chronotherapy

时间疗法
  • 文章类型: Journal Article
    这篇综述深入研究了生物钟与生理过程之间的复杂关系,强调它们在维持体内平衡方面的关键作用。由互锁的时钟基因编排,昼夜节律计时系统调节基本过程,如睡眠-觉醒周期,能量代谢,免疫功能,和细胞增殖。下丘脑视交叉上核的中心振荡器与明暗周期同步,而外周组织时钟受到诸如进食时间等线索的影响。昼夜节律中断,与夜班工作等现代生活方式有关,与不良健康结果相关,包括代谢综合征,心血管疾病,感染,和癌症。我们探讨了生物钟基因的分子机制及其对代谢紊乱和癌症发病机制的影响。昼夜节律紊乱和内分泌肿瘤之间的特定关联,跨越乳房,卵巢,睾丸,前列腺,甲状腺,垂体,和肾上腺癌,被突出显示。轮班工作与乳腺癌风险增加有关,PER基因影响肿瘤进展和耐药性。CLOCK基因表达与卵巢癌顺铂耐药相关,而衰老和间歇性禁食等因素会影响前列腺癌。我们的评论强调了昼夜节律和癌症之间复杂的相互作用,涉及细胞周期的调节,DNA修复,新陈代谢,免疫功能,和肿瘤微环境。我们提倡将生物定时整合到个性化医疗保健的临床考虑中,提出理解这些联系可能会导致新的治疗方法。证据支持以昼夜节律为中心的疗法,尤其是时间疗法,用于治疗内分泌肿瘤。我们的评论呼吁进一步研究以揭示生物钟与癌症之间的详细联系,为靶向治疗提供必要的见解。我们强调了公共卫生干预措施对减轻与生活方式相关的昼夜节律干扰的重要性,并强调了昼夜节律在疾病机制和治疗干预中的关键作用。
    This review delved into the intricate relationship between circadian clocks and physiological processes, emphasizing their critical role in maintaining homeostasis. Orchestrated by interlocked clock genes, the circadian timekeeping system regulates fundamental processes like the sleep-wake cycle, energy metabolism, immune function, and cell proliferation. The central oscillator in the hypothalamic suprachiasmatic nucleus synchronizes with light-dark cycles, while peripheral tissue clocks are influenced by cues such as feeding times. Circadian disruption, linked to modern lifestyle factors like night shift work, correlates with adverse health outcomes, including metabolic syndrome, cardiovascular diseases, infections, and cancer. We explored the molecular mechanisms of circadian clock genes and their impact on metabolic disorders and cancer pathogenesis. Specific associations between circadian disruption and endocrine tumors, spanning breast, ovarian, testicular, prostate, thyroid, pituitary, and adrenal gland cancers, are highlighted. Shift work is associated with increased breast cancer risk, with PER genes influencing tumor progression and drug resistance. CLOCK gene expression correlates with cisplatin resistance in ovarian cancer, while factors like aging and intermittent fasting affect prostate cancer. Our review underscored the intricate interplay between circadian rhythms and cancer, involving the regulation of the cell cycle, DNA repair, metabolism, immune function, and the tumor microenvironment. We advocated for integrating biological timing into clinical considerations for personalized healthcare, proposing that understanding these connections could lead to novel therapeutic approaches. Evidence supports circadian rhythm-focused therapies, particularly chronotherapy, for treating endocrine tumors. Our review called for further research to uncover detailed connections between circadian clocks and cancer, providing essential insights for targeted treatments. We emphasized the importance of public health interventions to mitigate lifestyle-related circadian disruptions and underscored the critical role of circadian rhythms in disease mechanisms and therapeutic interventions.
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  • 文章类型: Journal Article
    作为生物体的中央调控系统,大脑负责监督生物体生存所必需的各种生理过程。为了维持神经元发挥作用所必需的环境,大脑需要通过血脑屏障(BBB)高度选择性地摄取和消除特定分子。由于生物体的活动在一天中各不相同,血脑屏障如何适应大脑不断变化的需求?一种机制是通过昼夜节律对血脑屏障通透性进行时间调节,这将是本章的重点。为了理解生物钟在血脑屏障中的作用,我们将首先检查BBB的解剖结构和运输机制,使其能够发挥其作为限制性屏障的作用。接下来,我们将定义生物钟,讨论将包括对昼夜节律的介绍,转录-翻译反馈环(TTFL)作为昼夜节律计时的机制基础,以及在生物体中发现的组织钟的组织。然后,我们将介绍昼夜节律在调节BBB的细胞机制和功能中的作用。我们讨论了这种调节对影响睡眠行为的影响,神经退行性疾病的进展,最后是治疗神经系统疾病的药物递送。
    As the central regulatory system of an organism, the brain is responsible for overseeing a wide variety of physiological processes essential for an organism\'s survival. To maintain the environment necessary for neurons to function, the brain requires highly selective uptake and elimination of specific molecules through the blood-brain barrier (BBB). As an organism\'s activities vary throughout the day, how does the BBB adapt to meet the changing needs of the brain? A mechanism is through temporal regulation of BBB permeability via its circadian clock, which will be the focal point of this chapter. To comprehend the circadian clock\'s role within the BBB, we will first examine the anatomy of the BBB and the transport mechanisms enabling it to fulfill its role as a restrictive barrier. Next, we will define the circadian clock, and the discussion will encompass an introduction to circadian rhythms, the Transcription-Translation Feedback Loop (TTFL) as the mechanistic basis of circadian timekeeping, and the organization of tissue clocks found in organisms. Then, we will cover the role of the circadian rhythms in regulating the cellular mechanisms and functions of the BBB. We discuss the implications of this regulation in influencing sleep behavior, the progression of neurodegenerative diseases, and finally drug delivery for treatment of neurological diseases.
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  • 文章类型: Journal Article
    昼夜节律紊乱与前列腺癌发病率增加密切相关。将昼夜节律纳入前列腺癌发病机制的研究中,可以更全面地了解癌症的病因,为精准治疗提供新的选择。因此,本文全面总结了前列腺癌的流行病学,阐述了昼夜节律紊乱与前列腺癌发病风险的矛盾关系,并阐明了昼夜节律调节器与前列腺癌发病率之间的关系。重要的是,本文还重点研究了昼夜节律与雄激素受体信号通路的相关性,以及时间疗法在前列腺癌中的适用性。这可能证明在增强前列腺癌的临床治疗方面具有重要意义。
    Circadian rhythm disruption is closely related to increased incidence of prostate cancer. Incorporating circadian rhythms into the study of prostate cancer pathogenesis can provide a more comprehensive understanding of the causes of cancer and offer new options for precise treatment. Therefore, this article comprehensively summarizes the epidemiology of prostate cancer, expounds the contradictory relationship between circadian rhythm disorders and prostate cancer risk, and elucidates the relationship between circadian rhythm regulators and the incidence of prostate cancer. Importantly, this article also focuses on the correlation between circadian rhythms and androgen receptor signaling pathways, as well as the applicability of time therapy in prostate cancer. This may prove significant in enhancing the clinical treatment of prostate cancer.
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  • 文章类型: Journal Article
    人体内的生理过程在大约24小时的周期中被调节,称为昼夜节律。适应环境变化。骨节律在骨骼发育中起关键作用,新陈代谢,矿化,和重塑过程。骨节律表现出细胞特异性,骨骼中的不同细胞显示各种时钟基因的表达。多种环境因素,包括光,喂养,锻炼,和温度,通过交感神经系统和各种激素影响骨骼昼夜节律。骨骼昼夜节律的破坏有助于骨骼疾病的发作,例如骨质疏松症,骨关节炎和骨骼发育不全。相反,当针对骨细胞的昼夜节律时,这些骨骼疾病可以得到有效治疗,包括时钟基因和药物靶标的节律表达。在这次审查中,我们描述了各种骨细胞生理活动中独特的昼夜节律。然后,我们总结了使骨骼昼夜节律与潜在机制同步的因素。根据审查,我们旨在全面了解骨骼昼夜节律,并总结骨骼疾病的新预防和治疗策略。
    Physiological processes within the human body are regulated in approximately 24-h cycles known as circadian rhythms, serving to adapt to environmental changes. Bone rhythms play pivotal roles in bone development, metabolism, mineralization, and remodeling processes. Bone rhythms exhibit cell specificity, and different cells in bone display various expressions of clock genes. Multiple environmental factors, including light, feeding, exercise, and temperature, affect bone diurnal rhythms through the sympathetic nervous system and various hormones. Disruptions in bone diurnal rhythms contribute to the onset of skeletal disorders such as osteoporosis, osteoarthritis and skeletal hypoplasia. Conversely, these bone diseases can be effectively treated when aimed at the circadian clock in bone cells, including the rhythmic expressions of clock genes and drug targets. In this review, we describe the unique circadian rhythms in physiological activities of various bone cells. Then we summarize the factors synchronizing the diurnal rhythms of bone with the underlying mechanisms. Based on the review, we aim to build an overall understanding of the diurnal rhythms in bone and summarize the new preventive and therapeutic strategies for bone disorders.
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  • 文章类型: Journal Article
    昼夜节律系统是一种保守的计时机制,可调节多种过程,例如睡眠/唤醒,喂养/禁食,和活动/休息周期来协调行为和生理。昼夜节律紊乱可能是代谢疾病发展的一个促成因素,炎症性疾病,和更高的癌症风险。胶质母细胞瘤(GBM)是一种高度侵袭性的4级脑肿瘤,对常规治疗有抵抗力,诊断后预后不良。中位生存期仅为12-15个月。培养的GBM细胞显示含有功能性昼夜节律振荡器。在寻求更有效、副作用更低的治疗方法时,我们通过用特异性抑制剂(分别为CHIR99021和PF670462)靶向胞质激酶糖原合酶激酶-3(GSK-3)和酪蛋白激酶1ε/δ(CK1ε/δ)来评估生物钟的药理学调节,隐色素蛋白稳定剂(KL001),或在GBM衍生的细胞中Per2敲低表达后的昼夜节律中断。CHIR99021处理的细胞对细胞活力有显著影响,时钟蛋白表达,迁移,和细胞周期分布。此外,与对照细胞相比,GSK-3抑制后,培养物表现出更高的活性氧水平和脂滴含量变化。发现与单独的替莫唑胺治疗相比,CHIR99021与替莫唑胺的组合治疗改善对细胞活力的作用。Per2破坏影响GBM迁移和细胞周期进程。总的来说,我们的研究结果表明,药理学调节或分子时钟破坏严重影响GBM细胞生物学.
    The circadian system is a conserved time-keeping machinery that regulates a wide range of processes such as sleep/wake, feeding/fasting, and activity/rest cycles to coordinate behavior and physiology. Circadian disruption can be a contributing factor in the development of metabolic diseases, inflammatory disorders, and higher risk of cancer. Glioblastoma (GBM) is a highly aggressive grade 4 brain tumor that is resistant to conventional therapies and has a poor prognosis after diagnosis, with a median survival of only 12-15 months. GBM cells kept in culture were shown to contain a functional circadian oscillator. In seeking more efficient therapies with lower side effects, we evaluated the pharmacological modulation of the circadian clock by targeting the cytosolic kinases glycogen synthase kinase-3 (GSK-3) and casein kinase 1 ε/δ (CK1ε/δ) with specific inhibitors (CHIR99021 and PF670462, respectively), the cryptochrome protein stabilizer (KL001), or circadian disruption after Per2 knockdown expression in GBM-derived cells. CHIR99021-treated cells had a significant effect on cell viability, clock protein expression, migration, and cell cycle distribution. Moreover, cultures exhibited higher levels of reactive oxygen species and alterations in lipid droplet content after GSK-3 inhibition compared to control cells. The combined treatment of CHIR99021 with temozolomide was found to improve the effect on cell viability compared to temozolomide therapy alone. Per2 disruption affected both GBM migration and cell cycle progression. Overall, our results suggest that pharmacological modulation or molecular clock disruption severely affects GBM cell biology.
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  • 文章类型: Journal Article
    目标:时序型,它捕捉了一个人对活动和睡眠的日常偏好,在癫痫研究中仍然是一个研究不足的领域。在癫痫患者(PWE)中找到常见的时间型特征并解释对癫痫发作管理的可能影响是主要目标。
    方法:本范围审查审查了2010年至2023年的11项大规模调查。这些研究包括1.167名PWE和4.657名对照受试者。
    结果:PWE通常具有中间型。成年患者总体上更倾向于早晨,而儿科队列是可变的。时间型和癫痫发作控制之间的关系是有限的,因为只有两项成人研究报告了这一点,这些结果相互矛盾。发现在全身性癫痫中晚发型型比局灶性癫痫更为常见。未研究时间型与特异性抗癫痫药物(ASM)治疗的关系。
    结论:大多数PWE显示中间型,但是基于年龄的分析显示出更细微的趋势,孩子们显示可变模式,成年人通常倾向于清晨,和广泛性癫痫与晚上有关。这篇综述强调了对癫痫结局与时间型之间复杂联系进行更多研究的重要性。它强调需要研究更大的PWE样本,并仔细记录癫痫发作控制和ASM治疗,包括剂量和给药时间,以更好地了解时序型对癫痫结局的作用。
    OBJECTIVE: Chronotype, which captures a person\'s daily preferences for activity and sleep, is still a poorly researched area in epilepsy research. Finding common chronotype characteristics in people with epilepsy (PWE) and explaining possible effects on seizure management are the main goals.
    METHODS: Eleven large-scale investigations from 2010 to 2023 were examined in this scoping review. These studies included 1.167 PWE and 4.657 control subjects.
    RESULTS: PWE had intermediate chronotypes more often than not. Adult patients were more morning-oriented overall, while pediatric cohorts were variable. Relationships between chronotype and seizure control were limited since only two studies in adults reported this and those results conflicted. An evening-type chronotype was found to be more common in generalized epilepsy than focal. The relationship of chronotype and specific antiseizure medication (ASM) therapy was not investigated.
    CONCLUSIONS: The majority of PWE displayed an intermediate chronotype, but analyses based on age showed more nuanced trends, with children displaying variable patterns, adults generally tending toward morningness, and generalized epilepsy being associated with eveningness. This review underscores the importance of more research on the complex connections between epilepsy outcomes and chronotype. It emphasizes the need to study larger samples of PWE with carefully documented seizure control and ASM therapy, including dose and timing of administration to better understand the role of chronotype on epilepsy outcomes.
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  • 文章类型: Editorial
    暂无摘要。
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  • 文章类型: Journal Article
    背景:主要使用抗抑郁药物治疗重度抑郁症(MDD),但临床效果可能会延迟数周至数月。这项研究调查了短暂治疗性睡眠剥夺(TSD)诱导MDD症状快速改善的功效。
    方法:从2020年11月至2023年2月,将54例MDD住院患者随机分为TSD组和对照组。TSD组(23例)保持清醒36h,对照组(31例)保持规律的睡眠模式。所有参与者继续常规药物治疗。两组在基线和干预后使用24项汉密尔顿抑郁量表(HAMD-24)评估情绪。在TSD组中,使用视觉模拟量表(VAS)评估干预期间和干预后的主观情绪.使用蒙特利尔认知评估(MoCA)在基线和干预后评估认知功能。通过多导睡眠图记录TSD组的客观睡眠参数。随访期为一周。
    结果:HAMD-24评分在基线或干预后组间无差异。然而,干预后第3天TSD组的临床反应率比对照组高34.8%(3.2%),但没有持续到第七天。此外,在TSD期间,应答者的VAS评分比无应答者改善更快(p=0.047).两组间MoCA评分或客观睡眠参数无显著差异。
    结论:样本量小,损耗率显著。
    结论:治疗性睡眠剥夺可迅速改善MDD症状,而不影响睡眠参数或认知功能。有必要评估长期效果并确定预测TSD反应的因素。
    BACKGROUND: Major depressive disorder (MDD) is treated primarily using antidepressant drugs, but clinical effects may be delayed for weeks to months. This study investigated the efficacy of brief therapeutic sleep deprivation (TSD) for inducing rapid improvements in MDD symptoms.
    METHODS: From November 2020 to February 2023, 54 inpatients with MDD were randomly allocated to TSD and Control groups. The TSD group (23 cases) remained awake for 36 h, while the Control group (31 cases) maintained regular sleep patterns. All participants continued regular drug therapy. Mood was assessed using the 24-item Hamilton Depression Scale (HAMD-24) at baseline and post-intervention in both groups. In the TSD group, the Visual Analogue Scale (VAS) was utilized to evaluate subjective mood during and after the intervention. Cognitive function was assessed at baseline and post-intervention using the Montreal Cognitive Assessment (MoCA). Objective sleep parameters were recorded in the TSD group by polysomnography. The follow-up period spanned one week.
    RESULTS: HAMD-24 scores did not differ between groups at baseline or post-intervention. However, the clinical response rate was 34.8 % higher in the TSD group on day 3 post-intervention compared to the Control group (3.2 %), but not sustained by day 7. Moreover, responders demonstrated a faster improvement in the VAS score during TSD than non-responders (p = 0.047). There were no significant differences in MoCA scores or objective sleep parameters between the groups.
    CONCLUSIONS: Small sample size and notable attrition rate.
    CONCLUSIONS: Therapeutic sleep deprivation can rapidly improve MDD symptoms without influencing sleep parameters or cognitive functions. Assessment of longer-term effects and identification of factors predictive of TSD response are warranted.
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  • 文章类型: Journal Article
    血管疾病通常是由巨噬细胞和血管平滑肌细胞(VSMC)之间的相互作用引起的。本研究旨在阐明罗格列酮(RSG)的时间疗法是否可以调节巨噬细胞的分泌节律,从而控制VSMC的表型转换并阐明潜在的分子机制,为血管疾病的治疗提供了一种时间治疗方法。
    RAW264.7细胞和A7r5细胞通过50%FBS处理进行同步。通过脂多糖(LPS)暴露诱导M1型巨噬细胞。此外,将靶向PPARγ的siRNA和质粒转染到巨噬细胞中。评估包括细胞活力,迁移,炎症因子水平,脂质代谢物,时钟基因表达,和相对蛋白表达。
    我们透露,与核心时钟基因Bmal1和CLOCK对齐,在ZT2的RSG给药提前了TNF-α释放节律的阶段,而ZT12政府将其向后移动。在ZT2与TNF-α一起孵育显着促进了VSMC的表型转换。在ZT12孵育时,这种作用减弱,这表明VSMC中clock-MAPK途径的参与。此外,在ZT2的RSG给药提前了PPARγ和Bmal1基因的阶段,而ZT12管理将它们向后转移。此外,PPARγ过表达显著诱导巨噬细胞中甘油三酯(TG)积累。外源性TG上调巨噬细胞中Bmal1和CLOCK基因表达并显著增加TNF-α释放。
    涉及RSG的时间疗法诱导巨噬细胞内TG积累,导致昼夜节律基因的改变。这些变化,反过来,调节有节律的TNF-α释放阶段,并在VSMC表型转换中起调节作用。我们的研究为PPARγ激动剂的时间疗法奠定了理论基础。
    UNASSIGNED: Vascular diseases are often caused by the interaction between macrophages and vascular smooth muscle cells (VSMCs). This study aims to elucidate whether chronotherapy with rosiglitazone (RSG) can regulate the secretion rhythm of macrophages, thereby controlling the phenotypic switch of VSMCs and clarifying the potential molecular mechanisms, providing a chronotherapeutic approach for the treatment of vascular diseases.
    UNASSIGNED: RAW264.7 cells and A7r5 cells were synchronized via a 50 % FBS treatment. M1-type macrophages were induced through Lipopolysaccharide (LPS) exposure. Additionally, siRNA and plasmids targeting PPARγ were transfected into macrophages. The assessment encompassed cell viability, migration, inflammatory factor levels, lipid metabolites, clock gene expression, and relative protein expression.
    UNASSIGNED: We revealed that, in alignment with core clock genes Bmal1 and CLOCK, RSG administration at ZT2 advanced the phase of TNF-α release rhythm, while ZT12 administration shifted it backward. Incubation with TNF-α at ZT2 significantly promoted the phenotype switch of VSMCs. This effect diminished when incubated at ZT12, implicating the involvement of the clock-MAPK pathway in VSMCs. Furthermore, RSG administration at ZT2 advanced the phases of PPARγ and Bmal1 genes, whereas ZT12 administration shifted them backward. Additionally, PPARγ overexpression significantly induced triglyceride (TG) accumulation in macrophages. Exogenous TG upregulated Bmal1 and CLOCK gene expression in macrophages and significantly increased TNF-α release.
    UNASSIGNED: Chronotherapy involving RSG induces TG accumulation within macrophages, resulting in alterations in circadian gene rhythms. These changes, in turn, modulate the phase of rhythmic TNF-α release and play a regulatory role in VSMCs phenotype switch. Our study establishes a theoretical foundation for chronotherapy of PPARγ agonists.
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  • 文章类型: Journal Article
    这篇综述旨在收集有关内分泌节律的病理生理和临床方面的知识及其在临床实践中的意义。来自已发表的文献和关于这个主题的一些个人经历。我们选择复习,根据PRISMA指南,原始和观察性研究的结果,reviews,截至2024年3月发表的荟萃分析和病例报告。因此,在总结了生物节律的一般方面之后,我们将描述几种内分泌节律的特征及其破坏的后果,特别注意临床实践中的影响。有节奏的内分泌分泌物,像其他生理节律一样,是由位于视交叉上核的中央下丘脑时钟基因决定和调节的,它将节奏的时间与独立的时钟联系起来,在调节生理和行为的分层组织中。然而,一些环境因素,例如每天的光明/黑暗循环,睡眠/唤醒,和食物摄入的时机,可能会影响节奏特征。内分泌节律涉及重要的生理过程,它们的破坏可能导致几种疾病和癌症。因此,通过早期矫正时间疗法防止内分泌节律的破坏和恢复以前改变的节律是非常重要的。
    This review was aimed at collecting the knowledge on the pathophysiological and clinical aspects of endocrine rhythms and their implications in clinical practice, derived from the published literature and from some personal experiences on this topic. We chose to review, according to the PRISMA guidelines, the results of original and observational studies, reviews, meta-analyses and case reports published up to March 2024. Thus, after summarizing the general aspects of biological rhythms, we will describe the characteristics of several endocrine rhythms and the consequences of their disruption, paying particular attention to the implications in clinical practice. Rhythmic endocrine secretions, like other physiological rhythms, are genetically determined and regulated by a central hypothalamic CLOCK located in the suprachiasmatic nucleus, which links the timing of the rhythms to independent clocks, in a hierarchical organization for the regulation of physiology and behavior. However, some environmental factors, such as daily cycles of light/darkness, sleep/wake, and timing of food intake, may influence the rhythm characteristics. Endocrine rhythms are involved in important physiological processes and their disruption may cause several disorders and also cancer. Thus, it is very important to prevent disruptions of endocrine rhythms and to restore a previously altered rhythm by an early corrective chronotherapy.
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