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首页> 外文期刊>Contrast media & molecular imaging >Thyroid Cancer Detection by Ultrasound Molecular Imaging with SHP2-Targeted Perfluorocarbon Nanoparticles
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Thyroid Cancer Detection by Ultrasound Molecular Imaging with SHP2-Targeted Perfluorocarbon Nanoparticles

机译:通过SHP2靶向全氟化碳纳米粒子的超声分子成像检测甲状腺癌。

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Background. Contrast-enhanced ultrasound imaging has been widely used in the ultrasound diagnosis of a variety of tumours with high diagnostic accuracy, especially in patients with hepatic carcinoma, while its application is rarely reported in thyroid cancer. The currently used ultrasound contrast agents, microbubbles, cannot be targeted to molecular markers expressed in tumour cells due to their big size, leading to a big challenge for ultrasound molecular imaging. Phase-changeable perfluorocarbon nanoparticles may resolve the penetrability limitation of microbubbles and serve as a promising probe for ultrasound molecular imaging. Methods. 65 thyroid tumour samples and 40 normal samples adjacent to thyroid cancers were determined for SHP2 expression by IHC. SHP2-targeted PLGA nanoparticles (NPs-SHP2) encapsulating perfluoropentane (PFP) were prepared with PLGA-PEG as a shell material, and their specific target-binding ability was assessed in vitro and in vivo, and the effect on the enhancement of ultrasonic imaging induced by LIFU was studied in vivo. Results. In the present study, we verified that tumour overexpression of SHP2 and other protein tyrosine phosphatases regulated several cellular processes and contributed to tumorigenesis, which could be introduced to ultrasound molecular imaging for differentiating normal from malignant thyroid diagnostic nodes. The IHC test showed remarkably high expression of SHP2 in human thyroid carcinoma specimens. In thyroid tumour xenografts in mice, the imaging signal was significantly enhanced by SHP2-targeted nanoparticles after LIFU induction. Conclusion. This study provides a basis for preclinical exploration of ultrasound molecular imaging with NPs-SHP2 for clinical thyroid nodule detection to enhance diagnostic accuracy.
机译:背景。造影增强超声成像已被广泛用于超声诊断各种肿瘤中,具有很高的诊断准确性,尤其是在肝癌患者中,而在甲状腺癌中很少报道其应用。当前使用的超声造影剂微泡由于其大尺寸而不能靶向于在肿瘤细胞中表达的分子标记,从而导致超声分子成像的巨大挑战。相变全氟化碳纳米粒子可以解决微气泡的渗透性限制,并可以作为超声分子成像的有前途的探针。方法。通过IHC测定了65份甲状腺肿瘤样品和40份与甲状腺癌相邻的正常样品的SHP2表达。以PLGA-PEG为壳材料制备包裹全氟戊烷(SFP2)的SHP2靶向PLGA纳米颗粒(NPs-SHP2),并在体内和体外评估其特异性靶标结合能力,以及对超声成像增强的影响在体内研究了LIFU诱导的凋亡。结果。在本研究中,我们验证了SHP2和其他蛋白酪氨酸磷酸酶的肿瘤过度表达调节了几个细胞过程并促进了肿瘤的发生,可将其引入超声分子成像中以区分正常与恶性甲状腺诊断结节。 IHC测试显示SHP2在人甲状腺癌标本中的高表达。在小鼠的甲状腺肿瘤异种移植物中,LIFU诱导后,SHP2靶向纳米颗粒显着增强了成像信号。结论。这项研究为临床分子探查NPs-SHP2进行超声分子成像以临床诊断甲状腺结节以提高诊断准确性提供了基础。

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