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1 - Introduction to Circadian Rhythms

Published online by Cambridge University Press:  07 October 2023

By
Laura K. Fonken  and
Randy J. Nelson
Edited by
Laura K. Fonken  and
Randy J. Nelson
Laura K. Fonken
Affiliation:
University of Texas, Austin
Randy J. Nelson
Affiliation:
West Virginia University

Summary

Circadian rhythms have a period of approximately 24 hours and are set to precisely 24 hours by various zeitgebers (time givers), light being the most prominent zeitgeber. The central pacemakers for mammalian circadian rhythms are the suprachiasmatic nuclei (SCN) in the anterior hypothalamus. Humoral and neural signals from the SCN help synchronize circadian clocks throughout the body. At the molecular level, cellular circadian rhythms are formed from interlocking transcriptional-translational feedback loops (TTFL) of circadian clock genes that drive spontaneous oscillations of gene and protein expression with an approximately 24-hour period. Remarkably, the molecular clock components are expressed rhythmically in nearly every cell of the body and are entrained by signals from the SCN. Disruption of clock genes either through genes or environment can impair optimal biological function. Circadian rhythms regulate myriad homeostatic systems including the cardiac, immune, metabolic, and central nervous systems. Circadian regulation of physiological and behavioral functions can be disrupted by several factors including the timing of light exposure and food intake. This chapter reviews circadian disruptors to set up the remainder of the book.

Keywords

circadian disruptionlight at nightdiurnalmetabolismimmune
Type
Chapter
Information
Biological Implications of Circadian Disruption
A Modern Health Challenge
 , pp. 1 - 22
Publisher: Cambridge University Press
Print publication year: 2023

1.1 Introduction

For the past 3–4 billion years, life on Earth evolved under the predictable pattern of solar days; that is, exposure to light during the day and dark at night. Temporal constraints are obvious when considering the “rules of life.” That is, individuals cannot do everything all the time. For instance, energetic requirements are somewhat continuous, whereas energy production or consumption is somewhat sporadic. All organisms partition temporal energetic activities. Indeed, temporal partitioning of photosynthesis, metabolism, gene expression, reproduction, defense, growth, activity, and inactivity is universal among plants and animals. During the evolution of life, organisms internalized the temporal rhythm of Earth’s rotation and eventually developed self-sustaining biological clocks. These internal rhythms with periods of approximately 24 hours are called circadian rhythms, and the structures that generate them are called circadian clocks. A human’s primary circadian biological clock is a paired cluster of about 20,000 nerve cells in the hypothalamus at the base of the brain, called the suprachiasmatic nucleus (SCN). The period of a circadian clock is approximately 24 hours, but daily light exposure sets it to precisely 24 hours. Having our clocks set closer to our environment’s light–dark rhythms optimizes how our bodies function and how we behave.

Circadian clocks are a nearly universal feature of life on this planet, yet over the past century and a half we have managed to manipulate the amount of light in the environment so much that we are disrupting them. As we will learn throughout this book, either too much light exposure at night or too little light exposure during the day can disrupt central and peripheral timing mechanisms, how internal rhythms are entrained to the external environment, and the typical and optimal 24-hour physiological and behavioral functioning of individuals.

1.1.1 Central Pacemaker in the Suprachiasmatic Nucleus

Circadian rhythms in mammals are ubiquitously expressed throughout the body and are regulated by a hierarchy of independent self-sustaining molecular and cellular clocks. This hierarchy is entrained by external Zeitgebers (“time givers”) including light (primary), food, exercise, and even social cues. Rhythms throughout the body are subsequently maintained in a synchronized manner via intermediary neural and humoral cues. But where are these signals initiated? The primary pacemakers in mammals are the paired suprachiasmatic nuclei (SCN) that govern rhythms throughout the brain and body. The SCN are located directly above the optic chiasm in the anterior hypothalamus and contain a diverse cellular make-up. SCN neurons produce the inhibitory neurotransmitter gamma aminobutyric acid (GABA) and various neuropeptides including arginine vasopressin (AVP), cholecystokinin (CCK), gastrin-releasing peptide (GRP), prokineticin 2 (Prok2), and vasoactive intestinal polypeptide (VIP) (reviewed in Moore et al., Reference Moore, Speh and Leak2002; Patton & Hastings, Reference Patton and Hastings2018). The SCN comprise two distinct regions with unique neuropeptide expression: the ventrolateral “core” contains neurons that express VIP and GRP, whereas the dorsal shell contains neurons that express AVP and CCK.

SCN neuron firing is tightly synchronized in “core” and “shell” regions through neural connections and timed release of these key neuropeptides (Patton & Hastings, Reference Patton and Hastings2018). VIP is an important synchronizer of neuronal networks in the SCN (Abrahamson & Moore, Reference Abrahamson and Moore2001); mice lacking VIP or VIP receptor 2 (VPAC2) exhibit attenuated behavioral rhythms and desynchronized circadian rhythms in cultured neurons from the SCN (Aton et al., Reference Aton, Colwell, Harmar, Waschek and Herzog2005; Colwell et al., Reference Colwell, Michel, Itri, Rodriguez, Tam, Lelievre, Hu, Liu and Waschek2003; Harmar et al., Reference Harmar, Marston, Shen, Spratt, West, Sheward, Morrison, Dorin, Piggins, Reubi, Kelly, Maywood and Hastings2002). Interestingly, in SCN neurons with the VIP or VPAC2 genes knocked out, circadian rhythms are restored by co-culture with neurons from a wild-type SCN, suggesting that other molecules such as AVP also synchronize rhythms in the SCN (Maywood et al., Reference Maywood, Chesham, O’Brien and Hastings2011). Indeed, an AVP receptor antagonist prevents restoration of rhythms in VPAC2 knockout SCN neurons (Maywood et al., Reference Maywood, Chesham, O’Brien and Hastings2011).

Rhythms in the SCN are primarily entrained by light information that is communicated directly from the retina through the retinohypothalamic tract to the SCN (Beier et al., Reference Beier, Zhang, Yurgel and Hattar2021; Hattar et al., Reference Hattar, Kumar, Park, Tong, Tung, Yau and Berson2006; Moore & Qavi, Reference Moore and Qavi1971). In addition to retinal input, the SCN core receives input from the thalamus and raphe nucleus and the shell receives input from the hypothalamus, neocortex, and brainstem (Fernandez et al., Reference Fernandez, Chang, Hattar and Chen2016; Leak & Moore, Reference Abrahamson and Moore2001).

The SCN have unique circadian-focused properties that define them as the primary pacemaker: they receive direct retinal light input; neurons in the SCN have topographically organized coupling mechanisms, which allow them to remain synchronized in the absence of light input (Aton & Herzog, Reference Aton and Herzog2005); The SCN are protected from feedback by systemic clock-modifying factors such as glucocorticoids or feeding (Schibler et al., Reference Schibler, Gotic, Saini, Gos, Curie, Emmenegger, Sinturel, Gosselin, Gerber, Fleury-Olela, Rando, Demarque and Franken2015); SCN lesions abolish circadian rhythms throughout the body (Moore & Eichler, Reference Moore and Eichler1972; Stephan & Zucker, Reference Stephan and Zucker1972; Weaver, Reference Weaver1998); electrical and chemical stimulation of the SCN induce phase shifts (Albers et al., Reference Albers, Ferris, Leeman and Goldman1984; Rusak & Groos, Reference Rusak and Groos1982); and transplanting an SCN into an SCN-ablated animal restores circadian activity (Silver et al., Reference Silver, LeSauter, Tresco and Lehman1996). Furthermore, cultured SCN tissue will maintain long-term (>1 month) oscillations in the absence of external stimulation (Welsh et al., Reference Welsh, Logothetis, Meister and Reppert1995; Yamazaki et al., Reference Yamazaki, Numano, Abe, Hida, Takahashi, Ueda, Block, Sakaki, Menaker and Tei2000; Yoo et al., Reference Yoo, Yamazaki, Lowrey, Shimomura, Ko, Buhr, Siepka, Hong, Oh, Yoo, Menaker and Takahashi2004). Thus, the SCN features direct retinal input, synchronized output, and few peripheral feedback mechanisms, thereby optimizing this brain region to act as the primary circadian oscillator. Additional details about the central clock dynamics are provided in Chapter 2.

1.2 Molecular Mechanisms of the Circadian Clock

At the molecular level, cellular circadian rhythms are formed from interlocking transcriptional–translational feedback loops (TTFL) that drive spontaneous oscillations of gene and protein expression with an approximately 24 hour period. Remarkably, the molecular clock components are expressed rhythmically in nearly every cell of the body and are entrained by signals from the primary clock. The core components of this loop involve the induction of Period (Per1, Per2, and Per3) and Cryptochrome (Cry1 and Cry2) gene expression through E-box enhancers by the transcriptional activators circadian locomotor output cycles kaput (CLOCK) and brain and muscle arnt-like protein 1 (BMAL1) (Gekakis et al., Reference Gekakis, Staknis, Nguyen, Davis, Wilsbacher, King, Takahashi and Weitz1998; Hogenesch et al., Reference Hogenesch, Gu, Jain and Bradfield1998; Jin et al., Reference Jin, Shearman, Weaver, Zylka, de Vries and Reppert1999). Per and Cry proteins accumulate in the cytoplasm and then form large multimeric complexes which translocate back to the nucleus to interact with CLOCK and BMAL1 and repress their own transcription (Griffin et al., Reference Griffin, Staknis and Weitz1999; Kume et al., Reference Kume, Zylka, Sriram, Shearman, Weaver, Jin, Maywood, Hastings and Reppert1999; Lee et al., Reference Lee, Etchegaray, Cagampang, Loudon and Reppert2001). Progressive degradation of the existing inhibitory complexes then occurs, ultimately leading to renewed transcription of Per and Cry. This feedback loop takes approximately 24 hours to complete a cycle. There are additional feedback loops interlocked with the CLOCK-BMAL1/Per-Cry loop. A prominent loop involves the activation of the retinoic acid receptor-related orphan receptor (ROR) and REV-ERB by the CLOCK-BMAL1 complex which feeds back on BMAL1 to stabilize rhythms (Preitner et al., Reference Preitner, Damiola, Lopez-Molina, Zakany, Duboule, Albrecht and Schibler2002). Deletion of “core clock genes” (or, in some cases, 2+ paralogs of clock genes) reveals their requirement for rhythms in activity (Bunger et al., Reference Bunger, Wilsbacher, Moran, Clendenin, Radcliffe, Hogenesch, Simon, Takahashi and Bradfield2000; Cox & Takahashi, Reference Cox and Takahashi2019; Vitaterna et al., Reference Vitaterna, King, Chang, Kornhauser, Lowrey, McDonald, Dove, Pinto, Turek and Takahashi1994).

1.2.1 The Circadian System Is Synchronized to the Environment

Circadian rhythms oscillate at approximately but not exactly 24 hours. Variations in rhythm period occur at the whole organism level down to the individual cellular level (Czeisler et al., Reference Czeisler, Duffy, Shanahan, Brown, Mitchell, Rimmer, Ronda, Silva, Allan, Emens, Dijk and Kronauer1999). For example, humans display different “chronotypes,” meaning some people are early risers or “larks” and others prefer to stay up later and are known as “night owls.” These variations in preferred sleep and wake time are associated with distinct endogenous circadian periods: morning larks tend to have circadian rhythms that are shorter than night owls (Roenneberg et al., Reference Roenneberg, Wirz-Justice and Merrow2003). A number of genetic factors are associated with distinct chronotypes that include genes related to circadian regulation, as well as glutamate and insulin signaling pathways (Jones et al., Reference Jones, Lane, Wood, van Hees, Tyrrell, Beaumont, Jeffries, Dashti, Hillsdon, Ruth, Tuke, Yaghootkar, Sharp, Jie, Thompson, Harrison, Dawes, Byrne, Tiemeier and Weedon2019). Input to the circadian system is essential for maintaining everyone on the same 24 hour schedule.

1.2.2 Light Is the Dominant Entrainment Factor for the SCN

Light is the primary entrainment factor for synchronizing circadian rhythms to the 24 hour day. The major neural route of light entrainment occurs via activation of specialized cells in the retina called intrinsically photosensitive retinal ganglion cells (ipRGCs) (Berson et al., Reference Berson, Dunn and Takao2002; Provencio et al., Reference Provencio, Rollag and Castrucci2002). ipRGCs are a population of non-vision forming cells that are critical in transducing light information via the retinohypothalamic tract to the SCN (Beier et al., Reference Beier, Zhang, Yurgel and Hattar2021; Hattar et al., Reference Hattar, Kumar, Park, Tong, Tung, Yau and Berson2006; Moore & Qavi, Reference Moore and Qavi1971). Prior to the discovery of ipRGCs approximately 20 years ago, the existence of a non-vision forming cell was suspected as some individuals that lacked visual awareness maintained circadian rhythmicity and melatonin responses to light (Czeisler et al., Reference Czeisler, Shanahan, Klerman, Martens, Brotman, Emens, Klein and Rizzo1995). Moreover, responses to light in animals were poorly explained by the properties of rods and cones (e.g., Brainard et al., Reference Brainard, Hanifin, Greeson, Byrne, Glickman, Gerner and Rollag2001; Mrosovsky et al., Reference Mrosovsky, Lucas and Foster2001; Takahashi et al., Reference Takahashi, DeCoursey, Bauman and Menaker1984).

ipRGCs have extensive arbors and are activated by short (blue to humans) wavelengths of light due to their expression of the photopigment melanopsin (Do, Reference Do2019). Light activates melanopsin to trigger a G protein cascade, causing membrane depolarization and the release of glutamate and the neuropeptide pituitary adenylate cyclase activating peptide (PACAP) (Hannibal et al., Reference Hannibal, Hindersson, Knudsen, Georg and Fahrenkrug2002). Although the number of ipRGCs in the mammalian retina is limited, they display remarkable heterogeneity with six different morphological subtypes, M1–M6 (reviewed in Do, Reference Do2019). The distinct subtypes of ipRGCs are thought to regulate specific light intensity or times of day responses. The sensitivity of ipRGCs specifically to blue light has led to an interest in regulating the circadian system by manipulating the wavelength of light environment. Studies in humans have shown that high intensity blue light can be disruptive to the circadian system, resulting in melatonin suppression and sleep loss (Chang et al., Reference Chang, Aeschbach, Duffy and Czeisler2015; Hanifin et al., Reference Hanifin, Lockley, Cecil, West, Jablonski, Warfield, James, Ayers, Byrne, Gerner, Pineda, Rollag and Brainard2019; West et al., Reference West, Jablonski, Warfield, Cecil, James, Ayers, Maida, Bowen, Sliney, Rollag, Hanifin and Brainard2011). This has led to blue light filters in technology (e.g., laptops and smartphones) that eliminate these wavelengths of light at night. However, it is important to note that filtering out blue light is not a cure all: ipRGCs also receive input from rods and cones. Melanopsin knockout mice maintain some circadian responses to light, but mice lacking melanopsin coupled with disabled rod and cone phototransduction do not (Hattar et al., Reference Hattar, Lucas, Mrosovsky, Thompson, Douglas, Hankins, Lem, Biel, Hofmann, Foster and Yau2003).

Light input is transduced from an electrical signal – via propagation along the retinohypothalamic tract – to a chemical signal when the tract terminates in the SCN with the release of glutamate. Glutamate acts on NMDA receptors to increase calcium release in SCN neurons (Ding et al., Reference Ding, Faiman, Hurst, Kuriashkina and Gillette1997). This increased calcium activates the transcription factor CREB to increase Per transcription (Gau et al., Reference Gau, Lemberger, von Gall, Kretz, Le Minh, Gass, Schmid, Schibler, Korf and Schutz2002; Ginty et al., Reference Ginty, Kornhauser, Thompson, Bading, Mayo, Takahashi and Greenberg1993; Schurov et al., Reference Schurov, McNulty, Best, Sloper and Hastings1999). For instance, a brief flash of light during the inactive phase induces de novo expression of Per (Albrecht et al., Reference Albrecht, Sun, Eichele and Lee1997). Through these mechanisms, the SCN are optimized in mammals to link light timing in the environment with physiologic function.

1.2.3 Food, Exercise, and Other Factors Regulate Peripheral Circadian Rhythms

Although most strongly synchronized by light, the circadian system is also entrained by other factors. Early observations by Richter (Reference Richter1922) characterized anticipatory activity in response to timed feeding: rats fed one meal per day increase wheel running several hours prior to food availability. Indeed, both feeding (Boulos et al., Reference Boulos, Rosenwasser and Terman1980) and exercise (Edgar & Dement, Reference Edgar and Dement1991) can entrain circadian rhythms in locomotor activity. Moreover, when maintained in constant lighting conditions, rodents will also synchronize activity rhythms based on social cues (Paul et al., Reference Paul, Indic and Schwartz2015). As discussed in Section 1.3, non-photic entrainment factors are typically more salient for extra-SCN clocks.

1.3 Circadian Rhythms Occur Throughout the Body: Extra-SCN Tissue-Specific Clocks

In addition to the central clock in the SCN, individual organs and cells outside the SCN rhythmically express core clock genes. These are termed peripheral or extra-SCN tissue-specific clocks. Individual cells contain autonomous clocks; importantly, all cells work in concert to time the occurrence of physiological events optimally. The SCN regulates peripheral clocks both through indirect and direct means. Direct regulation of peripheral processes by the SCN are evoked by neural or humoral signaling (e.g., Mohawk et al., Reference Mohawk, Green and Takahashi2012; Ramanathan et al., Reference Ramanathan, Kathale, Liu, Lee, Freeman, Hogenesch, Cao and Liu2018). Indirectly, the SCN regulates the peripheral clocks via neural and humoral signaling factors, as well as by modulating the expression of circadian clock genes. For example, the SCN regulates secretion of hormonal cues that synchronize extra-SCN clocks, such as melatonin and glucocorticoids. Glucocorticoids are hormones released by the adrenal gland, and act via the glucocorticoid receptor in nearly all cells to regulate gene expression. Upon binding the cytosolic glucocorticoid receptor, the ligand-receptor complex enters the nucleus and binds to glucocorticoid response elements on DNA to activate or repress gene expression. Importantly, at baseline there are circadian rhythms in glucocorticoid levels and several circadian genes have glucocorticoid response elements in their regulatory regions (Reddy et al., Reference Reddy, Maywood, Karp, King, Inoue, Gonzalez, Lilley, Kyriacou and Hastings2007). Application of glucocorticoids to isolated cells can induce Per gene expression and thus serves as an important factor for regulating extra-SCN clocks (Balsalobre et al., Reference Balsalobre, Brown, Marcacci, Tronche, Kellendonk, Reichardt, Schutz and Schibler2000; Fonken et al., Reference Fonken, Frank, Kitt, Barrientos, Watkins and Maier2015).

In addition, physiologic cues coordinate or amplify circadian rhythms in extra-SCN cells; these cues include body temperature, feeding, and activity (Schibler et al., Reference Schibler, Gotic, Saini, Gos, Curie, Emmenegger, Sinturel, Gosselin, Gerber, Fleury-Olela, Rando, Demarque and Franken2015). These neural, humoral, and physiologic factors are sensitive to entrainment by the SCN – but they are also regulated by other systemic factors (S. Zhang et al., Reference Zhang, Dai, Wang, Jiang, Hu, Zhang and Zhang2020).

External events, such as food intake (Damiola et al., Reference Damiola, Le Minh, Preitner, Kornmann, Fleury-Olela and Schibler2000) and physical exercise (Ripperger & Schibler, Reference Ripperger and Schibler2001), can indirectly reset peripheral clock rhythms in the liver and elsewhere (Chen et al., Reference Chen, Feng, Zhang, Dong, Wang, Zhang and Liu2019; Landgraf et al., Reference Landgraf, Tsang, Leliavski, Koch, Barclay, Drucker and Oster2015). For example, restricting food intake to certain times of day (time-restricted feeding or TRF) can uncouple the SCN and extra-SCN clocks (Damiola et al., Reference Damiola, Le Minh, Preitner, Kornmann, Fleury-Olela and Schibler2000). Indeed, timing of food intake strongly regulates the liver clock (Hatori et al., Reference Hatori, Vollmers, Zarrinpar, DiTacchio, Bushong, Gill, Leblanc, Chaix, Joens, Fitzpatrick, Ellisman and Panda2012) as well as cardiovascular function (see Chapter 11). Another mechanism of SCN-mediated peripheral clock regulation is by direct modulation of the autonomic nervous system, as described in Section 1.4.

Importantly, synchronizing clock gene expression in these extra-SCN tissues coordinates transcriptional programming of clock-controlled genes (Mavroudis et al., Reference Mavroudis, DuBois, Almon and Jusko2018). This means that myriad cellular functions are governed by the clock in peripheral tissues and also suggests that, during pathology, these intermediary circadian synchronizers may be susceptible to harmful perturbation that could desynchronize circadian oscillators. The remainder of this chapter will introduce circadian regulation of several major body systems; specific chapters in this book will then review clock disruption-elicited pathology in these systems.

1.4 Circadian Regulation of CNS Function

Central nervous system (CNS) function of animals displays distinct and overlapping circadian rhythms (Chapter 6). Indeed examples of circadian fluctuations in learning and memory, sensation and perception, attention, food intake, mating behaviors, maternal behaviors, aggression, drug and alcohol seeking behaviors, as well as regulation of locomotor activity have been reported (Nelson et al., Reference Nelson, Bumgarner, Walker and DeVries2021). These temporal variations are often overlooked and can significantly affect experimental outcomes. In this section we review some common examples of circadian regulation of CNS function. Notably, disrupted circadian rhythms negatively affect CNS function.

1.4.1 Locomotor Behavior

Early research on circadian rhythms focused on behavior as an output, especially locomotor behavior (Richter, Reference Richter1922). Monitoring of activity cycles is adapted to the species under investigation. For example, small mammals are kept in a cage equipped with a running wheel connected to a counting device that automatically produces a continuous record of the individual’s locomotor activity. The locomotor activity of small birds can be determined by monitoring perch-hopping activities around the clock. Humans can be equipped with electronic smart devices that transmit their locomotor activities to a central monitoring station.

Individuals of species are typically either diurnal or nocturnal in their locomotor activities. As noted, internal clocks display a period of about 24 hours and are set to precisely 24 hours by exposure to light. In the presence of constant lighting conditions (i.e., dim light, bright light, or darkness), locomotor rhythms display a temporal drift from 24 hours that mirrors the internal period (tau) of the circadian clock and is out of phase with the solar day.

Indeed, observing the locomotor activity of a colony of Syrian hamsters (Mesocricetus auratus) led to the discovery of an individual male with a very short tau (~22 hours) when housed in constant dark conditions (Ralph & Menaker, Reference Ralph and Menaker1988). After a return to typical light–dark conditions, this individual displayed aberrant entrainment properties, beginning its locomotor activity about four hours prior to lights out, when hamsters typically begin their activities. This male was mated with three wild-type females with typical taus and, via standard cross-breeding studies, it was revealed that hamsters heterozygous for the mutation displayed periods of about 22 hours, whereas homozygous hamsters displayed locomotor rhythms with taus of about 20 hours. The tau mutant is encoded by casein kinase I epsilon (CKIɛ) and was the first gene identified that was associated with mammalian circadian rhythms (Lowrey et al., Reference Lowrey, Shimomura, Antoch, Yamazaki, Zemenides, Ralph, Menaker and Takahashi2000). Animals display species-specific times of locomotor activity onset that are often linked to the timing of food intake, water consumption, and reproductive behavior, and have been a critical tool for understanding the genetics and other properties of circadian rhythms. Gene expression patterns are temporally similar in both nocturnal and diurnal animals (Challet, Reference Challet2007).

1.4.2 Cognition

There are strong daily rhythms in all aspects of cognition (Fisk et al., Reference Fisk, Tam, Brown, Vyazovskiy, Bannerman and Peirson2018; Schmidt et al., Reference Schmidt, Collette, Cajochen and Peigneux2007; Smarr et al., Reference Smarr, Jennings, Driscoll and Kriegsfeld2014) (Chapter 6). Generally, memory formation peaks during individuals’ active periods. Thus, rats and mice tend to display optimal memory for performance in the Morris water maze during the night, whereas diurnal grass rats display best memory performance during the day (Krishnan & Lyons, Reference Krishnan and Lyons2015; Martin-Fairey & Nunez, Reference Martin-Fairey and Nunez2014).

In rodents, both sensory sensation and perception vary across the day. For example, visual sensation and perception and auditory sensation and perception change across the day in humans and nocturnal rodents (e.g., Basinou et al., Reference Basinou, Park, Cederroth and Canlon2017; Finlay & Sengelaub, Reference Finlay and Sengelaub1981; Meltser et al., Reference Meltser, Cederroth, Basinou, Savelyev, Lundkvist and Canlon2014). Tasks requiring attention display significant circadian fluctuations in both humans (van der Heijden et al., Reference van der Heijden, de Sonneville and Althaus2010) and rodents (Gritton et al., Reference Gritton, Kantorowski, Sarter and Lee2012). These fluctuations appear to reflect circadian changes in cholinergic activities (Hut & Van der Zee, Reference Hut and Van der Zee2011).

1.5 Circadian Regulation of Cardiac Function

Cardiac function is regulated by circadian rhythms (Liu et al., Reference Liu, Walton, DeVries and Nelson2021; Melendez-Fernandez et al., Reference Melendez-Fernandez, Walton, DeVries and Nelson2021; Thosar et al., Reference Thosar, Butler and Shea2018) (Chapter 13). Cardiovascular regulation is associated with sleep–wake patterns (Bastianini et al., Reference Bastianini, Silvani, Berteotti, Martire and Zoccoli2012; Smolensky et al., Reference Smolensky, Hermida, Castriotta and Portaluppi2007) that are linked to underlying circadian rhythms. The circadian regulation of sympathetic and parasympathetic activation modulates heart rate, heart rate variability, blood pressure, vascular tone, and endothelial function (reviewed in Melendez-Fernandez et al., Reference Melendez-Fernandez, Walton, DeVries and Nelson2021). This temporal organization allows the vascular system to produce the necessary factors and mediators, such as prothrombotic and antithrombotic factors, and nitric oxide, at the appropriate time of the day to support activity during the active phase or support recovery and replenishment during the inactive phase. Dysregulation of these circadian fluctuations in cardiac function has been associated with cardiovascular pathology including myocardial infarction, ventricular tachycardia, and sudden cardiac death, which all peak during the early morning (Khan & Ahmad, Reference Khan and Ahmad2003; Manfredini et al., Reference Manfredini, Boari, Salmi, Fabbian, Pala, Tiseo and Portaluppi2013; Muller, Reference Muller1999; Muller et al., Reference Muller, Ludmer, Willich, Tofler, Aylmer, Klangos and Stone1987).

Cells comprising cardiovascular tissue display robust circadian oscillations including vascular smooth muscle, fibroblasts, cardiomyocytes, and cardiac progenitor-like cells, all of which regulate physiological functions including endothelial function, blood pressure, and heart rate (Paschos & FitzGerald, Reference Paschos and FitzGerald2010). Disruption of these rhythms is associated with misalignment of cardiovascular dynamics, including endothelial (Etsuda et al., Reference Etsuda, Takase, Uehata, Kusano, Hamabe, Kuhara, Akima, Matsushima, Arakawa, Satomura, Kurita and Ohsuzu1999), prothrombotic (Takeda et al., Reference Takeda, Maemura, Horie, Oishi, Imai, Harada, Saito, Shiga, Amiya, Manabe, Ishida and Nagai2007), and clotting (Dalby et al., Reference Dalby, Davidson, Burman and Davies2000) factors, which can provoke a pathological response (Rana et al., Reference Rana, Prabhu and Young2020).

Taken together, the available data indicate circadian regulation of the cardiovascular system. Indeed, peripheral clocks and clock genes are expressed in these tissues (Davidson et al., Reference Davidson, London, Block and Menaker2005; Storch et al., Reference Storch, Lipan, Leykin, Viswanathan, Davis, Wong and Weitz2002). Rhythms in vascular function are also observed at the molecular level. RNA sequencing data indicate that 6 percent and 4 percent of protein-coding genes in the heart and aorta, respectively, are transcribed in a circadian fashion (Zhang et al., Reference Zhang, Lahens, Ballance, Hughes and Hogenesch2014). At the cellular level, the core clock genes, including Bmal1, Clock, Per, Cry, and Rev-Erb, serve an important role in maintaining physiological homeostasis of the cardiovascular system. For example, mice with Per2 mutations display reduced nitric oxide production and decreased vasodilatory prostaglandins and elevated vasoconstrictors (Curtis et al., Reference Curtis, Cheng, Kapoor, Reilly, Price and Fitzgerald2007). Cry1/2 deletion leads to salt-sensitive hypertension and increased baroreflex sensitivity in mice (Stow et al., Reference Stow, Richards, Cheng, Lynch, Jeffers, Greenlee, Cain, Wingo and Gumz2012). Given the importance of circadian organization for typical cardiovascular function, the potential of disrupted circadian rhythms for cardiovascular health is dramatic (see Chapter 13).

1.6 Circadian Regulation of Metabolism

Energy acquisition, storage, and utilization are critical for life. Metabolism regulates chemical changes in a cell or organism in order to generate energy or materials needed to grow, reproduce, and function appropriately. The circadian system helps optimize metabolic processes based on distinct metabolic requirements throughout the day to maintain homeostasis. Circadian rhythms in metabolism persist at multiple levels from the function of cellular mitochondria, to hormonal release, to behavioral rhythms in food intake.

Humans and other organisms face distinct metabolic demands based on time of day. A critical aspect of this is that daily behavior is partitioned into an active (wakefulness) and rest (sleep) phase. For understandable reasons, the majority of food intake occurs during an animals active phase, with circadian fluctuations in hunger and appetite contributing to this time of day difference in feeding (Scheer et al., Reference Scheer, Morris and Shea2013). There are also differences in cravings for specific foods based on time of day, with an increased preference for higher caloric foods as the onset of the sleep phase approaches (Scheer et al., Reference Scheer, Morris and Shea2013). This is thought to contribute to the increased risk for obesity and metabolic disorders that occurs in night shift workers – night shift workers are awake and active at a time where their bodies are primed for higher calorie food intake (Bouillon-Minois et al., Reference Bouillon-Minois, Thivel, Croizier, Ajebo, Cambier, Boudet, Adeyemi, Ugbolue, Bagheri, Vallet, Schmidt, Trousselard and Dutheil2022).

Importantly, metabolic regulation is not simply an output of the circadian system. Food intake feeds back on the clock to reinforce rhythms and to adapt physiology to tissue-specific needs. Along with changes in food intake, there are also time-of-day differences in whole body energy expenditure: metabolic rate is reduced during sleep compared to wakefulness (Fraser et al., Reference Fraser, Trinder, Colrain and Montgomery1989). Increases in energy expenditure occur during sleep restriction (although increases in energy expenditure are often countered by increased food intake) (Markwald et al., Reference Markwald, Melanson, Smith, Higgins, Perreault, Eckel and Wright2013; McHill et al., Reference McHill, Melanson, Higgins, Connick, Moehlman, Stothard and Wright2014). However, when humans are sleep restricted and maintained on bed rest, energy expenditure during the typical sleep phase is still lower than during the early active phase (Jung et al., Reference Jung, Melanson, Frydendall, Perreault, Eckel and Wright2011), suggesting the presence of an underlying endogenous rhythm.

Because of the differences in energy intake and expenditure that occur with predictable daily rhythm, there are also rhythms in the underlying hormonal and cellular processes associated with metabolism. Regulation of key metabolic hormones varies throughout the day both due to circadian regulation and as a direct consequence of timing of food intake. For example, because food intake occurs primarily during the active phase, there are increases in most intermediary metabolites including glucose, amino acids, and lipids in the blood during the active phase (reviewed in Reinke & Asher, Reference Reinke and Asher2019). The circadian clock, however, is critical for buffering against excessive fluctuations in metabolic factors. For example, blood glucose is regulated by the circadian system; glucose transporters oscillate in a circadian manner, presumably in anticipation of relative nutrient abundance during the active compared to the inactive phase (Reinke & Asher, Reference Reinke and Asher2019). Circadian function in key tissues and cells that mediate blood glucose are critical. Indeed, disrupting clock function in the liver and pancreas impacts glucose regulation (Lamia et al., Reference Lamia, Storch and Weitz2008; Marcheva et al., Reference Marcheva, Ramsey, Buhr, Kobayashi, Su, Ko, Ivanova, Omura, Mo, Vitaterna, Lopez, Philipson, Bradfield, Crosby, JeBailey, Wang, Takahashi and Bass2010).

Given this tight regulation between the circadian system and metabolism, it follows that disruption of the circadian clock by genetic or environmental means results in metabolic disruption. Susceptibility to diet-induced obesity in a genetic circadian model was first shown in clock mutant mice (Turek et al., Reference Turek, Joshu, Kohsaka, Lin, Ivanova, McDearmon, Laposky, Losee-Olson, Easton, Jensen, Eckel, Takahashi and Bass2005). Subsequently, mutations in many clock linked genes have been associated with metabolic dysfunction (see table 2 in Fonken & Nelson, Reference Fonken and Nelson2014). Environmental circadian disruption in rodent models, including exposure to light at night (Fonken, Aubrecht, et al., Reference Fonken, Aubrecht, Melendez-Fernandez, Weil and Nelson2013; Fonken et al., Reference Fonken, Workman, Walton, Weil, Morris, Haim and Nelson2010; Fonken & Nelson, Reference Fonken and Nelson2013; Fonken, Weil, et al., Reference Fonken, Aubrecht, Melendez-Fernandez, Weil and Nelson2013), constant light (Coomans et al., Reference Coomans, van den Berg, Houben, van Klinken, van den Berg, Pronk, Havekes, Romijn, van Dijk, Biermasz and Meijer2013; Fonken et al., Reference Fonken, Workman, Walton, Weil, Morris, Haim and Nelson2010), simulated shift-work protocols (Barclay et al., Reference Barclay, Husse, Bode, Naujokat, Meyer-Kovac, Schmid, Lehnert and Oster2012; Salgado-Delgado et al., Reference Salgado-Delgado, Saderi, Basualdo Mdel, Guerrero-Vargas, Escobar and Buijs2013), and non-24 hour light cycles (Karatsoreos et al., Reference Karatsoreos, Bhagat, Bloss, Morrison and McEwen2011), are also associated with metabolic dysfunction. Furthermore, humans that are at risk for circadian disruption by engaging in activities such as shift work are at increased risk for developing metabolic syndrome (Pietroiusti et al., Reference Pietroiusti, Neri, Somma, Coppeta, Iavicoli, Bergamaschi and Magrini2010). Perhaps not coincidental, the global obesity epidemic parallels rapid increases in disruptive nighttime light exposure in recent decades. This work is reviewed in Chapter 10. Overall, metabolism and the circadian system are integrally associated.

1.7 Circadian Regulation of Immune Function

The diverse activities in which humans and other animals engage throughout the day come with different risks for encountering pathogens, toxins, and injuries. This suggests that coordinating responses to such threats would also be adaptive, with the immune system representing a major responder. Under healthy conditions, the immune systems may promote a state of anticipation and enhanced vigilance prior to the onset of the active phase, and repair and rejuvenation at the end of the active phase (Curtis et al., Reference Curtis, Bellet, Sassone-Corsi and O’Neill2014).

The immune system differentially responds to challenges based on time of day (Haspel et al., Reference Haspel, Anafi, Brown, Cermakian, Depner, Desplats, Gelman, Haack, Jelic, Kim, Laposky, Lee, Mongodin, Prather, Prendergast, Reardon, Shaw, Sengupta, Szentirmai and Solt2020). For example, exposure to the same E. coli endotoxin challenge during the active versus inactive phase produces striking differences in mortality: rats that receive E. coli endotoxin during their inactive phase exhibit approximately 10 percent mortality versus approximately 80 percent mortality to the exact same dose during the active phase (Halberg et al., Reference Halberg, Johnson, Brown and Bittner1960). Similarly, humans with rheumatoid arthritis show increased pain and inflammatory markers during the nighttime (rest phase) and early morning (Gibbs & Ray, Reference Gibbs and Ray2013; Ingpen, Reference Ingpen1968; Perry et al., Reference Perry, Kirwan, Jessop and Hunt2009). These changes in immune function are associated with direct circadian regulation of immune cells as well as due to circadian regulation of hormones that gate immune responses (e.g., glucocorticoids).

Recent work has illuminated how the circadian system drives healthy daily rhythms in immune responsivity and migration. Every immune cell examined expresses the circadian clockwork necessary for approximately 24 hour rhythms entrained by intermediary oscillators, and these clock genes refine expression of immune-related genes. In mouse macrophages, the clock gene Rev-erba (e.g., Nr1d1) peaks around Zeitgeber time (ZT) 12 (late inactive phase, where ZT represents 24 hours of the day with ZT0 = lights on) (Alexander et al., Reference Alexander, Liou, Knudsen, Starost, Xu, Hyde, Liu, Jacobi, Liao and Lee2020; Gibbs et al., Reference Gibbs, Blaikley, Beesley, Matthews, Simpson, Boyce, Farrow, Else, Singh, Ray and Loudon2012); this transcriptional repressor inhibits expression of the core clock gene Bmal1, while also repressing expression of inflammatory genes. At the nadir of Rev-erb expression – during the active phase – genes with REV-ERB regulatory binding sites are derepressed and are present at higher levels. Thus, REV-ERB provides an example of how a clock-related gene can drive daily oscillations in the functional outputs of immune cells.

Similar daily patterns in expression and reactivity are observed for other clock genes and cell types, respectively. Interestingly, there are also rhythms in immune cell release into blood and extravasation into inflamed tissue: most subsets show highest release and migration in mice during the inactive phase, and Bmal1 deletion in either endothelial cells or leukocyte subsets ablate these migratory rhythms (He et al., Reference He, Holtkamp, Hergenhan, Kraus, de Juan, Weber, Bradfield, Grenier, Pelletier, Druzd, Chen, Ince, Bierschenk, Pick, Sperandio, Aurrand-Lions and Scheiermann2018). The existence of this intrinsic daily rhythm in immunity suggests it may have an adaptive benefit for optimally balancing preparation of immunity for experiencing infection or injury during active phases versus undergoing rejuvenation or repair during rest (Westwood et al., Reference Westwood, O’Donnell, de Bekker, Lively, Zuk and Reece2019).

1.8 How Do We Disrupt the Clock?

As noted, circadian rhythms can be entrained by several external cues, primarily light exposure and food intake; thus, disrupting these entraining cues can perturb circadian regulation of physiology and behavior (Vetter, Reference Vetter2020).

1.8.1 Environmental Lighting

As mentioned, life evolved on Earth with an internal timing system aligned with bright days and dark nights. The invention of electric lighting approximately 150 years ago initiated social and economic revolutions, but also effectively ended completely dark nights (Figure 1.1). Artificial light currently floods the skies with a night glow known as “light pollution.” Light pollution is defined as the alteration of natural night light caused by anthropogenic sources of light (Falchi et al., Reference Falchi, Cinzano, Duriscoe, Kyba, Elvidge, Baugh, Portnov, Rybnikova and Furgoni2016). According to Falchi et al., 80 percent of the world and over 99 percent of Europe and the United States live under polluted night skies. Sources of outdoor artificial light include vehicles, buildings, street and traffic lights, and signs. Of course, light has also been brought indoors; sources of indoor artificial light includes light bulbs, TVs, computer screens, e-books, tablets, phones, and other electronic devices. Incandescent light bulbs initially emitted light of a full spectral composition. Technological advances and ecological concerns have driven the development of more cost- and energy-efficient sources of light, viz., light-emitting diodes (LEDs). The spectral composition of LED lights negatively affect the environment (Gaston et al., Reference Gaston, Visser and Holker2015), as well as circadian rhythms. LEDs emit light spectra with a short-wavelength peak, that, as previously described, coincides with the maximal sensitivity of melanopsin, the primary photopigment that conveys environmental light information to the SCN to entrain circadian rhythms. Activation of this pathway during the evening or night may disrupt the internal cycle of clock gene expression/interactions, reset the circadian clock(s), and lead to disrupted circadian rhythms in humans (Brown et al., Reference Brown, Brainard, Cajochen, Czeisler, Hanifin, Lockley, Lucas, Munch, O’Hagan, Peirson, Price, Roenneberg, Schlangen, Skene, Spitschan, Vetter, Zee and Wright2022) as well as other animals exposed to anthropogenic light pollution (see Chapter 15).

Figure 1.1 Satellite image illustrating nighttime skyglow across the globe.

Credit: NASA Earth Observatory images by Joshua Stevens, using Suomi NPP VIRS data from Miguel Roman, NASA’s Goddard Space Flight Center.

1.8.2 Night Shift Work, Jet Lag, and Social Jetlag

Night shift work, jet lag, and social jet lag all combine altered exposure to light as well as altered timing of food intake; as such, these factors can potently and significantly disrupt circadian rhythms. Night shift work has become common across the globe coincident with increased use of electricity, light at night, and industrial development. Among Americans and Europeans, approximately 15 and 30 percent of the population work night shifts, at least part time (Boivin & Boudreau, Reference Boivin and Boudreau2014). Although many economic and other benefits arise from night shift work, many longitudinal studies have reported that night shift work disrupts circadian rhythms and is associated with negative consequences on health and wellness (e.g., Dutheil et al., Reference Dutheil, Baker, Mermillod, De Cesare, Vidal, Moustafa, Pereira and Navel2020; Hansen, Reference Hansen2017; Q. Zhang et al., Reference Zhang, Chair, Lo, Chau, Schwade and Zhao2020). Use of animal models of night shift work has revealed a causative effect on several diseases (e.g., Arble et al., Reference Arble, Ramsey, Bass and Turek2010; Evans & Davidson, Reference Evans and Davidson2013; IARC Monographs Vol 124 group, 2019).

Another relatively recent technological development that can dysregulate circadian rhythms is travel by jet. Jet travel across four or more time zones induces a syndrome termed jet lag. Jet lag occurs in response to simultaneous shifts in zeitgebers that desynchronize internal circadian rhythms. Symptoms include sleep disruption, disruption of digestive processes, impaired psychological processes, including attention, perception, and motivation, as well as a general feeling of malaise. Most people report that jet lag is worse on eastward compared to westward flights (Herxheimer, Reference Herxheimer2014). However, extensive jet travel and jet lag is relatively uncommon among the general population.

However, a phenomenon termed social jetlag is relatively common among us. Social jet lag is defined as the difference in the time of sleep onset on work days compared to the time of sleep onset on so-called free days (e.g., weekends (Roenneberg et al., Reference Roenneberg, Wirz-Justice and Merrow2003; Sudy et al., Reference Sudy, Ella, Bodizs and Kaldi2019)). Thus, it is common for people to shift their wake–sleep and other circadian rhythms by 3–6 hours in both directions every weekend voluntarily. Both chronic night shift work and social jet lag uncouple central and peripheral clocks and impair physiological and behavioral functioning.

1.9 Conclusions

Billions of years of daily light–dark cycles led to the evolution and refinement of the circadian system. In mammals, the primary pacemakers are the SCN, which help entrain peripheral clocks via secreted cues and direct nervous system input. These cues, in combination with extra-SCN signals, control the timing of molecular clocks in nearly every cell of the body. Molecular clocks also regulate cell-specific processes, leading to circadian regulation of nearly every bodily function – here, we introduced how the circadian system regulates homeostasis throughout the body by regulating the function of major body systems including the CNS, metabolism, the cardiovascular system, and immunity. Circadian regulation of physiology is adaptive, as it optimizes body functions for predictable daily activities during active–inactive cycles. Unfortunately, circadian function in humans and other animals are disrupted by technologies developed over the past 150 years, such as artificial light at night. Overall, the circadian system is an extraordinary and evolutionarily conserved feature of animals on Earth that helps optimize physiology and biological output for the time-of-day. Future research will further explore how the circadian system is interwoven with nearly every bodily system and how this ubiquitous system can be manipulated to improve health and survival of life on Earth.

References

Abrahamson, E. E., & Moore, R. Y. (2001). The posterior hypothalamic area: Chemoarchitecture and afferent connections. Brain Res, 889(1–2), 122.Google Scholar
Albers, H. E., Ferris, C. F., Leeman, S. E., & Goldman, B. D. (1984). Avian pancreatic polypeptide phase shifts hamster circadian rhythms when microinjected into the suprachiasmatic region. Science, 223(4638), 833835.Google Scholar
Albrecht, U., Sun, Z. S., Eichele, G., & Lee, C. C. (1997). A differential response of two putative mammalian circadian regulators, mper1 and mper2, to light. Cell, 91(7), 10551064.Google Scholar
Alexander, R. K., Liou, Y. H., Knudsen, N. H., Starost, K. A., Xu, C., Hyde, A. L., Liu, S., Jacobi, D., Liao, N. S., & Lee, C. H. (2020). Bmal1 integrates mitochondrial metabolism and macrophage activation. Elife, 9, https://doi.org/10.7554/eLife.54090.Google Scholar
Arble, D. M., Ramsey, K. M., Bass, J., & Turek, F. W. (2010). Circadian disruption and metabolic disease: Findings from animal models. Best Pract Res Clin Endocrinol Metab, 24(5), 785800.Google Scholar
Aton, S. J., Colwell, C. S., Harmar, A. J., Waschek, J., & Herzog, E. D. (2005). Vasoactive intestinal polypeptide mediates circadian rhythmicity and synchrony in mammalian clock neurons. Nat Neurosci, 8(4), 476483.Google Scholar
Aton, S. J., & Herzog, E. D. (2005). Come together, right … now: Synchronization of rhythms in a mammalian circadian clock. Neuron, 48(4), 531534.Google Scholar
Balsalobre, A., Brown, S. A., Marcacci, L., Tronche, F., Kellendonk, C., Reichardt, H. M., Schutz, G., & Schibler, U. (2000). Resetting of circadian time in peripheral tissues by glucocorticoid signaling. Science, 289(5488), 23442347.Google Scholar
Barclay, J. L., Husse, J., Bode, B., Naujokat, N., Meyer-Kovac, J., Schmid, S. M., Lehnert, H., & Oster, H. (2012). Circadian desynchrony promotes metabolic disruption in a mouse model of shiftwork. PLoS One, 7(5), e37150.Google Scholar
Basinou, V., Park, J. S., Cederroth, C. R., & Canlon, B. (2017). Circadian regulation of auditory function. Hear Res, 347, 4755.CrossRefGoogle ScholarPubMed
Bastianini, S., Silvani, A., Berteotti, C., Martire, V. L., & Zoccoli, G. (2012). Mice show circadian rhythms of blood pressure during each wake–sleep state. Chronobiol Int, 29(1), 8286.Google Scholar
Beier, C., Zhang, Z., Yurgel, M., & Hattar, S. (2021). Projections of ipRGCs and conventional RGCs to retinorecipient brain nuclei. J Comp Neurol, 529(8), 18631875.Google Scholar
Berson, D. M., Dunn, F. A., & Takao, M. (2002). Phototransduction by retinal ganglion cells that set the circadian clock. Science, 295(5557), 10701073.CrossRefGoogle ScholarPubMed
Boivin, D. B., & Boudreau, P. (2014). Impacts of shift work on sleep and circadian rhythms. Pathol Biol (Paris), 62(5), 292301.CrossRefGoogle ScholarPubMed
Bouillon-Minois, J. B., Thivel, D., Croizier, C., Ajebo, E., Cambier, S., Boudet, G., Adeyemi, O. J., Ugbolue, U. C., Bagheri, R., Vallet, G. T., Schmidt, J., Trousselard, M., & Dutheil, F. (2022 ). The negative impact of night shifts on diet in emergency healthcare workers. Nutrients, 14(4), 829.Google Scholar
Boulos, Z., Rosenwasser, A. M., & Terman, M. (1980). Feeding schedules and the circadian organization of behavior in the rat. Behav Brain Res, 1(1), 3965.CrossRefGoogle ScholarPubMed
Brainard, G. C., Hanifin, J. P., Greeson, J. M., Byrne, B., Glickman, G., Gerner, E., & Rollag, M. D. (2001). Action spectrum for melatonin regulation in humans: Evidence for a novel circadian photoreceptor. J Neurosci, 21(16), 64056412.Google Scholar
Brown, T. M., Brainard, G. C., Cajochen, C., Czeisler, C. A., Hanifin, J. P., Lockley, S. W., Lucas, R. J., Munch, M., O’Hagan, J. B., Peirson, S. N., Price, L. L. A., Roenneberg, T., Schlangen, L. J. M., Skene, D. J., Spitschan, M., Vetter, C., Zee, P. C., & Wright, K. P. Jr. (2022). Recommendations for daytime, evening, and nighttime indoor light exposure to best support physiology, sleep, and wakefulness in healthy adults. PLoS Biol, 20(3), e3001571.Google Scholar
Bunger, M. K., Wilsbacher, L. D., Moran, S. M., Clendenin, C., Radcliffe, L. A., Hogenesch, J. B., Simon, M. C., Takahashi, J. S., & Bradfield, C. A. (2000). Mop3 is an essential component of the master circadian pacemaker in mammals. Cell, 103(7), 10091017.CrossRefGoogle ScholarPubMed
Challet, E. (2007). Minireview: Entrainment of the suprachiasmatic clockwork in diurnal and nocturnal mammals. Endocrinology, 148(12), 56485655.Google Scholar
Chang, A. M., Aeschbach, D., Duffy, J. F., & Czeisler, C. A. (2015). Evening use of light-emitting eReaders negatively affects sleep, circadian timing, and next-morning alertness. Proc Natl Acad Sci USA, 112, 12321237.Google Scholar
Chen, S., Feng, M., Zhang, S., Dong, Z., Wang, Y., Zhang, W., & Liu, C. (2019). Angptl8 mediates food-driven resetting of hepatic circadian clock in mice. Nat Commun, 10(1), 3518.Google Scholar
Colwell, C. S., Michel, S., Itri, J., Rodriguez, W., Tam, J., Lelievre, V., Hu, Z., Liu, X., & Waschek, J. A. (2003). Disrupted circadian rhythms in VIP- and PHI-deficient mice. Am J Physiol Regul Integr Comp Physiol, 285(5), R939R949.Google Scholar
Coomans, C. P., van den Berg, S. A., Houben, T., van Klinken, J. B., van den Berg, R., Pronk, A. C., Havekes, L. M., Romijn, J. A., van Dijk, K. W., Biermasz, N. R., & Meijer, J. H. (2013 ). Detrimental effects of constant light exposure and high-fat diet on circadian energy metabolism and insulin sensitivity. Faseb J, 27(4), 17211732.Google Scholar
Cox, K. H., & Takahashi, J. S. (2019). Circadian clock genes and the transcriptional architecture of the clock mechanism. J Mol Endocrinol, 63(4), R93R102.Google Scholar
Curtis, A. M., Bellet, M. M., Sassone-Corsi, P., & O’Neill, L. A. (2014). Circadian clock proteins and immunity. Immunity, 40(2), 178186.Google Scholar
Curtis, A. M., Cheng, Y., Kapoor, S., Reilly, D., Price, T. S., & Fitzgerald, G. A. (2007). Circadian variation of blood pressure and the vascular response to asynchronous stress. Proc Natl Acad Sci USA, 104(9), 34503455.Google Scholar
Czeisler, C. A., Duffy, J. F., Shanahan, T. L., Brown, E. N., Mitchell, J. F., Rimmer, D. W., Ronda, J. M., Silva, E. J., Allan, J. S., Emens, J. S., Dijk, D. J., & Kronauer, R. E. (1999). Stability, precision, and near-24-hour period of the human circadian pacemaker. Science, 284(5423), 21772181.Google Scholar
Czeisler, C. A., Shanahan, T. L., Klerman, E. B., Martens, H., Brotman, D. J., Emens, J. S., Klein, T., & Rizzo, J. F. (1995). Suppression of melatonin secretion in some blind patients by exposure to bright light [see comments]. N Engl J Med, 332, 611.Google Scholar
Dalby, M. C., Davidson, S. J., Burman, J. F., & Davies, S. W. (2000). Diurnal variation in platelet aggregation with the PFA-100 platelet function analyser. Platelets, 11(6), 320324.Google Scholar
Damiola, F., Le Minh, N., Preitner, N., Kornmann, B., Fleury-Olela, F., & Schibler, U. (2000). Restricted feeding uncouples circadian oscillators in peripheral tissues from the central pacemaker in the suprachiasmatic nucleus. Genes Dev, 14(23), 29502961.Google Scholar
Davidson, A. J., London, B., Block, G. D., & Menaker, M. (2005). Cardiovascular tissues contain independent circadian clocks. Clin Exp Hypertens, 27(2–3), 307311.Google Scholar
Ding, J. M., Faiman, L. E., Hurst, W. J., Kuriashkina, L. R., & Gillette, M. U. (1997). Resetting the biological clock: Mediation of nocturnal CREB phosphorylation via light, glutamate, and nitric oxide. J Neurosci, 17(2), 667675.Google Scholar
Do, M. T. H. (2019). Melanopsin and the intrinsically photosensitive retinal ganglion cells: Biophysics to behavior. Neuron, 104(2), 205226.Google Scholar
Dutheil, F., Baker, J. S., Mermillod, M., De Cesare, M., Vidal, A., Moustafa, F., Pereira, B., & Navel, V. (2020). Shift work, and particularly permanent night shifts, promote dyslipidaemia: A systematic review and meta-analysis. Atherosclerosis, 313, 156169.CrossRefGoogle ScholarPubMed
Edgar, D. M., & Dement, W. C. (1991). Regularly scheduled voluntary exercise synchronizes the mouse circadian clock. Am J Physiol, 261(4 Pt 2), R928R933.Google Scholar
Etsuda, H., Takase, B., Uehata, A., Kusano, H., Hamabe, A., Kuhara, R., Akima, T., Matsushima, Y., Arakawa, K., Satomura, K., Kurita, A., & Ohsuzu, F. (1999). Morning attenuation of endothelium-dependent, flow-mediated dilation in healthy young men: Possible connection to morning peak of cardiac events? Clin Cardiol, 22(6), 417421.CrossRefGoogle ScholarPubMed
Evans, J. A., & Davidson, A. J. (2013). Health consequences of circadian disruption in humans and animal models. Prog Mol Biol Transl Sci, 119, 283323.Google Scholar
Falchi, F., Cinzano, P., Duriscoe, D., Kyba, C. C., Elvidge, C. D., Baugh, K., Portnov, B. A., Rybnikova, N. A., & Furgoni, R. (2016). The new world atlas of artificial night sky brightness. Sci Adv, 2(6), e1600377.Google Scholar
Fernandez, D. C., Chang, Y. T., Hattar, S., & Chen, S. K. (2016). Architecture of retinal projections to the central circadian pacemaker. Proc Natl Acad Sci USA, 113(21), 60476052.Google Scholar
Finlay, B. L., & Sengelaub, D. R. (1981). Toward a neuroethology of mammalian vision: Ecology and anatomy of rodent visuomotor behavior. Behav Brain Res, 3(2), 133149.Google Scholar
Fisk, A. S., Tam, S. K. E., Brown, L. A., Vyazovskiy, V. V., Bannerman, D. M., & Peirson, S. N. (2018). Light and cognition: Roles for circadian rhythms, sleep, and arousal. Front Neurol, 9, 56.Google Scholar
Fonken, L. K., Aubrecht, T. G., Melendez-Fernandez, O. H., Weil, Z. M., & Nelson, R. J. (2013). Dim light at night disrupts molecular circadian rhythms and increases body weight. J Biol Rhythms, 28(4), 262271.CrossRefGoogle ScholarPubMed
Fonken, L. K., Frank, M. G., Kitt, M. M., Barrientos, R. M., Watkins, L. R., & Maier, S. F. (2015). Microglia inflammatory responses are controlled by an intrinsic circadian clock. Brain Behav Immun, 45, 171179.CrossRefGoogle ScholarPubMed
Fonken, L. K., & Nelson, R. J. (2013). Dim light at night increases depressive-like responses in male C3H/HeNHsd mice. Behav Brain Res, 243, 7478.CrossRefGoogle ScholarPubMed
Fonken, L. K., & Nelson, R. J. (2014). The effects of light at night on circadian clocks and metabolism. Endocr Rev, 35(4), 648670.Google Scholar
Fonken, L. K., Weil, Z. M., & Nelson, R. J. (2013). Dark nights reverse metabolic disruption caused by dim light at night. Obesity (Silver Spring), 21(6), 11591164.Google Scholar
Fonken, L. K., Workman, J. L., Walton, J. C., Weil, Z. M., Morris, J. S., Haim, A., & Nelson, R. J. (2010). Light at night increases body mass by shifting the time of food intake. Proc Natl Acad Sci USA, 107(43), 1866418669.Google Scholar
Fraser, G., Trinder, J., Colrain, I. M., & Montgomery, I. (1989). Effect of sleep and circadian cycle on sleep period energy expenditure. J Appl Physiol (1985), 66(2), 830836.Google Scholar
Gaston, K. J., Visser, M. E., & Holker, F. (2015). The biological impacts of artificial light at night: The research challenge. Philosophical Transactions of the Royal Society B, 370, 20140133.Google Scholar
Gau, D., Lemberger, T., von Gall, C., Kretz, O., Le Minh, N., Gass, P., Schmid, W., Schibler, U., Korf, H. W., & Schutz, G. (2002). Phosphorylation of CREB Ser142 regulates light-induced phase shifts of the circadian clock. Neuron, 34(2), 245253.Google Scholar
Gekakis, N., Staknis, D., Nguyen, H. B., Davis, F. C., Wilsbacher, L. D., King, D. P., Takahashi, J. S., & Weitz, C. J. (1998). Role of the CLOCK protein in the mammalian circadian mechanism. Science, 280(5369), 15641569.CrossRefGoogle ScholarPubMed
Gibbs, J. E., Blaikley, J., Beesley, S., Matthews, L., Simpson, K. D., Boyce, S. H., Farrow, S. N., Else, K. J., Singh, D., Ray, D. W., & Loudon, A. S. (2012). The nuclear receptor REV-ERBalpha mediates circadian regulation of innate immunity through selective regulation of inflammatory cytokines. Proc Natl Acad Sci USA, 109(2), 582587.CrossRefGoogle ScholarPubMed
Gibbs, J. E., & Ray, D. W. (2013). The role of the circadian clock in rheumatoid arthritis. Arthritis Res Ther, 15(1), 205.CrossRefGoogle ScholarPubMed
Ginty, D. D., Kornhauser, J. M., Thompson, M. A., Bading, H., Mayo, K. E., Takahashi, J. S., & Greenberg, M. E. (1993). Regulation of CREB phosphorylation in the suprachiasmatic nucleus by light and a circadian clock. Science, 260(5105), 238241.Google Scholar
Griffin, E. A. Jr., Staknis, D., & Weitz, C. J. (1999). Light-independent role of CRY1 and CRY2 in the mammalian circadian clock. Science, 286(5440), 768771.Google Scholar
Gritton, H. J., Kantorowski, A., Sarter, M., & Lee, T. M. (2012). Bidirectional interactions between circadian entrainment and cognitive performance. Learn Mem, 19(3), 126141.Google Scholar
Halberg, F., Johnson, E. A., Brown, B. W., & Bittner, J. J. (1960). Susceptibility rhythm to E. coli endotoxin and bioassay. Proc Soc Exp Biol Med, 103, 142144.Google Scholar
Hanifin, J. P., Lockley, S. W., Cecil, K., West, K., Jablonski, M., Warfield, B., James, M., Ayers, M., Byrne, B., Gerner, E., Pineda, C., Rollag, M., & Brainard, G. C. (2019). Randomized trial of polychromatic blue-enriched light for circadian phase shifting, melatonin suppression, and alerting responses. Physiol Behav, 198, 5766.Google Scholar
Hannibal, J., Hindersson, P., Knudsen, S. M., Georg, B., & Fahrenkrug, J. (2002). The photopigment melanopsin is exclusively present in pituitary adenylate cyclase-activating polypeptide-containing retinal ganglion cells of the retinohypothalamic tract. J Neurosci, 22(1), RC191.Google Scholar
Hansen, J. (2017). Night shift work and risk of breast cancer. Curr Environ Health Rep, 4(3), 325339.CrossRefGoogle ScholarPubMed
Harmar, A. J., Marston, H. M., Shen, S., Spratt, C., West, K. M., Sheward, W. J., Morrison, C. F., Dorin, J. R., Piggins, H. D., Reubi, J. C., Kelly, J. S., Maywood, E. S., & Hastings, M. H. (2002). The VPAC(2) receptor is essential for circadian function in the mouse suprachiasmatic nuclei. Cell, 109(4), 497508.CrossRefGoogle ScholarPubMed
Haspel, J. A., Anafi, R., Brown, M. K., Cermakian, N., Depner, C., Desplats, P., Gelman, A. E., Haack, M., Jelic, S., Kim, B. S., Laposky, A. D., Lee, Y. C., Mongodin, E., Prather, A. A., Prendergast, B. J., Reardon, C., Shaw, A. C., Sengupta, S., Szentirmai, E., … Solt, L. A. (2020). Perfect timing: Circadian rhythms, sleep, and immunity: An NIH workshop summary. JCI Insight, 5(1).Google Scholar
Hatori, M., Vollmers, C., Zarrinpar, A., DiTacchio, L., Bushong, E. A., Gill, S., Leblanc, M., Chaix, A., Joens, M., Fitzpatrick, J. A., Ellisman, M. H., & Panda, S. (2012). Time-restricted feeding without reducing caloric intake prevents metabolic diseases in mice fed a high-fat diet. Cell Metab, 15(6), 848860.Google Scholar
Hattar, S., Kumar, M., Park, A., Tong, P., Tung, J., Yau, K. W., & Berson, D. M. (2006). Central projections of melanopsin-expressing retinal ganglion cells in the mouse [Comparative Study Research Support, N.I.H., Extramural]. J Comp Neurol, 497(3), 326349.CrossRefGoogle ScholarPubMed
Hattar, S., Lucas, R. J., Mrosovsky, N., Thompson, S., Douglas, R. H., Hankins, M. W., Lem, J., Biel, M., Hofmann, F., Foster, R. G., & Yau, K. W. (2003). Melanopsin and rod-cone photoreceptive systems account for all major accessory visual functions in mice. Nature, 424(6944), 7681.Google Scholar
He, W., Holtkamp, S., Hergenhan, S. M., Kraus, K., de Juan, A., Weber, J., Bradfield, P., Grenier, J. M. P., Pelletier, J., Druzd, D., Chen, C. S., Ince, L. M., Bierschenk, S., Pick, R., Sperandio, M., Aurrand-Lions, M., & Scheiermann, C. (2018). Circadian expression of migratory factors establishes lineage-specific signatures that guide the homing of leukocyte subsets to tissues. Immunity, 49(6), 11751190.Google Scholar
van der Heijden, K. B., de Sonneville, L. M., & Althaus, M. (2010). Time-of-day effects on cognition in preadolescents: A trails study. Chronobiol Int, 27(9–10), 18701894.Google Scholar
Herxheimer, A. (2014). Jet lag. BMJ Clin Evid, 2014, 2303.Google Scholar
Hogenesch, J. B., Gu, Y. Z., Jain, S., & Bradfield, C. A. (1998). The basic-helix-loop-helix-PAS orphan MOP3 forms transcriptionally active complexes with circadian and hypoxia factors. Proc Natl Acad Sci USA, 95(10), 54745479.Google Scholar
Hut, R. A., & Van der Zee, E. A. (2011). The cholinergic system, circadian rhythmicity, and time memory. Behav Brain Res, 221(2), 466480.CrossRefGoogle ScholarPubMed
IARC Monographs Vol 124 group. (2019). Carcinogenicity of night shift work. Lancet Oncol, 20(8), 10581059.Google Scholar
Ingpen, M. L. (1968). The quantitative measurement of joint changes in rheumatoid arthritis. Ann Phys Med, 9(8), 322327.Google Scholar
Jin, X., Shearman, L. P., Weaver, D. R., Zylka, M. J., de Vries, G. J., & Reppert, S. M. (1999). A molecular mechanism regulating rhythmic output from the suprachiasmatic circadian clock. Cell, 96(1), 5768.Google Scholar
Jones, S. E., Lane, J. M., Wood, A. R., van Hees, V. T., Tyrrell, J., Beaumont, R. N., Jeffries, A. R., Dashti, H. S., Hillsdon, M., Ruth, K. S., Tuke, M. A., Yaghootkar, H., Sharp, S. A., Jie, Y., Thompson, W. D., Harrison, J. W., Dawes, A., Byrne, E. M., Tiemeier, H., … Weedon, M. N. (2019). Genome-wide association analyses of chronotype in 697,828 individuals provides insights into circadian rhythms. Nat Commun, 10(1), 343.Google Scholar
Jung, C. M., Melanson, E. L., Frydendall, E. J., Perreault, L., Eckel, R. H., & Wright, K. P. (2011). Energy expenditure during sleep, sleep deprivation and sleep following sleep deprivation in adult humans. J Physiol, 589(Pt 1), 235244.Google Scholar
Karatsoreos, I. N., Bhagat, S., Bloss, E. B., Morrison, J. H., & McEwen, B. S. (2011). Disruption of circadian clocks has ramifications for metabolism, brain, and behavior. Proc Natl Acad Sci USA, 108(4), 16571662.Google Scholar
Khan, M. S., & Ahmad, S. I. (2003). Circadian variation: Increased morning incidence of acute myocardial infarction in patients with coronary artery disease. J Pak Med Assoc, 53(2), 8487.Google Scholar
Krishnan, H. C., & Lyons, L. C. (2015). Synchrony and desynchrony in circadian clocks: Impacts on learning and memory. Learn Mem, 22(9), 426437.Google Scholar
Kume, K., Zylka, M. J., Sriram, S., Shearman, L. P., Weaver, D. R., Jin, X., Maywood, E. S., Hastings, M. H., & Reppert, S. M. (1999). mCRY1 and mCRY2 are essential components of the negative limb of the circadian clock feedback loop. Cell, 98(2), 193205.Google Scholar
Lamia, K. A., Storch, K. F., & Weitz, C. J. (2008). Physiological significance of a peripheral tissue circadian clock. Proc Natl Acad Sci USA, 105(39), 1517215177.Google Scholar
Landgraf, D., Tsang, A. H., Leliavski, A., Koch, C. E., Barclay, J. L., Drucker, D. J., & Oster, H. (2015). Oxyntomodulin regulates resetting of the liver circadian clock by food. Elife, 4, e06253.Google Scholar
Leak, R. K., & Moore, R. Y. (2001). Topographic organization of suprachiasmatic nucleus projection neurons. J Comp Neurol, 433(3), 312334.Google Scholar
Lee, C., Etchegaray, J. P., Cagampang, F. R., Loudon, A. S., & Reppert, S. M. (2001). Posttranslational mechanisms regulate the mammalian circadian clock. Cell, 107(7), 855867.Google Scholar
Liu, J. A., Walton, J. C., DeVries, A. C., & Nelson, R. J. (2021). Disruptions of circadian rhythms and thrombolytic therapy during ischemic stroke intervention. Front Neurosci, 15, 675732.CrossRefGoogle ScholarPubMed
Lowrey, P. L., Shimomura, K., Antoch, M. P., Yamazaki, S., Zemenides, P. D., Ralph, M. R., Menaker, M., & Takahashi, J. S. (2000). Positional syntenic cloning and functional characterization of the mammalian circadian mutation tau. Science, 288(5465), 483492.Google Scholar
Manfredini, R., Boari, B., Salmi, R., Fabbian, F., Pala, M., Tiseo, R., & Portaluppi, F. (2013). Twenty-four-hour patterns in occurrence and pathophysiology of acute cardiovascular events and ischemic heart disease. Chronobiol Int, 30(1–2), 616.Google Scholar
Marcheva, B., Ramsey, K. M., Buhr, E. D., Kobayashi, Y., Su, H., Ko, C. H., Ivanova, G., Omura, C., Mo, S., Vitaterna, M. H., Lopez, J. P., Philipson, L. H., Bradfield, C. A., Crosby, S. D., JeBailey, L., Wang, X. Z., Takahashi, J. S., & Bass, J. (2010). Disruption of the clock components CLOCK and BMAL1 leads to hypoinsulinaemia and diabetes. Nature, 466(7306), 627631.Google Scholar
Markwald, R. R., Melanson, E. L., Smith, M. R., Higgins, J., Perreault, L., Eckel, R. H., & Wright, K. P. Jr. (2013). Impact of insufficient sleep on total daily energy expenditure, food intake, and weight gain. Proc Natl Acad Sci USA, 110(14), 56955700.Google Scholar
Martin-Fairey, C. A., & Nunez, A. A. (2014). Circadian modulation of memory and plasticity gene products in a diurnal species. Brain Res, 1581, 3039.CrossRefGoogle Scholar
Mavroudis, P. D., DuBois, D. C., Almon, R. R., & Jusko, W. J. (2018). Modeling circadian variability of core-clock and clock-controlled genes in four tissues of the rat. PLoS One, 13(6), e0197534.Google Scholar
Maywood, E. S., Chesham, J. E., O’Brien, J. A., & Hastings, M. H. (2011). A diversity of paracrine signals sustains molecular circadian cycling in suprachiasmatic nucleus circuits. Proc Natl Acad Sci USA, 108(34), 1430614311.Google Scholar
McHill, A. W., Melanson, E. L., Higgins, J., Connick, E., Moehlman, T. M., Stothard, E. R., & Wright, K. P. Jr. (2014). Impact of circadian misalignment on energy metabolism during simulated nightshift work. Proc Natl Acad Sci USA, 111(48), 1730217307.CrossRefGoogle ScholarPubMed
Melendez-Fernandez, O. H., Walton, J. C., DeVries, A. C., & Nelson, R. J. (2021). Clocks, rhythms, sex, and hearts: How disrupted circadian rhythms, time-of-day, and sex influence cardiovascular health. Biomolecules, 11(6), 883.Google Scholar
Meltser, I., Cederroth, C. R., Basinou, V., Savelyev, S., Lundkvist, G. S., & Canlon, B. (2014). TrkB-mediated protection against circadian sensitivity to noise trauma in the murine cochlea. Curr Biol, 24(6), 658663.Google Scholar
Mohawk, J. A., Green, C. B., & Takahashi, J. S. (2012). Central and peripheral circadian clocks in mammals. Annu Rev Neurosci, 35, 445462.Google Scholar
Moore, R. Y., & Eichler, V. B. (1972). Loss of a circadian adrenal corticosterone rhythm following suprachiasmatic lesions in the rat. Brain Res, 42(1), 201206.Google Scholar
Moore, R. Y., & Qavi, H. B. (1971). Circadian rhythm in adrenal adenyl cyclase and corticosterone abolished by medial forebrain bundle transection in the rat. Experientia, 27(3), 249250.Google Scholar
Moore, R. Y., Speh, J. C., & Leak, R. K. (2002). Suprachiasmatic nucleus organization. Cell Tissue Res, 309(1), 8998.Google Scholar
Mrosovsky, N., Lucas, R. J., & Foster, R. G. (2001). Persistence of masking responses to light in mice lacking rods and cones. J Biol Rhythms, 16(6), 585588.CrossRefGoogle ScholarPubMed
Muller, J. E. (1999 ). Circadian variation and triggering of acute coronary events. Am Heart J, 137(4 Pt 2), S1S8.Google Scholar
Muller, J. E., Ludmer, P. L., Willich, S. N., Tofler, G. H., Aylmer, G., Klangos, I., & Stone, P. H. (1987). Circadian variation in the frequency of sudden cardiac death. Circulation, 75(1), 131138.CrossRefGoogle ScholarPubMed
Nelson, R. J., Bumgarner, J. R., Walker, W. H., 2nd, & DeVries, A. C. (2021 ). Time-of-day as a critical biological variable. Neurosci Biobehav Rev, 127, 740746.CrossRefGoogle ScholarPubMed
Paschos, G. K., & FitzGerald, G. A. (2010). Circadian clocks and vascular function. Circ Res, 106(5), 833841.Google Scholar
Patton, A. P., & Hastings, M. H. (2018). The suprachiasmatic nucleus. Curr Biol, 28(15), R816R822.Google Scholar
Paul, M. J., Indic, P., & Schwartz, W. J. (2015). Social synchronization of circadian rhythmicity in female mice depends on the number of cohabiting animals. Biol Lett, 11(6), 20150204.Google Scholar
Perry, M. G., Kirwan, J. R., Jessop, D. S., & Hunt, L. P. (2009). Overnight variations in cortisol, interleukin 6, tumour necrosis factor alpha and other cytokines in people with rheumatoid arthritis. Ann Rheum Dis, 68(1), 6368.Google Scholar
Pietroiusti, A., Neri, A., Somma, G., Coppeta, L., Iavicoli, I., Bergamaschi, A., & Magrini, A. (2010). Incidence of metabolic syndrome among night-shift healthcare workers. Occup Environ Med, 67(1), 5457.Google Scholar
Preitner, N., Damiola, F., Lopez-Molina, L., Zakany, J., Duboule, D., Albrecht, U., & Schibler, U. (2002). The orphan nuclear receptor REV-ERBalpha controls circadian transcription within the positive limb of the mammalian circadian oscillator. Cell, 110(2), 251260.Google Scholar
Provencio, I., Rollag, M. D., & Castrucci, A. M. (2002). Photoreceptive net in the mammalian retina. This mesh of cells may explain how some blind mice can still tell day from night. Nature, 415(6871), 493.Google Scholar
Ralph, M. R., & Menaker, M. (1988). A mutation of the circadian system in golden hamsters. Science, 241, 12251227.CrossRefGoogle ScholarPubMed
Ramanathan, C., Kathale, N. D., Liu, D., Lee, C., Freeman, D. A., Hogenesch, J. B., Cao, R., & Liu, A. C. (2018). mTOR signaling regulates central and peripheral circadian clock function. PLoS Genet, 14(5), e1007369.Google Scholar
Rana, S., Prabhu, S. D., & Young, M. E. (2020). Chronobiological influence over cardiovascular function: The good, the bad, and the ugly. Circ Res, 126(2), 258279.Google Scholar
Reddy, A. B., Maywood, E. S., Karp, N. A., King, V. M., Inoue, Y., Gonzalez, F. J., Lilley, K. S., Kyriacou, C. P., & Hastings, M. H. (2007). Glucocorticoid signaling synchronizes the liver circadian transcriptome. Hepatology, 45(6), 14781488.Google Scholar
Reinke, H., & Asher, G. (2019). Crosstalk between metabolism and circadian clocks. Nat Rev Mol Cell Biol, 20(4), 227241.Google Scholar
Richter, C. P. (1922). A behavioristic study of the activity of the rat. Compar Psychol Monogr, 1, 155.Google Scholar
Ripperger, J. A., & Schibler, U. (2001). Circadian regulation of gene expression in animals. Curr Opin Cell Biol, 13(3), 357362.Google Scholar
Roenneberg, T., Wirz-Justice, A., & Merrow, M. (2003). Life between clocks: Daily temporal patterns of human chronotypes. J Biol Rhythms, 18(1), 8090.Google Scholar
Rusak, B., & Groos, G. (1982). Suprachiasmatic stimulation phase shifts rodent circadian rhythms. Science, 215(4538), 14071409.Google Scholar
Salgado-Delgado, R. C., Saderi, N., Basualdo Mdel, C., Guerrero-Vargas, N. N., Escobar, C., & Buijs, R. M. (2013). Shift work or food intake during the rest phase promotes metabolic disruption and desynchrony of liver genes in male rats. PLoS One, 8(4), e60052.Google Scholar
Scheer, F. A., Morris, C. J., & Shea, S. A. (2013). The internal circadian clock increases hunger and appetite in the evening independent of food intake and other behaviors. Obesity (Silver Spring), 21(3), 421423.Google Scholar
Schibler, U., Gotic, I., Saini, C., Gos, P., Curie, T., Emmenegger, Y., Sinturel, F., Gosselin, P., Gerber, A., Fleury-Olela, F., Rando, G., Demarque, M., & Franken, P. (2015). Clock-talk: Interactions between central and peripheral circadian oscillators in mammals. Cold Spring Harb Symp Quant Biol, 80, 223232.Google Scholar
Schmidt, C., Collette, F., Cajochen, C., & Peigneux, P. (2007, Oct). A time to think: Circadian rhythms in human cognition. Cogn Neuropsychol, 24(7), 755789.Google Scholar
Schurov, I. L., McNulty, S., Best, J. D., Sloper, P. J., & Hastings, M. H. (1999). Glutamatergic induction of CREB phosphorylation and Fos expression in primary cultures of the suprachiasmatic hypothalamus in vitro is mediated by co-ordinate activity of NMDA and non-NMDA receptors. J Neuroendocrinol, 11(1), 4351.Google Scholar
Silver, R., LeSauter, J., Tresco, P. A., & Lehman, M. N. (1996). A diffusible coupling signal from the transplanted suprachiasmatic nucleus controlling circadian locomotor rhythms. Nature, 382(6594), 810813.Google Scholar
Smarr, B. L., Jennings, K. J., Driscoll, J. R., & Kriegsfeld, L. J. (2014). A time to remember: The role of circadian clocks in learning and memory. Behav Neurosci, 128(3), 283303.Google Scholar
Smolensky, M. H., Hermida, R. C., Castriotta, R. J., & Portaluppi, F. (2007). Role of sleep–wake cycle on blood pressure circadian rhythms and hypertension. Sleep Med, 8(6), 668680.Google Scholar
Stephan, F. K., & Zucker, I. (1972). Circadian rhythms in drinking behavior and locomotor activity of rats are eliminated by hypothalamic lesions. Proc Natl Acad Sci USA, 69(6), 15831586.Google Scholar
Storch, K. F., Lipan, O., Leykin, I., Viswanathan, N., Davis, F. C., Wong, W. H., & Weitz, C. J. (2002). Extensive and divergent circadian gene expression in liver and heart. Nature, 417(6884), 7883.Google Scholar
Stow, L. R., Richards, J., Cheng, K. Y., Lynch, I. J., Jeffers, L. A., Greenlee, M. M., Cain, B. D., Wingo, C. S., & Gumz, M. L. (2012). The circadian protein period 1 contributes to blood pressure control and coordinately regulates renal sodium transport genes. Hypertension, 59(6), 11511156.Google Scholar
Sudy, A. R., Ella, K., Bodizs, R., & Kaldi, K. (2019). Association of social jetlag with sleep quality and autonomic cardiac control during sleep in young healthy men. Front Neurosci, 13, 950.Google Scholar
Takahashi, J. S., DeCoursey, P. J., Bauman, L., & Menaker, M. (1984). Spectral sensitivity of a novel photoreceptive system mediating entrainment of mammalian circadian rhythms. Nature, 308(5955), 186188.CrossRefGoogle ScholarPubMed
Takeda, N., Maemura, K., Horie, S., Oishi, K., Imai, Y., Harada, T., Saito, T., Shiga, T., Amiya, E., Manabe, I., Ishida, N., & Nagai, R. (2007). Thrombomodulin is a clock-controlled gene in vascular endothelial cells. J Biol Chem, 282(45), 3256132567.Google Scholar
Thosar, S. S., Butler, M. P., & Shea, S. A. (2018). Role of the circadian system in cardiovascular disease. J Clin Invest, 128(6), 21572167.CrossRefGoogle ScholarPubMed
Turek, F. W., Joshu, C., Kohsaka, A., Lin, E., Ivanova, G., McDearmon, E., Laposky, A., Losee-Olson, S., Easton, A., Jensen, D. R., Eckel, R. H., Takahashi, J. S., & Bass, J. (2005). Obesity and metabolic syndrome in circadian clock mutant mice. Science, 308(5724), 10431045.Google Scholar
Vetter, C. (2020). Circadian disruption: What do we actually mean? Eur J Neurosci, 51(1), 531550.Google Scholar
Vitaterna, M. H., King, D. P., Chang, A. M., Kornhauser, J. M., Lowrey, P. L., McDonald, J. D., Dove, W. F., Pinto, L. H., Turek, F. W., & Takahashi, J. S. (1994). Mutagenesis and mapping of a mouse gene, clock, essential for circadian behavior. Science, 264(5159), 719725.Google Scholar
Weaver, D. R. (1998). The suprachiasmatic nucleus: A 25-year retrospective. J Biol Rhythms, 13(2), 100112.Google Scholar
Welsh, D. K., Logothetis, D. E., Meister, M., & Reppert, S. M. (1995). Individual neurons dissociated from rat suprachiasmatic nucleus express independently phased circadian firing rhythms. Neuron, 14(4), 697706.Google Scholar
West, K. E., Jablonski, M. R., Warfield, B., Cecil, K. S., James, M., Ayers, M. A., Maida, J., Bowen, C., Sliney, D. H., Rollag, M. D., Hanifin, J. P., & Brainard, G. C. (2011). Blue light from light-emitting diodes elicits a dose-dependent suppression of melatonin in humans. J Appl Physiol (1985), 110(3), 619626.Google Scholar
Westwood, M. L., O’Donnell, A. J., de Bekker, C., Lively, C. M., Zuk, M., & Reece, S. E. (2019). The evolutionary ecology of circadian rhythms in infection. Nat Ecol Evol, 3(4), 552560.Google Scholar
Yamazaki, S., Numano, R., Abe, M., Hida, A., Takahashi, R., Ueda, M., Block, G. D., Sakaki, Y., Menaker, M., & Tei, H. (2000). Resetting central and peripheral circadian oscillators in transgenic rats. Science, 288(5466), 682685.Google Scholar
Yoo, S. H., Yamazaki, S., Lowrey, P. L., Shimomura, K., Ko, C. H., Buhr, E. D., Siepka, S. M., Hong, H. K., Oh, W. J., Yoo, O. J., Menaker, M., & Takahashi, J. S. (2004). PERIOD2::LUCIFERASE real-time reporting of circadian dynamics reveals persistent circadian oscillations in mouse peripheral tissues. Proc Natl Acad Sci USA, 101(15), 53395346.Google Scholar
Zhang, Q., Chair, S. Y., Lo, S. H. S., Chau, J. P., Schwade, M., & Zhao, X. (2020). Association between shift work and obesity among nurses: A systematic review and meta-analysis. Int J Nurs Stud, 112, 103757.Google Scholar
Zhang, R., Lahens, N. F., Ballance, H. I., Hughes, M. E., & Hogenesch, J. B. (2014). A circadian gene expression atlas in mammals: Implications for biology and medicine. Proc Natl Acad Sci USA, 111(45), 1621916224.CrossRefGoogle ScholarPubMed
Zhang, S., Dai, M., Wang, X., Jiang, S. H., Hu, L. P., Zhang, X. L., & Zhang, Z. G. (2020). Signalling entrains the peripheral circadian clock. Cell Signal, 69, 109433.Google Scholar
Figure 0

Figure 1.1 Satellite image illustrating nighttime skyglow across the globe.

Credit: NASA Earth Observatory images by Joshua Stevens, using Suomi NPP VIRS data from Miguel Roman, NASA’s Goddard Space Flight Center.

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