Dawn-to-dusk dry fasting decreases circulating inflammatory cytokines in subjects with increased body mass index

Zahraa Al lami , Miray Kurtca , Moin Uddin Atique , Antone R. Opekun , Mohamad S. Siam , Prasun K. Jalal , Bijan Najafi , Sridevi Devaraj , Ayse L. Mindikoglu
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引用次数: 0

Abstract

Background

The circadian rhythm involves numerous metabolic processes, including sleep/awakening, body temperature regulation, hormone secretion, hepatic function, cellular plasticity, and cytokine release (inflammation), that appear to have a dynamic relationship with all the processes above. Studies have linked various cytokines to the chronic state of low-grade inflammation and oxidative stress in obesity. Dawn-to-dusk dry fasting (DDDF) could alleviate the adverse effects of obesity by decreasing inflammation. This study examined the effects of DDDF on circulating inflammatory cytokines in subjects with increased body mass index (BMI).

Methods

The current observational prospective study included adult subjects with a BMI equal to or greater than 25 kg/m2 who practiced the annual religious 30-day DDDF. Individuals with significant underlying medical conditions were excluded to limit confounding factors. All subjects were evaluated within two weeks before 30-day DDDF, within the fourth week of 30-day DDDF, and within two weeks after 30-day DDDF. Multiple cytokines and clinical health indicators were measured at each evaluation.

Results

Thirteen subjects (10 men and three women) with a mean age of 32.9 years (SD = 9.7 years) and a mean BMI of 32 kg/m2 (SD = 4.6 kg/m2) were included. An overall associated decrease in the levels of multiple cytokines with DDDF was observed. A significant decrease in the mean interleukin 1 beta level was observed within the fourth week of 30-day DDDF (P = 0.045), which persisted even after the fasting period (P = 0.024). There was also a significant decrease in the mean levels of interleukin 15 (IL-15) (P = 0.014), interleukin 1 receptor antagonist (P = 0.041), macrophage-derived chemokine (MDC) (P = 0.013), and monokine induced by interferon gamma/chemokine (C-X-C motif) ligand 9 (P = 0.027) within the fourth week of 30-day DDDF and in the mean levels of fibroblast growth factor 2 (P = 0.010), interleukin 12 p40 subunit (P = 0.038), interleukin 22 (P = 0.025) and tumor necrosis factor alpha (P = 0.046) within two weeks after 30-DDDF. In terms of anthropometric parameters, there was a decrease in mean body weight (P = 0.032), BMI (P = 0.028), and hip circumference (P = 0.007) within the fourth week of 30-day DDDF and a decrease in mean weight (P = 0.026), BMI (P = 0.033) and hip circumference (P = 0.016) within two weeks after 30-day DDDF compared with the levels measured within two weeks before 30-day DDDF. Although there was no significant correlation between changes in weight and changes in circulating inflammatory cytokines, there was a significant positive correlation between changes in waist circumference and changes in specific inflammatory cytokines (e.g., IL-15, MDC, platelet-derived growth factor, soluble CD40L, vascular endothelial growth factor A) within the fourth week of 30-day DDDF and/or two weeks after 30-day DDDF. A significant decrease in mean average resting heart rate within the fourth week of 30-day DDDF was also observed (P = 0.023), and changes between average resting heart rate and changes in interleukin-8 levels within the fourth week of 30-day DDDF compared with baseline levels were positively correlated (r = 0.57, P = 0.042).

Conclusion

DDDF appears to be a unique and potent treatment to reduce low-grade chronic inflammation caused by obesity and visceral adiposity. Further studies with more extended follow-up periods are warranted to investigate the long-term anti-inflammatory benefits of DDDF in individuals with increased BMI.

从黎明到黄昏的干性禁食可降低体重指数增加受试者体内循环炎性细胞因子的含量
背景昼夜节律涉及许多新陈代谢过程,包括睡眠/觉醒、体温调节、激素分泌、肝功能、细胞可塑性和细胞因子释放(炎症),它们似乎与上述所有过程都有着动态的关系。研究表明,各种细胞因子与肥胖症的慢性低度炎症和氧化应激状态有关。从黎明到黄昏的干禁食(DDDF)可以通过减少炎症来减轻肥胖的不良影响。本研究考察了DDDF对体重指数(BMI)增加的受试者循环炎症细胞因子的影响。方法本观察性前瞻性研究纳入了体重指数等于或大于25 kg/m2、每年进行30天DDDF的成年受试者。为限制混杂因素,排除了患有严重基础疾病的受试者。所有受试者都在 DDDF 30 天前的两周内、DDDF 30 天后的第四周内以及 DDDF 30 天后的两周内接受了评估。每次评估都会测量多种细胞因子和临床健康指标。结果纳入的 13 名受试者(10 名男性和 3 名女性)的平均年龄为 32.9 岁(SD = 9.7 岁),平均体重指数为 32 kg/m2(SD = 4.6 kg/m2)。观察发现,多种细胞因子水平的总体下降与 DDDF 有关。在为期 30 天的 DDDF 的第四周,白细胞介素 1 beta 的平均水平明显下降(P = 0.045),甚至在禁食期后仍持续下降(P = 0.024)。白细胞介素 15(IL-15)(P = 0.014)、白细胞介素 1 受体拮抗剂(P = 0.041)、巨噬细胞衍生趋化因子(MDC)(P = 0.013)和干扰素γ/趋化因子(C-X-C 矩阵)配体 9 诱导的单克隆(P = 0.027),以及成纤维细胞生长因子 2(P = 0.010)、白细胞介素 12 p40 亚基(P = 0.038)、白细胞介素 22(P = 0.025)和肿瘤坏死因子α(P = 0.046)的平均水平。在人体测量参数方面,与DDDF 30天前两周内测量的水平相比,DDDF 30天后第四周内的平均体重(P = 0.032)、体重指数(BMI)(P = 0.028)和臀围(P = 0.007)有所下降,DDDF 30天后两周内的平均体重(P = 0.026)、体重指数(BMI)(P = 0.033)和臀围(P = 0.016)有所下降。虽然体重变化与循环炎症细胞因子的变化之间没有明显的相关性,但在DDDF 30天后的第四周和/或两周内,腰围的变化与特定炎症细胞因子(如IL-15、MDC、血小板衍生生长因子、可溶性CD40L、血管内皮生长因子A)的变化之间存在明显的正相关性。结论DDDF似乎是减少肥胖和内脏脂肪引起的低度慢性炎症的一种独特而有效的治疗方法。有必要进行更多研究,延长随访时间,以调查 DDDF 对体重指数增加的个体的长期抗炎益处。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Metabolism open
Metabolism open Agricultural and Biological Sciences (General), Endocrinology, Endocrinology, Diabetes and Metabolism
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