Roche Véronique Pasquale, Mohamad-Djafari Ali, Innominato Pasquale Fabio, Karaboué Abdoulaye, Gorbach Alexander, Lévi Francis Albert
INSERM, U776, Biological Rhythms and Cancers , Villejuif , France .
Chronobiol Int. 2014 Apr;31(3):409-20. doi: 10.3109/07420528.2013.864301. Epub 2014 Jan 7.
The disruption of the temperature circadian rhythm has been associated with cancer progression, while its amplification resulted in cancer inhibition in experimental tumor models. The current study investigated the relevance of skin surface temperature rhythms as biomarkers of the Circadian Timing System (CTS) in order to optimize chronotherapy timing in individual cancer patients. Baseline skin surface temperature at four sites and wrist accelerations were measured every minute for 4 days in 16 patients with metastatic gastro-intestinal cancer before chronotherapy administration. Temperature and rest-activity were recorded, respectively, with wireless skin surface temperature patches (Respironics, Phillips) and an actigraph (Ambulatory Monitoring). Both variables were further monitored in 10 of these patients during and after a 4-day course of a fixed chronotherapy protocol. Collected at baseline, during and after therapy longitudinal data sets were processed using Fast Fourier Transform Cosinor and Linear Discriminant Analyses methods. A circadian rhythm was statistically validated with a period of 24 h (p < 0.05) for 49/61 temperature time series (80.3%), and 15/16 rest-activity patterns (93.7%) at baseline. However, individual circadian amplitudes varied from 0.04 °C to 2.86 °C for skin surface temperature (median, 0.72 °C), and from 16.6 to 146.1 acc/min for rest-activity (median, 88.9 acc/min). Thirty-nine pairs of baseline temperature and rest-activity time series (75%) were correlated (r > |0.7|; p < 0.05). Individual circadian acrophases at baseline were scattered from 15:18 to 6:05 for skin surface temperature, and from 12:19 to 15:18 for rest-activity, with respective median values of 01:10 (25-75% quartiles, 22:35-3:07) and 14:12 (13:14-14:31). The circadian patterns in skin surface temperature and rest-activity persisted or were amplified during and after fixed chronotherapy delivery for 5/10 patients. In contrast, transient or sustained disruption of these biomarkers was found for the five other patients, as indicated by the lack of any statistically significant dominant period in the circadian range. No consistent correlation (r < |0.7|, p ≥ 0.05) was found between paired rest-activity and temperature time series during fixed chronotherapy delivery. In conclusion, large inter-patient differences in circadian amplitudes and acrophases of skin surface temperature were demonstrated for the first time in cancer patients, despite rather similar rest-activity acrophases. The patient-dependent coupling between both CTS biomarkers, and its possible alteration on a fixed chronotherapy protocol, support the concept of personalized cancer chronotherapy.
体温昼夜节律的紊乱与癌症进展相关,而在实验性肿瘤模型中其增强则导致癌症抑制。本研究调查了皮肤表面温度节律作为昼夜节律系统(CTS)生物标志物的相关性,以便优化个体癌症患者的时辰治疗时机。在16例转移性胃肠道癌患者进行时辰治疗前,连续4天每分钟测量四个部位的基线皮肤表面温度和手腕加速度。分别使用无线皮肤表面温度贴片(Respironics,飞利浦)和活动记录仪(动态监测)记录温度和休息 - 活动情况。在这些患者中的10例接受为期4天的固定时辰治疗方案期间及之后,对这两个变量进行进一步监测。使用快速傅里叶变换余弦分析和线性判别分析方法处理在基线、治疗期间和治疗后收集的纵向数据集。在基线时,49/61个温度时间序列(80.3%)和15/16个休息 - 活动模式(93.7%)的昼夜节律经统计学验证,周期为24小时(p < 0.05)。然而,皮肤表面温度的个体昼夜振幅在0.04℃至2.86℃之间变化(中位数为0.72℃),休息 - 活动的昼夜振幅在16.6至146.1次/分钟之间变化(中位数为88.9次/分钟)。39对基线温度和休息 - 活动时间序列(75%)具有相关性(r > |0.7|;p < 0.05)。基线时,皮肤表面温度的个体昼夜峰值相位在15:18至6:05之间分散,休息 - 活动的昼夜峰值相位在12:19至15:18之间分散,各自的中位数分别为01:10(25 - 75%四分位数,22:35 - 3:07)和14:12(1 :14 - 14:31)。在5/10例患者接受固定时辰治疗期间及之后,皮肤表面温度和休息 - 活动的昼夜模式持续存在或增强。相反,在另外5例患者中发现这些生物标志物出现短暂或持续的紊乱,表现为在昼夜节律范围内缺乏任何具有统计学意义的主导周期。在固定时辰治疗期间,配对的休息 - 活动和温度时间序列之间未发现一致的相关性(r < |0.7|,p≥0.05)。总之,首次在癌症患者中证明了皮肤表面温度的昼夜振幅和峰值相位存在较大的个体间差异,尽管休息 - 活动的峰值相位较为相似。两种CTS生物标志物之间的患者依赖性耦合及其在固定时辰治疗方案中可能的改变,支持了个性化癌症时辰治疗的概念。
