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首页> 外文期刊>Clinical cancer research: an official journal of the American Association for Cancer Research >Serum molecular signatures of weight change during early breast cancer chemotherapy.
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Serum molecular signatures of weight change during early breast cancer chemotherapy.

机译:早期乳腺癌化疗期间体重变化的血清分子标志。

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摘要

PURPOSE: Weight gain in women receiving chemotherapy for breast cancer is associated with a higher risk of recurrence but its mechanisms are poorly understood. EXPERIMENTAL DESIGN: To investigate this, we assessed the metabolic, cytokine, and appetite-related peptide alterations during adjuvant chemotherapy for early breast cancer in postmenopausal women, and correlated these with body mass measurements. Specifically, we performed global metabolic profiling using (1)H-nuclear magnetic resonance spectroscopy of sequential sera, examined ghrelin immunoreactivity, RIAs for GLP-1 and peptide YY, and electrochemiluminescent cytokine analyses (tumor necrosis factor-alpha and interleukin-6) on sequential samples. RESULTS: In those who gained >1.5 kg, several metabolite levels were positively associated with weight gain, specifically lactate, which was 63.5% greater in patients with increased body weight during chemotherapy compared with those with no weight gain (P < 0.01; the prespecified primary end point). A strong correlation (r = 0.7, P < 0.001) was detected between the rate of weight change and serum lactate levels, and on average, lactate levels exhibited the greatest metabolic response to chemotherapy, increasing by up to 75%. Normalized levels of peptide YY were also observed to be elevated in patients not gaining weight posttreatment (+30% compared with -7% for the weight gain group; P < 10(-4)). Baseline lactate, alanine, and body fat were all prognostic for weight gain (area under the receiver operator characteristic curves, >0.77; P < 0.05). No associations were observed between any other parameter and weight gain, including cytokine levels. CONCLUSIONS: Metabonomics identifies excess energy expenditure pathways perturbed during chemotherapy for breast cancer, and establishes a significant association between serum lactate, body fat, and substantive weight gain during chemotherapy.
机译:目的:接受乳腺癌化疗的女性体重增加与复发风险较高有关,但其机理尚不清楚。实验设计:为了对此进行调查,我们评估了绝经后早期乳腺癌辅助化疗期间代谢,细胞因子和食欲相关肽的变化,并将其与体重测量结果相关联。具体而言,我们使用连续血清的(1)H核磁共振波谱进行了整体代谢谱分析,检查了生长素释放肽的免疫反应性,GLP-1和YY肽的RIA以及电化学发光细胞因子分析(肿瘤坏死因子-α和白介素-6)。顺序样本。结果:体重增加> 1.5 kg的人群中,几种代谢物水平与体重增加呈正相关,特别是乳酸,与无体重增加的患者相比,化疗期间体重增加的患者的乳酸盐含量高63.5%(P <0.01;预先设定主要终点)。体重变化率与血清乳酸水平之间存在很强的相关性(r = 0.7,P <0.001),平均而言,乳酸水平对化学疗法表现出最大的代谢反应,最多可增加75%。在未增加体重的患者中,还可以观察到正常的YY肽水平升高(+ 30%,而体重增加组为-7%; P <10(-4))。基线乳酸,丙氨酸和体脂均可预示体重增加(接受者操作员特征曲线下的面积,> 0.77; P <0.05)。在其他任何参数与体重增加(包括细胞因子水平)之间均未发现关联。结论:代谢组学确定了乳腺癌化学疗法中干扰的过多能量消耗途径,并建立了血清乳酸,体脂与化学疗法中体重的实质增加之间的显着关联。

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