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Molecular Imaging Without Radiopharmaceuticals?

机译:没有放射性药物的分子成像?

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The limitations on the sensitivity for detecting small changes in MRI, CT, and ultrasound pulse-echo images are used to estimate the practical requirements for molecular imaging and targeted contrast enhancement for these modalities. These types of imaging are highly unlikely to approach the sensitivity for detecting molecular processes of radionuclear methods, and the prospects for achieving sufficient concentrations of appropriate agents in vivo are poor for several types of applications such as small-molecule targeting of specific receptors. However, using relatively large carrier systems such as particles and liposomes, sufficient concentrations of paramagnetic agents may be delivered to achieve MR-signal changes adequate for detection. The use of higher-resolution MR images will aid the prospects for molecular imaging in small animals. Theoretic considerations also predict that a similar approach, using rather large particles or carriers of materials with a high atomic number, may also be successful for CT, especially with additional developments such as the use of monochromatic x-rays. The prospects of molecular imaging by x-ray imaging may not be as bleak as has been predicted. For ultrasound detection, gas-filled bubbles can provide a sufficient backscattered sound intensity to be detectable at concentrations and sizes not much different from agents designed for these other modalities.
机译:用于检测MRI,CT和超声脉冲回波图像中微小变化的灵敏度的局限性被用于估计这些模式的分子成像和目标对比增强的实际要求。这些类型的成像极不可能达到检测放射性核方法分子过程的灵敏度,并且对于几种类型的应用(例如特定受体的小分子靶向),体内获得足够浓度的合适药物的前景很差。但是,使用相对较大的载体系统(例如颗粒和脂质体),可以递送足够浓度的顺磁性试剂以实现足以进行检测的MR信号变化。高分辨率MR图像的使用将有助于小动物分子成像的前景。理论上的考虑还预测,使用较大原子数或具有高原子序数的材料的载体的类似方法也可能成功用于CT,尤其是在采用诸如单色X射线等其他开发技术的情况下。通过X射线成像进行分子成像的前景可能不像预期的那样黯淡。对于超声检测,充气的气泡可以提供足够的反向散射声强,以便在与针对这些其他方式设计的试剂没有太大区别的浓度和大小下可以检测到。

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