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The Association of IFI27 Expression and Fatigue Intensification during Localized Radiation Therapy: Implication of a Para-Inflammatory Bystander Response

机译:局部放射治疗期间IFI27表达与疲劳加剧的关联:副炎症旁观者反应的含义

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The mechanisms behind fatigue intensification during cancer therapy remain elusive. The interferon alpha-inducible protein 27 (IFI27) was the most up-regulated gene based on our previous microarray data in fatigued men with non-metastatic prostate cancer receiving localized external beam radiation therapy (EBRT). The purpose of this study was to confirm the IFI27 up-regulation and determine its association with fatigue intensification during EBRT. Peripheral blood samples and fatigue scores were collected at three time points—prior to EBRT, at midpoint, and at completion of EBRT. Confirmatory quantitative real time polymerase chain reaction (qPCR) and enzyme-linked immunosorbent assay (ELISA) were utilized to verify the microarray results. Subjects were a total of 40 Caucasian men with prostate cancer; 20 scheduled for EBRT (65.6 ± 7.5 years old), and 20 on active surveillance as controls (62.8 ± 6.1 years old). Significant IFI27 expression overtime during EBRT was confirmed by qPCR (p 0.5), which correlated with fatigue scores during EBRT (R = −0.90, p = 0.006). Alterations in mechanisms associated with immune response and mitochondrial function that explain the up-regulation of IFI27 may provide an understanding of the pathways related to the intensification of fatigue during localized radiation therapy.
机译:癌症治疗期间疲劳加剧的背后机制尚不清楚。干扰素α诱导蛋白27(IFI27)是基于我们先前的微阵列数据,在接受局部外照射治疗(EBRT)的非转移性前列腺癌疲劳男性中最上调的基因。这项研究的目的是确认IFI27上调并确定其与EBRT期间疲劳加剧的关系。在EBRT之前,中点和EBRT完成的三个时间点收集外周血样本和疲劳评分。验证性实时定量聚合酶链反应(qPCR)和酶联免疫吸附测定(ELISA)用于验证芯片结果。受试者共有40名患有前列腺癌的白人男子; 20例计划用于EBRT(65.6±7.5岁),20例作为对照进行积极监测(62.8±6.1岁)。 qPCR证实了EBRT期间IFI27的显着超时表达(p <0.5),这与EBRT期间的疲劳评分相关(R = -0.90,p = 0.006)。与免疫应答和线粒体功能相关的机制改变可以解释IFI27的上调,可能有助于了解与局部放射治疗过程中疲劳加剧有关的途径。

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