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首页> 外文期刊>NMR in biomedicine >Prediction of chemotherapeutic response of colorectal liver metastases with dynamic gadolinium-DTPA-enhanced MRI and localized 19F MRS pharmacokinetic studies of 5-fluorouracil.
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Prediction of chemotherapeutic response of colorectal liver metastases with dynamic gadolinium-DTPA-enhanced MRI and localized 19F MRS pharmacokinetic studies of 5-fluorouracil.

机译:动态dynamic-DTPA增强的MRI和5-氟尿嘧啶的19F MRS药代动力学研究预测大肠肝转移的化学治疗反应。

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Systemic chemotherapy is effective in only a subset of patients with metastasized colorectal cancer. Therefore, early selection of patients who are most likely to benefit from chemotherapy is desirable. Response to treatment may be determined by the delivery of the drug to the tumor, retention of the drug in the tumor and by the amount of intracellular uptake, metabolic activation and catabolism, as well as other factors. The first aim of this study was to investigate the predictive value of DCE-MRI with the contrast agent Gd-DTPA for tumor response to first-line chemotherapy in patients with liver metastases of colorectal cancer. The second aim was to investigate the predictive value of 5-fluorouracil (FU) uptake, retention and catabolism as measured by localized (19)F MRS for tumor response to FU therapy. Since FU uptake, retention and metabolism may depend on tumor vascularization, the relationship between (19)F MRS and the DCE-MRI parameters k(ep), K(trans) and v(e) was also examined (1). In this study, 37 patients were included. The kinetic parameters of DCE-MRI, k(ep), K(trans) and v(e), before start of treatment did not predict tumor response after 2 months, suggesting that the delivery of chemotherapy by tumor vasculature is not a major factor determining response in first-line treatment. No evident correlations between (19)F MRS parameters and tumor response were found. This suggests that in liver metastases that are not selected on the basis of their tumor diameter, FU uptake and catabolism are not limiting factors for response. The transfer constant K(trans), as measured by DCE-MRI before start of treatment, was negatively correlated with FU half-life in the liver metastases, which suggests that, in metastases with a larger tumor blood flow or permeability surface area product, FU is rapidly washed out from the tumor.
机译:全身化疗仅对转移性大肠癌患者有效。因此,期望尽早选择最有可能从化学疗法中受益的患者。对治疗的反应可以通过药物向肿瘤的递送,药物在肿瘤中的保留以及细胞内摄取,代谢激活和分解代谢的量以及其他因素来确定。这项研究的首要目的是研究DCE-MRI和造影剂Gd-DTPA对大肠癌肝转移患者对一线化疗的肿瘤反应的预测价值。第二个目的是研究5-氟尿嘧啶(FU)摄取,保留和分解代谢的预测价值,通过局部(19)F MRS测量对肿瘤对FU治疗的反应。由于FU的吸收,保留和代谢可能取决于肿瘤的血管形成,因此还检查了(19)F MRS与DCE-MRI参数k(ep),K(trans)和v(e)之间的关系(1)。在这项研究中,包括37名患者。开始治疗前DCE-MRI的动力学参数k(ep),K(trans)和v(e)不能预测2个月后的肿瘤反应,这表明通过肿瘤脉管系统进行化疗不是主要因素确定一线治疗的反应。在(19)F MRS参数和肿瘤反应之间未发现明显的相关性。这表明在未根据肿瘤直径进行选择的肝转移中,FU摄取和分解代谢不是限制反应的因素。在治疗开始之前,通过DCE-MRI测量的转移常数K(trans)与肝转移中FU的半衰期呈负相关,这表明在肿瘤血流或通透性表面积乘积较大的转移中, FU被迅速从肿瘤中冲洗掉。

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