应变促进无铜“点击”化学。
Angew Chem Int Ed Engl. 2011 Nov 18;50(47):11117-20. doi: 10.1002/anie.201105547. Epub 2011 Sep 28.
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A targeted low molecular weight near-infrared fluorescent probe for prostate cancer.一种用于前列腺癌的靶向低分子量近红外荧光探针。
Bioorg Med Chem Lett. 2010 Dec 1;20(23):7124-6. doi: 10.1016/j.bmcl.2010.09.057. Epub 2010 Sep 17.
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Prostate-specific membrane antigen-targeted photodynamic therapy induces rapid cytoskeletal disruption.前列腺特异性膜抗原靶向光动力疗法诱导快速细胞骨架破坏。
Cancer Lett. 2010 Oct 1;296(1):106-12. doi: 10.1016/j.canlet.2010.04.003. Epub 2010 May 8.
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Targeted photodynamic therapy for prostate cancer: inducing apoptosis via activation of the caspase-8/-3 cascade pathway.靶向光动力疗法治疗前列腺癌:通过激活胱天蛋白酶-8/-3 级联途径诱导细胞凋亡。
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Assessment of an 18F-labeled phosphoramidate peptidomimetic as a new prostate-specific membrane antigen-targeted imaging agent for prostate cancer.评估一种18F标记的氨基磷酸肽模拟物作为一种用于前列腺癌的新型前列腺特异性膜抗原靶向成像剂。
J Nucl Med. 2009 Dec;50(12):2042-8. doi: 10.2967/jnumed.109.066589. Epub 2009 Nov 12.
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Drug/dye-loaded, multifunctional iron oxide nanoparticles for combined targeted cancer therapy and dual optical/magnetic resonance imaging.用于联合靶向癌症治疗及双模态光学/磁共振成像的载药/载染料多功能氧化铁纳米颗粒
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PSMA 靶向 SPECT 探针:结合模式对体外性能的影响。

PSMA-targeted SPECT agents: mode of binding effect on in vitro performance.

机构信息

Department of Chemistry, Washington State University, Pullman, Washington 99164-4630, USA.

出版信息

Prostate. 2013 Mar;73(4):355-62. doi: 10.1002/pros.22575. Epub 2012 Aug 21.

DOI:10.1002/pros.22575
PMID:22911263
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4414331/
Abstract

BACKGROUND

The enzyme-biomarker prostate-specific membrane antigen (PSMA) is an active target for imaging and therapeutic applications for prostate cancer. The internalization of PSMA has been shown to vary with inhibitors' mode of binding: irreversible, slowly reversible, and reversible.

METHODS

In the present study, PSMA-targeted clickable derivatives of an irreversible phosphoramidate inhibitor DBCO-PEG(4) -CTT-54 (IC(50) = 1.0 nM) and a slowly reversible phosphate inhibitor, DBCO-PEG(4) -CTT-54.2 (IC(50) = 6.6 nM) were clicked to (99m) Tc(CO)(3) -DPA-azide to assemble a PSMA-targeted SPECT agent. The selectivity, percent uptake, and internalization of these PSMA-targeted SPECT agents were evaluated in PSMA-positive and PSMA-negative cells.

RESULTS

In vitro studies demonstrated that PSMA-targeted SPECT agents exhibited selective cellular uptake in the PSMA-positive LNCaP cells compared to PSMA-negative PC3 cells. More importantly, it was found that (99m) Tc(CO)(3) -DPA-DBCO-PEG(4) -CTT-54 based on an irreversible PSMA inhibitor core, exhibited greater uptake and internalization than (99m) Tc(CO)(3) -DPA-DBCO-PEG(4) -CTT-54.2 constructed from a slowly reversible PSMA inhibitor core.

CONCLUSIONS

We have demonstrated that a PSMA-targeted SPECT agent can be assembled efficiently using copper-less click chemistry. In addition, we demonstrated that mode of binding has an effect on internalization and percent uptake of PSMA-targeted SPECT agents; with the irreversible targeting agent demonstrating superior uptake and internalization in PSMA+ cells. The approach demonstrated in this work now supports a modular approach for the assembly of PSMA-targeted imaging and therapeutic agents.

摘要

背景

酶生物标志物前列腺特异性膜抗原(PSMA)是用于前列腺癌成像和治疗应用的活跃靶点。已经表明,PSMA 的内化随抑制剂结合模式的不同而变化:不可逆、缓慢可逆和可逆。

方法

在本研究中,将不可逆膦酰胺抑制剂 DBCO-PEG(4)-CTT-54(IC(50)=1.0 nM)和缓慢可逆磷酸酯抑制剂 DBCO-PEG(4)-CTT-54.2(IC(50)=6.6 nM)的 PSMA 靶向点击衍生化合物点击到 (99m)Tc(CO)(3)-DPA-叠氮化物上,以组装 PSMA 靶向单光子发射计算机断层扫描(SPECT)剂。在 PSMA 阳性和 PSMA 阴性细胞中评估了这些 PSMA 靶向 SPECT 剂的选择性、摄取百分比和内化。

结果

体外研究表明,与 PSMA 阴性 PC3 细胞相比,PSMA 阳性 LNCaP 细胞中 PSMA 靶向 SPECT 剂表现出选择性细胞摄取。更重要的是,发现基于不可逆 PSMA 抑制剂核心的 (99m)Tc(CO)(3)-DPA-DBCO-PEG(4)-CTT-54 比基于缓慢可逆 PSMA 抑制剂核心的 (99m)Tc(CO)(3)-DPA-DBCO-PEG(4)-CTT-54.2 具有更高的摄取和内化。

结论

我们已经证明可以使用无铜点击化学高效组装 PSMA 靶向 SPECT 剂。此外,我们证明结合模式对 PSMA 靶向 SPECT 剂的内化和摄取百分比有影响;不可逆靶向剂在 PSMA+细胞中表现出更高的摄取和内化。这项工作中展示的方法现在支持用于组装 PSMA 靶向成像和治疗剂的模块化方法。