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首页> 外文期刊>Journal of magnetic resonance imaging: JMRI >An ultrasound‐responsive dual‐modal US/T 1 1 ‐MRI contrast agent for potential diagnosis of prostate cancer
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An ultrasound‐responsive dual‐modal US/T 1 1 ‐MRI contrast agent for potential diagnosis of prostate cancer

机译:用于潜在诊断前列腺癌的超声响应双型US / T 1 1 -MRI造影剂

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Background Interest in an ultrasound‐mediated delivery system for effective T 1 ‐MRI of prostate cancer without adverse effects has steadily increased. Purpose To develop an ultrasound‐responsive dual‐modal ultrasound (US)/T 1 ‐MRI contrast agent for efficient diagnosis of prostate cancer cells overexpressing prostate‐specific membrane antigen (PSMA) and assess their potential. Study Type In vitro. Subjects Two prostate cancer cell lines. Field Strength/Sequence Each study group underwent 3.0T MRI under a TR 400 msec, TE 10 msec, a 240 × 240 matrix, a flip angle 90°, a slice thickness 3?mm, NSA with 4, bandwidth 115?Hz/pixel, and an FOV of 120 × 120?mm. Assessment Microscopes, quantitative and qualitative analyzing instruments, and clinical devices were used for assessing this novel contrast agent and its diagnosis effects. Statistical Tests We used linear regression analyses to determine the longitudinal relaxivity ( r 1 ) values of our US/T 1 ‐MRI contrast agent and gadobutrol. Results Microbubble+Fe 3+ melanin nanoparticle+peptides (MB+Fe 3+ MNPPs) had a good US contrast effect, like a commercial US agent. The differences of US intensities between them was below 5%. The r 1 values of MB+Fe 3+ MNPPs and gadobutrol were 4.5 and 3.7 s ‐1 /mM, respectively. More than hundreds of Fe 3+ MNPPs were located in prostate cancer cells treated with MB+Fe 3+ MNPPs and US stimulus, but the number of Fe 3+ MNPPs was below dozens in the other prostate cancer cells expressing less PSMA. The former cells with MB+Fe 3+ MNPPs and US stimulus only showed the highest T 1 ‐MRI signal because of synergy effects of the peptides targeting the cells and US stimulus for delivery of Fe 3+ MNPPs to the cells. No cytotoxicity of MB+Fe 3+ MNPPs was confirmed by using a WST assay. Viability of the cells with the complexes was above 90%. Data Conclusion We synthesized MB+Fe 3+ MNPPs as a potential US/T 1 ‐MRI contrast agent. This complex was applicable for diagnosing desired prostate cancer cells. Level of Evidence: 1 Technical Efficacy: Stage 2 J. Magn. Reson. Imaging 2018;48:1610–1616
机译:背景技术在没有不良反应的前列腺癌的有效T 1 -MRI的超声介导的递送系统的兴趣已经稳步增加。目的是开发超声响应的双型超声(US)/ T 1 -MRI造影剂,用于高估过表达前列腺癌细胞的前列腺癌细胞(PSMA)的高效诊断并评估其潜力。研究类型体外。受试两种前列腺癌细胞系。场强/序列每种研究组在TR 400毫秒下进行3.0T MRI,TE 10毫秒,240×240矩阵,翻转角90°,切片厚度3≤mm,NSA带4,带宽115?Hz /像素,120×120?mm的foV。评估显微镜,定量和定性分析仪器和临床装置用于评估这种新型造影剂及其诊断效果。统计测试我们使用线性回归分析来确定我们/ T 1 -MRI造影剂和加蟾蜍的纵向松弛率(R 1)值。结果Microbubble + Fe 3+黑色素纳米粒子+肽(MB + Fe 3+ MNPP)具有良好的美国对比效果,如商业美国代理商。它们之间的强度的差异低于5%。 Mb + Fe 3+ Mnpps和Gadobutrol的R 1值分别为4.5和3.7S -1 / mm。超过数百款的Fe 3+ MNPPS位于用MB + Fe 3+ MNPP和美国刺激治疗的前列腺癌细胞,但在其他前列腺癌细胞中,Fe 3+ MnPP的数量低于表达较少的PSMA。具有MB + Fe 3+ MNPP和美国刺激的前细胞仅显示出最高的T 1 -MRI信号,因为靶向细胞和美国刺激的肽的协同效应,用于将Fe 3+ MnPP递送给细胞。通过使用WST测定,确认MB + Fe 3+ MNPP的细胞毒性。将细胞与复合物的可生存性高于90%。数据结论我们合成MB + Fe 3+ MNPP作为潜在的US / T 1 -MRI造影剂。该复合体适用于诊断所需的前列腺癌细胞。证据水平:1技术效果:第2阶段J. MANG。恢复。 2018年成像; 48:1610-1616

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