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基于LAT1靶向递送由M(III)金属离子衍生的蛋氨酸基成像探针,用于使用分子成像模式对增殖性肿瘤进行早期诊断。

LAT1 targeted delivery of methionine based imaging probe derived from M(III) metal ions for early diagnosis of proliferating tumours using molecular imaging modalities.

作者信息

Hazari Puja Panwar, Prakash Surbhi, Meena Virendra K, Jaswal Ambika, Khurana Harleen, Mishra Surabhi Kirti, Bhonsle Hemanth Kumar, Singh Lokendra, Mishra Anil K

机构信息

Scientist G, Additional Director, Brig. S. K. Mazumdar Road, Delhi-110054, India.

出版信息

Curr Cancer Drug Targets. 2015;14(9):817-31. doi: 10.2174/1568009614666141020102337.

DOI:10.2174/1568009614666141020102337
PMID:25329672
Abstract

We investigated the potential of DTPA-bis(Methionine), a target specific amino acid based probe for detection of L-type amino acid transporters (LAT1) known to over express in proliferating tumours using multimodality imaging. The ligand, DTPA-bis(Met) was readily converted to lanthanide complexes and was found capable of targeting cancer cells using multimodality imaging. DTPA-bis(Met) complexes were synthesized and characterized by mass spectroscopy. MR longitudinal relaxivity, r₁ = 4.067 ± 0.31 mM⁻¹s⁻¹ and transverse relaxivity, r₂ = 8.61 ± 0.07 mM⁻¹s⁻¹ of Gd(III)-DTPA-bis(Met) were observed at pH 7.4 at 7 T. Bright, localized fluorescence of Eu(III)-DTPA-bis(Met) was observed with standard microscopy and displacement studies indicated ligand functionality. K(D) value determined for Eu(III)-DTPA-bis(Met) on U-87 MG cells was found to be 17.3 pM and showed appreciable fluorescence within the cells. Radio HPLC showed a radiochemical purity more than 95% (specific activity = 400-500 MBq/μmol, labelling efficiency 78 %) for ⁶⁸Ga(III)-DTPA-bis(Met). Pre-treatment of xenografted U-87 MG athymic mice with ⁶⁸Ga(III)-DTPA-bis(Met) following unlabelled L-methionine administration reduced tumour uptake by 10-folds in Micro PET. These data support the specific binding of ⁶⁸Ga(III)-DTPA-bis(Met) to the LAT1 transporter. To summarize, this agent possesses high stability in biological environment and exhibits effective interaction with its LAT1 transporters giving high accumulation in tumour area, excellent tumour/non-tumour ratio and low non-specific retention in vivo.

摘要

我们使用多模态成像技术研究了二乙三胺五乙酸双(甲硫氨酸)(DTPA-bis(Methionine))的潜力,它是一种基于靶标特异性氨基酸的探针,用于检测已知在增殖肿瘤中过表达的L型氨基酸转运体(LAT1)。配体DTPA-双(甲硫氨酸)(DTPA-bis(Met))很容易转化为镧系元素配合物,并且发现能够使用多模态成像技术靶向癌细胞。合成了DTPA-双(甲硫氨酸)配合物并通过质谱进行了表征。在7T、pH 7.4条件下,观察到钆(III)-DTPA-双(甲硫氨酸)(Gd(III)-DTPA-bis(Met))的磁共振纵向弛豫率r₁ = 4.067 ± 0.31 mM⁻¹s⁻¹和横向弛豫率r₂ = 8.61 ± 0.07 mM⁻¹s⁻¹。用标准显微镜观察到铕(III)-DTPA-双(甲硫氨酸)(Eu(III)-DTPA-bis(Met))发出明亮的局部荧光,置换研究表明配体具有功能性。发现Eu(III)-DTPA-双(甲硫氨酸)对U-87 MG细胞的解离常数K(D)值为17.3 pM,并且在细胞内显示出明显的荧光。放射性高效液相色谱显示,⁶⁸镓(III)-DTPA-双(甲硫氨酸)(⁶⁸Ga(III)-DTPA-bis(Met))的放射化学纯度超过95%(比活度 = 400 - 500 MBq/μmol,标记效率78%)。在未标记的L-甲硫氨酸给药后,用⁶⁸Ga(III)-DTPA-bis(Met)对异种移植的U-87 MG无胸腺小鼠进行预处理,在微型正电子发射断层显像(Micro PET)中肿瘤摄取减少了10倍。这些数据支持⁶⁸Ga(III)-DTPA-bis(Met)与LAT1转运体的特异性结合。总之,该试剂在生物环境中具有高稳定性,并且与其LAT1转运体表现出有效的相互作用,在肿瘤区域具有高积累、出色的肿瘤/非肿瘤比值以及体内低非特异性滞留。

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