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用于99mTc靶向NTS1受体肿瘤显像的稳定N4修饰神经降压素的研究

Toward stable N4-modified neurotensins for NTS1-receptor-targeted tumor imaging with 99mTc.

作者信息

Nock Berthold A, Nikolopoulou Anastasia, Reubi Jean-Claude, Maes Veronique, Conrath Peter, Tourwé Dirk, Maina Theodosia

机构信息

Institute of Radioisotopes - Radiodiagnostic Products, National Center for Scientific Research Demokritos, 15310 Athens, Greece.

出版信息

J Med Chem. 2006 Jul 27;49(15):4767-76. doi: 10.1021/jm060415g.

Abstract

A series of Gly-neurotensin(8-13) analogues modified at the N-terminus by acyclic tetraamines (Demotensin 1-4) were obtained by solid-phase peptide synthesis techniques. Strategic replacement of amino acids and/or reduction of sensitive peptide bonds were performed to enhance conjugate resistance against proteolytic enzymes. During 99mTc-labeling, single species radiopeptides, [99mTc]Demotensin 1-4, were easily obtained in high yields and typical specific activities of 1 Ci/micromol. Peptide conjugates displayed a high affinity binding to the human neurotensin subtype 1 receptor (NTS1-R) expressed in colon adenocarcinoma HT-29 or WiDr cells and/or in human tumor sections. [99mTc]Demotensin 1-4 internalized very rapidly in HT-29 or WiDr cells by a NTS1-R-mediated process. [99mTc]Demotensin 3 and 4, which remained stable during 1 h incubation in murine plasma, were selectively studied in nude mice bearing human HT-29 and WiDr xenografts. After injection, [99mTc]Demotensin 3 and 4 effectively and specifically localized in the experimental tumors and were rapidly excreted via the kidneys into the urine, exhibiting overall biodistribution patterns favorable for NTS1-R-targeted tumor imaging in man.

摘要

通过固相肽合成技术获得了一系列在N端被无环四胺修饰的甘氨-神经降压素(8 - 13)类似物(去甲降压素1 - 4)。通过策略性地替换氨基酸和/或减少敏感肽键来增强缀合物对蛋白水解酶的抗性。在99mTc标记过程中,很容易以高产率获得单一物种放射性肽[99mTc]去甲降压素1 - 4,其典型比活为1 Ci/μmol。肽缀合物对在结肠腺癌HT - 29或WiDr细胞和/或人肿瘤切片中表达的人神经降压素1型受体(NTS1 - R)显示出高亲和力结合。[99mTc]去甲降压素1 - 4通过NTS1 - R介导的过程在HT - 29或WiDr细胞中非常迅速地内化。在携带人HT - 29和WiDr异种移植瘤的裸鼠中对在鼠血浆中孵育1小时仍保持稳定的[99mTc]去甲降压素3和4进行了选择性研究。注射后,[99mTc]去甲降压素3和4有效且特异地定位在实验肿瘤中,并通过肾脏迅速排泄到尿液中,显示出有利于人类NTS1 - R靶向肿瘤成像的总体生物分布模式。

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