一种新的99mTc放射性标记环肽作为CXCR4受体有前途的分子显像剂的设计:分子对接、合成、放射性标记和生物学评价。

IF 1.5 4区 医学 Q3 PHARMACOLOGY & PHARMACY
Leila Hassanzadeh, Mostafa Erfani, Safura Jokar, Marjan Shariatpanahi
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引用次数: 0

摘要

简介:C-X-C趋化因子受体4型(CXCR4)在不同类型和阶段的癌症疾病中通常过度表达或过度活化。因此,它被认为是原发性肿瘤和转移的成像和早期检测的一个有前途的靶点。在本研究中,以亲本LY251029肽为基础,设计了一种新的99mTc放射性标记的环肽,即99mTc环[D-Phe-D-Tyr-Lys(HYNIC)-D-Arg-2-Nal-Gly-Lys(iPr)],作为表达CXCR4的肿瘤的潜在体内显像剂。方法:采用Fmoc固相肽合成法成功制备了放射性配体,并对其进行了生物学评价。分子对接结果显示,CXCR4受体(PDB代码:3OE0)的结合口袋中的环[D-Phe-D-Tyr-Lys(HYNIC)-D-Arg-2-Nal-Gly-Lys(iPr)]具有高亲和力(结合能-9.7kcal/mol)和有效相互作用。结果:采用反相高效液相色谱法(RP-HPLC)和质谱法对合成的肽及其纯度进行了测定。在人血清中具有高稳定性(95%,n=3),在B16-F10细胞系中具有良好的亲和力(Kd=28.70±13.56nM和Bmax=1.896±0.123fmol/mg蛋白)。小鼠的生物分布评估结果和平面图像解释都显示出放射性示踪剂对CXCR4受体的高亲和力和选择性。结论:因此,研究结果表明,该设计的放射性配体可作为高增殖CXCR4受体肿瘤的潜在SPECT显像剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Design of a New 99mTc-radiolabeled Cyclo-peptide as Promising Molecular Imaging Agent of CXCR4 Receptor: Molecular Docking, Synthesis, Radiolabeling, and Biological Evaluation.

Introduction: C-X-C Chemokine receptor type 4 (CXCR4) is often overexpressed or overactivated in different types and stages of cancer disease. Therefore, it is considered a promising target for imaging and early detection of primary tumors and metastasis. In the present research, a new cyclo-peptide radiolabelled with 99mTc, 99mTc-Cyclo [D-Phe-D-Tyr-Lys (HYNIC)- D-Arg-2-Nal-Gly-Lys(iPr)], was designed based on the parental LY251029 peptide, as a potential in vivo imaging agent of CXCR4-expressing tumors.

Methods: The radioligand was successfully prepared using the method of Fmoc solid-phase peptide synthesis and was evaluated in biological assessment. Molecular docking findings revealed high affinity (binding energy of -9.7 kcal/mol) and effective interaction of Cyclo [D-Phe- D-Tyr-Lys (HYNIC)-D-Arg-2-Nal-Gly-Lys(iPr)] in the binding pocket of CXCR4 receptor (PDB code: 3OE0) as well.

Result: The synthesized peptide and its purity were assessed by both reversed-phase high-performance liquid chromatography (RP-HPLC) and mass spectroscopy. High stability (95%, n = 3) in human serum and favorable affinity (Kd = 28.70 ± 13.56 nM and Bmax = 1.896 ± 0.123 fmol/mg protein) in the B16-F10 cell line resulted. Biodistribution evaluation findings and planar image interpretation of mice both showed high affinity and selectivity of the radiotracer to the CXCR4 receptors.

Conclusion: Therefore, the findings indicate this designed radioligand could be used as a potential SPECT imaging agent in highly proliferated CXCR4 receptor tumors.

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来源期刊
Current radiopharmaceuticals
Current radiopharmaceuticals PHARMACOLOGY & PHARMACY-
CiteScore
3.20
自引率
4.30%
发文量
43
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