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Magnetic Resonance Spectroscopic Imaging of Tumor Metabolic Markers for Cancer Diagnosis, Metabolic Phenotyping, and Characterization of Tumor Microenvironment

机译:肿瘤代谢标记物的磁共振波谱成像,用于癌症诊断,代谢表型分析和肿瘤微环境表征

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Cancer cells display heterogeneous genetic characteristics, depending on the tumor dynamic microenvironment. Abnormal tumor vasculature and poor tissue oxygenation generate a fraction of hypoxic tumor cells that have selective advantages in metastasis and invasion and often resist chemo- and radiation therapies. The genetic alterations acquired by tumors modify their biochemical pathways, which results in abnormal tumor metabolism. An elevation in glycolysis known as the “Warburg effect” and changes in lipid synthesis and oxidation occur. Magnetic resonance spectroscopy (MRS) has been used to study tumor metabolism in preclinical animal models and in clinical research on human breast, brain, and prostate cancers. This technique can identify specific genetic and metabolic changes that occur in malignant tumors. Therefore, the metabolic markers, detectable by MRS, not only provide information on biochemical changes but also define different metabolic tumor phenotypes. When combined with the contrast-enhanced Magnetic Resonance Imaging (MRI), which has a high sensitivity for cancer diagnosis,in vivomagnetic resonance spectroscopic imaging (MRSI) improves the diagnostic specificity of malignant human cancers and is becoming an important clinical tool for cancer management and care. This article reviews the MRSI techniques as molecular imaging methods to detect and quantify metabolic changes in various tumor tissue types, especially in extracranial tumor tissues that contain high concentrations of fat. MRI/MRSI methods have been used to characterize tumor microenvironments in terms of blood volume and vessel permeability. Measurements of tissue oxygenation and glycolytic rates by MRS also are described to illustrate the capability of the MR technology in probing molecular information non-invasively in tumor tissues and its important potential for studying molecular mechanisms of human cancers in physiological conditions.
机译:癌细胞显示出异质的遗传特征,这取决于肿瘤的动态微环境。异常的肿瘤脉管系统和不良的组织氧合产生一部分缺氧的肿瘤细胞,这些细胞在转移和侵袭中具有选择性优势,并且经常抵抗化学疗法和放射疗法。肿瘤获得的遗传改变会改变其生化途径,从而导致异常的肿瘤代谢。发生糖酵解的现象称为“ Warburg效应”,脂质合成和氧化也发生变化。磁共振波谱(MRS)已被用于研究临床前动物模型中的肿瘤代谢以及人类乳腺癌,脑癌和前列腺癌的临床研究。该技术可以识别发生在恶性肿瘤中的特定遗传和代谢变化。因此,可通过MRS检测的代谢标记不仅提供有关生化变化的信息,而且还定义了不同的代谢肿瘤表型。体内磁共振波谱成像(MRSI)与对癌症诊断具有高敏感性的对比增强磁共振成像(MRI)结合使用时,可提高人类恶性肿瘤的诊断特异性,并且正成为癌症管理和治疗的重要临床工具。关心。本文将MRSI技术作为分子成像方法进行综述,以检测和量化各种肿瘤组织类型中的代谢变化,尤其是在含有高浓度脂肪的颅外肿瘤组织中。 MRI / MRSI方法已被用于根据血容量和血管通透性表征肿瘤微环境。还描述了通过MRS对组织氧合和糖酵解速率的测量,以说明MR技术在肿瘤组织中无创地探测分子信息的能力及其在生理条件下研究人类癌症分子机制的重要潜力。

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