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首页> 外文期刊>Molecular imaging and biology: MIB : the official publication of the Academy of Molecular Imaging >Synthesis and Biological Evaluation of Cyclic [Tc-99m]-HYNIC-CGPRPPC as a Fibrin-Binding Peptide for Molecular Imaging of Thrombosis and Its Comparison with [Tc-99m]-HYNIC-GPRPP
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Synthesis and Biological Evaluation of Cyclic [Tc-99m]-HYNIC-CGPRPPC as a Fibrin-Binding Peptide for Molecular Imaging of Thrombosis and Its Comparison with [Tc-99m]-HYNIC-GPRPP

机译:循环[TC-99M] -HYNIC-CGPRPPC作为纤维蛋白结合肽的合成及生物学评价,用于血栓形成的分子成像及其与[TC-99M] -HYNIC-GPRPP的比较

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摘要

Many patients worldwide suffer from cardiovascular diseases for which an underlying factor is thrombosis. Devising a molecular imaging technique for early detection of thrombosis in a clinical setting is highly recommended. Because fibrin is a major constituent of clots and is present in all types of thrombi but absent in circulation, it is a highly specific and sensitive target for molecular imaging of thrombi. It is assumed that cyclization of peptides will improve the receptor binding affinity and stability of the peptide. In the present study, we have developed linear and cyclic fibrin-binding peptides for thrombus imaging and compared their biological properties.
机译:许多全世界患者患有心血管疾病,其中潜在的因素是血栓形成。 强烈推荐使用用于早期检测临床环境中血栓形成的分子成像技术。 因为纤维蛋白是凝块的主要成分,并且存在于各种类型的血栓中,但在循环中缺席,它是血栓分子成像的高度特异性和敏感的靶标。 假设肽的环化将改善肽的受体结合亲和力和稳定性。 在本研究中,我们开发了用于血栓成像的线性和环纤维蛋白结合肽,并比较其生物学性质。

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