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Strategic Steps for Advanced Molecular Imaging with Magnetic Resonance-Based Diagnostic Modalities

机译:基于磁共振的诊断方式进行高级分子成像的战略步骤

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With the rapidly-expanding sophistication in our understanding of cancer cell biology, molecular imaging offers a critical bridge to oncology. Molecular imaging through magnetic resonance spectroscopy (MRS) can provide information about many metabolites at the same time. Since MRS entails no ionizing radiation, repeated monitoring, including screening can be performed. However, MRS via the fast Fourier transform (FFT) has poor resolution and signal-to-noise ratio (SNR). Moreover, subjective and non-unique (ambiguous) fittings of FFT spectra cannot provide reliable quantification of clinical usefulness. In sharp contrast, objective and unique (unambiguous) signal processing by the fast Padé transform (FPT) can increase resolution and retrieve the true quantitative metabolic information. To illustrate, we apply the FPT to in vitro MRS data as encoded from malignant ovarian cyst fluid and perform detailed analysis. This problem area is particularly in need of timely diagnostics by more advanced modalities, such as high-resolution MRS, since conventional methods usually detect ovarian cancers at late stages with poor prognosis, whereas at an early stage the prognosis is excellent. The reliability and robustness of the FPT is assessed for time signals contaminated with varying noise levels. In the presence of higher background noise, all physical metabolites were unequivocally identified and their concentrations precisely extracted, using small fractions of the total signal length. Via the “signal-noise separation” concept alongside the “stability test”, all non-physical information was binned, such that fully denoised spectra were generated. These results imply that a reformulation of data acquisition is needed, as guided by the FPT in MRS, since a small number of short transient time signals can provide high resolution and good SNR. This would enhance the diagnostic accuracy of MRS and shorten examination times, thereby improving efficiency and cost-effectiveness of this high throughput cancer diagnostic modality. Such advantages could be particularly important for more effective ovarian cancer detection, as well as more broadly for improved diagnostics and treatment within oncology.
机译:随着我们对癌细胞生物学的理解迅速发展,分子成像为肿瘤学提供了重要的桥梁。通过磁共振波谱(MRS)进行的分子成像可以同时提供有关许多代谢物的信息。由于MRS不需要电离辐射,因此可以进行重复监测,包括筛查。但是,通过快速傅立叶变换(FFT)的MRS具有较差的分辨率和信噪比(SNR)。此外,FFT谱的主观和非唯一(模棱两可)拟合无法提供临床实用性的可靠量化。与之形成鲜明对比的是,通过快速Padé变换(FPT)进行的客观,独特(明确)的信号处理可以提高分辨率并检索真正的定量代谢信息。为了说明这一点,我们将FPT应用于从恶性卵巢囊肿液中编码的体外MRS数据,并进行详细分析。这个问题领域特别需要通过更先进的方式(例如高分辨率MRS)进行及时诊断,因为常规方法通常在预后较差的晚期检测出卵巢癌,而在早期则预后良好。 FPT的可靠性和鲁棒性是针对被变化的噪声水平污染的时间信号进行评估的。在较高背景噪音的情况下,使用总信号长度的一小部分即可明确鉴定所有物理代谢物,并精确提取其浓度。通过“信号噪声分离”概念以及“稳定性测试”,将所有非物理信息合并在一起,从而生成完全去噪的光谱。这些结果表明,由于MRS中FPT的指导,需要重新构造数据采集,因为少量的短瞬态时间信号可以提供高分辨率和良好的SNR。这将提高MRS的诊断准确性并缩短检查时间,从而提高这种高通量癌症诊断方法的效率和成本效益。这样的优势对于更有效地检测卵巢癌以及在肿瘤内改善诊断和治疗可能更重要。

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