What this is
- This review examines how disturbances in circadian rhythms affect the musculoskeletal system.
- It highlights the role of nutritional strategies in maintaining musculoskeletal health.
- The interplay between circadian regulation and physiological processes is emphasized.
Essence
- disturbances can negatively impact musculoskeletal health, increasing the risk of conditions like osteoporosis. Nutritional strategies play a crucial role in mitigating these effects.
Key takeaways
- Circadian rhythms regulate both skeletal muscle and bone functions. Disruptions in these rhythms can lead to metabolic issues and increased risks of fractures and osteoporosis.
- Nutritional strategies, including adequate intake of calcium and vitamin D, are essential for maintaining bone health, particularly in populations with circadian disruptions.
- The timing of nutrient intake can influence metabolic responses and should be considered in dietary recommendations for musculoskeletal health.
Caveats
- The review is based on existing literature, which may have limitations in study design and sample sizes. Further empirical studies are needed to substantiate the proposed nutritional strategies.
- Individual variations in circadian rhythms and their effects on health outcomes are not fully explored, necessitating more personalized approaches.
Definitions
- circadian rhythm: A roughly 24-hour cycle in biological processes, influenced by environmental cues like light and feeding schedules.
- chrononutrition: The study of how the timing of food intake affects health and metabolism, particularly in relation to circadian rhythms.
AI simplified
1. Introduction
Human physiological functions are highly dependent on the regulation of the internal circadian clock. The complete biological clock includes the master clock in the hypothalamusâs suprachiasmatic nucleus (SCN) and the peripheral clocks. Both clocks must work in symphony, with the SCN playing the role of the timekeeper of the whole body [1]. The bodyâs musculoskeletal system is part of the peripheral clocks; hence, the system relies on the SCN regulation of neural and endocrine pathways to work synchronously with other systems [2].
Despite the reliance on the light that entrains the sleep and wake cycle, the peripheral clock in the musculoskeletal system also depends on the regulation of the 24 h schedule of feeding and physical activities. These scheduled regulations that influence the musculoskeletal systemâs circadian clock are independent of the SCN clock. Zhang et al. found that there are approximately 1600 circadian genes expressed in the skeletal muscle [3]. Clock-controlled genes (CCGs) that are important for the circadian maintenance of skeletal muscle and specific to the musculoskeletal system include Myod1, Atrogin (Fbxo32), Mef2, and Glut4 [3,4].
Skeletal muscle constitutes approximately 40% of total body weight and contains 50 to 75% of the bodyâs total proteins. Therefore, it consists of the largest collection of peripheral clocks in the human body. Metabolically, the skeletal muscle is responsible for maintaining homeostasis in the balance between energy intake and utilisation [5]. Equilibrium is always achieved because of the unique musculoskeletal capabilities to adapt based on the bodyâs demand (physical activity) and supply (nutrient). This flexibility allows the skeletal muscle system to decide on the usage and storage of energy required for the body based on the 24 h schedule of fastingâfeeding and restingâactive state [6,7].
Similar to skeletal muscle, the circadian rhythm that regulates bone functions also depends on the cues from scheduled feeding and fasting. Serum C-telopeptide fragments of collagen type 1 (S-CTX), a serum marker on bone resorption, showed that its daily rhythm is highly influenced by the fastingâfeeding schedule. Its serum level is higher in the early morning and reaches a peak at around 05:00â08:00, whereas in the late afternoon, from 12:00 to 16:00, the serum level reaches its lowest level. An apparent change in diminished diurnal rhythm of the marker is seen in fasting [8]. Besides that, the diurnal rhythm also varies with changes in the intake of glucose, protein, and fat [9]. Due to the influence of the circadian rhythm on the musculoskeletal system, those working in shifts and with circadian disruption are at increased risk of bone fractures and osteoporosis [10,11].
Both central and peripheral clocks regulate the interactions between the musculoskeletal system and energy metabolism. Thus, external factors such as feeding time and various nutrients mediate its regulation. This review discusses the disturbance of the circadian rhythm and its resultant effect on the musculoskeletal system. We also discuss the nutritional strategies that are potentially effective in maintaining the systemâs homeostasis.
2. Methods
The search strategy was developed collaboratively with the research team. A time frame for publication access was set to focus on the recent studies on circadian rhythm and the resultant effect on the musculoskeletal system of the body, together with the related nutritional strategies (from 2012 to 2022). The systematic search was performed in electronic databases using standardised search terms specific to the needs of each respective database and revised by the research team. The databases selected were Scopus, Pubmed, EBSCOHost, and Google Scholar. The search was conducted with MeSH (Medical Subject Headings in PubMed) terms including âcircadian rhythmâ, âbiological clockâ âmusculoskeletal diseaseâ, âmusculoskeletal abnormalitiesâ, âdietâ, ânutritionâ, and ânutritional statusâ. Boolean operators (AND, OR, AND NOT) were used to combine search terms within related keywords. An additional search was performed using modified search terms if search terms were incomplete. For this review, articles were restricted to English publications.
3. Human Circadian Rhythm
Humans display a circadian rhythm of an approximately 24 h cycle. The word âcircadianâ is derived from the Latin phrase circa diem, which means about a day. The rhythm may vary from one human to another depending on their lifestyle and environment. In a healthy human, the circadian rhythm influences major physiological functions, including the 24 h biological cycle of behavioural, physical, and mental changes. More specifically, the major physiology functions of circadian rhythm involve, among others, the sleepâwake cycle [12,13], blood pressure [14,15], body temperature [16,17], hormonal homeostasis [18], prothrombotic factor regulation [19], and hormone release in the digestive system to match eating habits [20]. Besides these, circadian rhythm is also important in the promotion of good metabolic balance, haemostasis, alertness or functional cognition, optimum cell repair, a healthy body, and healthy brain development, in addition to the boosting of the immune system [21]. Figure 1 illustrates the 24 h circadian rhythm and human body response.
A group of nerve cells forming the suprachiasmatic nucleus (SCN) in the anterior hypothalamus play roles in regulating the circadian rhythm. The SCN is set by the circadian rhythm clock, which receives signals through the optic nerve (input) connected to the eyes. The molecular mechanism of circadian rhythms involves the circadian oscillation mechanism within cells that is controlled by a genetically encoded molecular clock. The endogenous biological pacemaker primarily controls the circadian rhythm. Many people believed that the circadian rhythm was solely controlled by the SCN, acting as the master clock. However, recent studies discovered that the circadian rhythm is also controlled by peripheral cells, such as those cells in the cardiovascular system, which possess a similar circadian clock [22,23]. As a result, both the central clock (SCN) and the peripheral clock (non-SCN) work together to provide the essential rhythmic function of the bodyâs systemic cues.
A gene mutation encoding a protein or unnatural light exposure may disrupt the circadian rhythm [24]. A chronically disrupted circadian rhythm can cause conditions such as jetlag, fatigue, insomnia, and other chronic medical conditions such as cancer, diabetes, and cardiovascular disease [14,25]. Period (PER) was the first gene identified in the circadian rhythm. Other core genes were later discovered, such as the transcription factors CLOCK-BMAL1 in the main loop which induces negative regulators, which are the important protein encoding genes, Period (PER) and Cryptochrome (CRY) proteins [26]. Other core genes, such as REVERBs/ROSs and Albumin D-site-Binding Protein (DBP) have also been found to be involved in the circadian rhythm [27]. At the molecular level, the circadian clock comprises various sets of transcription factors that lead to the autoregulation of transcriptionâtranslation feedback loops (TTFLs). The regulation represents the core mechanism of a mammalâs circadian clock. Figure 2 represents the simplified version of molecular interaction of cell cycle components with the circadian core clock.
3.1. The Biological Clock
The mammalian circadian rhythm is controlled by the biological âclock geneâ to produce the clock protein [29]. The central component of the molecular mechanism for naturally occurring circadian rhythm involves the interlocking of transcriptionâtranslation feedback loops (TTFL) with other core genes [27,30,31,32]. This component controls the oscillation of cells and tissues on their built-in (endogenous) and adjustable (entrainable) adaptation to external factors, such as daily regular environmental changes, i.e., the sleepâwake cycle [13,22]. Additionally, the central component controls melatonin secretion to control sleep patterns [33,34]. The molecular mechanism and genes involved in the circadian rhythmâs biological clock in mammals are primarily controlled by light exposure. The alerting system follows a pathway called the photic neural input pathway. In the pathway, light plays a role as a signal molecule that is detected by the retina in the presence or absence of light. The light alters the pineal gland secretion, and the eyes are closed involuntarily to avoid any excessive exposure to light [35,36,37]. These mechanisms are regulated by the circadian rhythm, thus explaining their importance in daily life.
Moreover, there are pathways that serve as modulators for peripheral tissues. First, the pathways are activated by the signals detected by the photosensitive retinal ganglion cells, followed by the retinohypothalamic tract (RHT) pathway, which is then connected to the SCN, which then releases the output instruction via the paraventricular nucleus (PVN) and superior cervical ganglia (SCG). Then, the output is delivered to the targeted endocrine gland, such as the pineal gland, for melatonin inhibition and secretion [35]. Reduced blood pressure, lower levels of melatonin secretion, and an increase in cortisol are the factors that cause the body to naturally feel awake in the early morning, as the body has optimal cardiovascular efficiency, compromised muscle strength, and increased brain performance.
3.2. How Is Circadian Rhythm Measured?
Measuring circadian rhythm is important to assess an individualâs sleepâwake cycles, especially in patients with circadian rhythm sleepâwake disorder (CRSWD). A variety of measures mainly involving physiological function and instruments or objective tools can be used to assess circadian rhythm. Melatonin level, core body temperature, and the restâactivity cycle are examples of physiological functions. Melatonin level is commonly used due to its accessibility, as it can be detected through plasma and/or saliva. This allows for frequent sampling. However, the assay is not a standard used in laboratories due to its cost and high turnaround time (7â10 days) [38]. Dim light melatonin onset (DLMO) is a marker commonly used and recommended to confirm the diagnosis of sleepâwake disorder [39]. Aside from that, core body temperature has previously been used to assess circadian timing due to the faster results obtained compared to a melatonin assay [40]. Previously, this method was less convenient as a probe had to be inserted into the rectum, but technology advancements have led to devices that can be swallowed to transmit real-time data through the digestive tract, as well as measure skin temperature [41]. The restâactivity cycle can be used to measure circadian timing. Wrist actigraphy measures the sleepâwake cycle and light level to track the timing of restâactivity. Multiple features are available in commercially available wrist-worn activity monitors, which are believed to be beneficial in estimating sleepâwake cycles that are associated with sleepâwake disorders [39]. Assessing light levels was also found to have a relationship with mood, sleep quality, and health-related outcomes [42,43].
Besides physiological function, objective measurements using tools such as sleep diaries and chronotype questionnaires were also commonly used due to their feasibility in population studies. Clinicians can use sleep logs to characterise patterns of sleepâwake. The diaries also included information about medications, alcohol or caffeine consumption, naps, and exercised activity, which was useful in assessing the pattern to improve circadian disturbance in patients with sleep disorders [39]. Circadian chronotype is an individualâs preferred time to perform daily activities. As an alternative to timing the circadian rhythm, questionnaires are frequently used tools. The questionnaires fit well in healthy control populations, but evidence was lacking in patient populations [44]. Examples of the questionnaires include the MorningâEveningness Questionnaire (MEQ), Munich Chronotype Questionnaire (MCTQ), and Munich Chronotype Questionnaire for Shiftworkers (MCTQShift) [45].
3.3. Effect of Circadian Rhythm on the Body
The circadian rhythm holds a crucial regulatory role in human physiology by regulating many different body systems, including hormone production, glucose homeostasis, the central nervous system, cardiovascular maintenance, and lipid metabolism, to name a few. All these systems are interrelated and dependent on each other, thus imposing the role of circadian rhythm on human physiology. Since the SCN regulates body temperature, neuronal activities, hormone secretion, and musculoskeletal systems, it is deduced that disruption in the normal circadian rhythm can impair the regulated systems. The SCN, in turn, is majorly dependent upon light. At a molecular level, the circadian rhythm is regulated by the transcriptional and translational regulation feedback loop of core clock genes, which include Bmal1 (Bain and muscle ARNT-like 1), CLOCK, Per1 (Period1), Per2, Cry1 (cryptochrome1), and Cry2. Thus, the CLOCK: Bmal1 regulators are an integral part of SCN regulation and are directly affected by external factors such as sleep quality, diet, and exercise. Sleep disturbances, for example, have been linked to neuro-disorders such as attention-deficit hyperactivity disorder (ADHD) [46]. ADHD studies showed that children with delayed melatonin secretion are predisposed to ADHD [47]. In adults, impaired CLOCK gene expressions caused by disturbed sleep have been reported to perturb the diurnal rhythms of endocrine secretion [48]. Thus, compromised sleep has been correlated with ADHD in adults.
Apart from melatonin secretion, another example of hormonal regulation by the SCN is the maintenance of the hormone leptin. Leptin increases the activation of the sympathetic nervous system and increases thermogenesis by stimulating the thyroid hormones [49]. Studies show that the peak of leptin secretion occurs during the night. In a study by Buonfiglio et al., lack of sleep resulted in long-term resistance to leptin, and led to reduced metabolism and increased adipose tissue in rats [50]. Conversely, numerous studies demonstrated that rats supplemented with oral melatonin showed increased body weight loss [51]. Such studies have also shown increased weight loss in post-menopausal women [52]. In this study, 81 women between the ages 25 and 65 years were subjected to melatonin administration and a balanced diet to improve their sleep cycle. The tested subjects reported weight loss and improved sleep quality after 24 weeks. On top of obesity, circadian rhythms have also been implicated in other metabolic illnesses, including type 2 diabetes and several neurological disorders.
Numerous studies have also shown a positive correlation between circadian rhythm and glucose homeostasis. Significant changes in transcription factors in liver genes such as forkhead box O1 Foxo1 and peroxisome proliferator-activated receptor alpha, Pparα, increased. Such oscillations restored homeostasis and increased insulin sensitivity to accommodate glucose metabolism in disrupted sleep cycles [53]. However, glucose homeostasis is significantly affected in diabetic conditions and by chronic circadian disruption. In clock-disrupted clock-gene Bmal1-knockout mice, insulin secretion was reduced, and they were prone to obesity. In shift work mice, the liver clock genes and glucose metabolism-related genes oscillated. Restored Bmal1 genes rescued the phenotype, thus highlighting the role of circadian genes in insulin expression [54].
Interestingly, recent work by Xu et al. (2022) shows that even in the prediagnostic phase of diabetes mellitus, the mild disruption of circadian rhythms and daily restâactivity impairs glucose homeostasis and thus predisposes one to diabetes mellitus [55]. Since metabolism is crucial in cellular turnover, perturbations in the circadian cycle can induce metabolic disorders such as non-alcoholic fatty liver disease [56]. Non-alcoholic fatty liver disease is also commonly associated with the loss of skeletal muscle mass, or sarcopenia. Such a correlation indicates the relationship between musculoskeletal systems and metabolism [57]. Both the skeletal and muscle systems are implicated in the bodyâs locomotor activity and nutrition homeostasis which, in turn, maintain tissue mass and metabolism.
3.4. Effect of Circadian Rhythm on the Musculoskeletal System
The CLOCK: Bmal1 circuit also regulates the circadian regulation of the musculoskeletal system (Figure 3). In osseous structures, a synchronous circadian rhythm promotes healthy cartilage and bone formation [58,59,60]. The regulation of bone formation by osteoblasts and absorption by osteoclasts is maintained by glucose homeostasis and parathyroid hormones [61], all of which are regulated by circadian rhythms [62,63]. A study showed that a combined high-fat diet and circadian rhythm disruption lead to a diabetic skeletal phenotype in mice [24]. The disruption of the Bmal1 expression system has been shown to compromise bone and cartilage formation. Transcriptomics in Bmal1-knockout mice showed degenerating knee cartilage due to chronically impaired circadian clock activity [64]. Bmal1 disruption also perturbs glucose homeostasis in the musculoskeletal system. The disruption of Bmal1 expression resulted in a muscle-specific loss by disrupting muscle triglyceride biosynthesis and accumulating bioactive lipids and amino acids [65]. In 9-month-old Bmal1-knockout mice, the absence of Bmal1 expression led to muscle atrophy, reduced body weight in healthy mice, weak skeletal muscles, and structural muscle pathologies [66]. Muscle pathologies were also shown to occur due to impaired glucose metabolism. Numerous studies show that diurnal oscillations cause insulin resistance [67] and diminish the expression of the glucose transporter 4 (GLUT4) [68,69]. Another study showed that GLUT4 expression is increased with exercise and increases insulin sensitivity and glucose absorption, thereby promoting muscle health [70]. The musculoskeletal system is heavily involved with locomotion, feeding, and sleep quality. Thus, intervention through the chrono diet, sleep, and exercise can be used to maintain and sustain healthy bone and muscle growth [71].
3.5. Role of Skeletal Muscle Circadian Clock in Lipid and Glucose Metabolism
It is generally well-established that clock genes regulate the circadian rhythm which is associated with glucose and lipid metabolism [72]. Hence, disturbances in the circadian rhythm, particularly due to shift work, impair lipid and glucose homeostasis, ultimately impacting human health [73]. The circadian-regulating process has been recognized as one of the factors that is linked to the oscillation of glucose metabolism via the hepatocyte circadian clock. Due to this, shift work in the long term has been shown to reduce tolerance towards glucose [73]. Various genes which regulate glucose metabolism, such as Gys2 [74], PEPCK [75], CRY1, and CRY2 [76], have been studied to be associated with cellular circadian rhythm.
An experimental tissue-specific Bmal1 knockout (KO) model has unravelled the critical role that peripheral oscillator circadian clocks have on glucose metabolism, especially in the pancreas, liver, and skeletal muscle [77]. Studies using the skeletal muscle-specific Bmal1 KO have shown that the muscle clock is essential in anticipating the transition from resting to active phase at awakening and promoting glucose uptake and metabolism, as the predominant fuel for skeletal muscle [78].
Dyar et al. revealed that the muscle clock via the Bmal1 and REV-ERBα is a key factor in regulating various normal physiological process such as muscle energy homeostasis [65]. This occurs through the direct activation of transcriptional activities that promote lipid storage, insulin sensitivity, and glucose metabolism, while simultaneously inhibiting lipid oxidation and protein catabolism. Disturbances in the muscle clock genes results in increased lipid oxidation and protein turnover, which culminates in a metabolic inefficiency condition.
A short-term controlled experimental circadian misalignment study using a shift work clock revealed a disruption in skeletal muscle lipidome, which led to insulin resistance [79]. In an earlier experiment on circadian misalignment, skeletal muscle insulin sensitivity was decreased by 23% in contrast to the normal circadian condition [80]. This suggests that circadian misalignment disrupts skeletal muscle lipid metabolism, which contributes to the occurrence of muscle insulin resistance, eventually becoming a precursor to type 2 diabetes mellitus [79]. Inevitably, alterations in the circadian rhythms and the genes that control them affect normal physiological metabolism, eventually resulting in various metabolic disorders [81].
4. Circadian Rhythm and Bone Health
Bone health is dependent on the dynamic balance between bone formation by osteoblasts and bone resorption by osteoclasts. Biological factors such as hormones, chronobiological properties, and cytokines, as well as mechanical factors such as load and stressor, influence these activities. Circadian rhythm has been postulated to have an effect on bone remodelling. Our body needs to keep up with its circadian clock to stay healthy. Those who have an altered or reversed circadian rhythm, such as shift workers, were found to have pre-osteoporotic features such as reduced bone mass and density, altered bone microstructure, and decreased bone strength [82]. Animal studies are also in accordance with this finding, in which circadian gene knockout mice showed abnormal bone remodelling [83].
Previous studies have reported that clock genes are involved in osteoblasts and osteoclastsâ activities as well as cartilage formation [84]. The serum level of calcium and bone markers such as alkaline phosphatase, C-telopeptide of type I collagen (CTX), tartrate-resistant acid phosphatase (TRAP), and osteocalcin showed diurnal variation, which peaked in late night or early morning about 15â20% higher than the nadir value, which occurs in the afternoon [85]. Most bone cells, such as osteoblasts, osteoclasts, and osteocytes, have been shown to express circadian clock genes. The main clock genes that regulate circadian rhythm and bone health are Bmal1, Bmal2, Clock, Cry, and Per [8]. Bmal1 plays a vital role in regulating bone remodelling by upregulating the expression of bone microRNAs, such as the nuclear factor of activated T cells and inhibiting the receptor activator of nuclear factor kappaâbeta ligand (RANKL). RANKL binds to RANK on osteoblasts which later activate osteoclast differentiation. This stimulation of osteoclastic activity increases bone resorption. The overexpression of RANKL is associated with bone degenerative diseases such as osteoarthritis and rheumatoid arthritis. Bmal1-/- mice were found to have osteopenia. This is in accordance with the fact that Bmal1 is associated with the inhibition of RANKL. Hence, the absence of Bmal1 promotes bone resorption activity and leads to a decrease in bone mass and density [86]. Cry and Per, which are also the main clock genes, have a negative regulation factor for circadian rhythm. The mutation of these genes results in increased osteoblast proliferation and reduced bone loss. Cry and Per have low expression during the day and high expression during the night. This is in congruence with the expression of bone-related genes, where osteoprotegrin (OPG) expression rises during the day and falls during the night, and vice versa for RANKL [87]. This evidence is in accordance with a study by Samsa et al., which reported that Per- and Cry-deficient mice had low bone volume [88]. Correspondingly, continuous light exposure can lead to bone loss and an increase in inflammatory cytokines, which result in an increased risk of osteoporosis.
Less Number of Hours of Sleep and Associated Bone Defects and Osteoporosis
The pathogenesis of osteoporosis includes an imbalance between bone resorption and bone formation activities as we age, an increase in inflammatory cytokines, a lack of sexual hormones, medications, and a shift in circadian rhythm. In recent years, it has been reported that disturbances in the darkâlight cycle, which generate a condition similar to shift work or chronic jet lag, showed a trend in alterations in bone structure and bone loss []. Adequate hours of sleep are important for biological processes and to maintain optimum health. Biochemical bone markers such as CTX, osteocalcin, and ALP peak overnight, with a peak in the early morning, which suggests that bone remodelling is affected in those who experience sleep disturbances []. There have been many reports of increased fracture risks among shift workers. Sleep disturbances and circadian reduction can increase somnolence, which indirectly reduces self-vigilance towards environmental hazards and increases risk of falls and fractures []. 89 90 91
In an osteoarthritis rat model, it was found that clock genes in the early stages of bone and cartilage degeneration were altered. Another animal study using rats with a 10-day sleep restriction showed a significant drop in osteoblast and increase in osteoclast activity []. Another study using a different method reported that mice exposed to continuous light for 24 weeks had decreased trabecular bone volume compared to mice exposed to normal lightâdark cycles []. Their trabecular bone was reported to be porous, with an increase in inflammatory markers. These findings supported the correlation between sleep disturbance, circadian rhythm, and bone health. Studies have demonstrated that those who worked night shifts had lower bone density compared to those who worked day shifts [,,]. It was speculated that the low bone density in night shift workers is due to an increase in cortisol and altered vitamin D status from sleep disturbances. 92 59 90 93 94
A study conducted by Shan et al. reported a correlation between shift work and an increased risk of obesity and type 2 diabetes mellitus (T2DM) []. Energy expenditure is affected due to sleep deprivation, and circadian rhythm disturbances cause an increase in energy intake. As a result, they contribute to overweight and T2DM. There is a close link between bone health and glucose metabolism. High blood sugar levels are reported to inhibit calcium absorption and bone calcification, which lead to an increased risk of osteoporosis []. In T2DM mice, serum osteocalcin was reduced, and serum TRAP was significantly increased. Bone density and bone strength were also significantly reduced in those T2DM mice. Hence, we can corroborate that sleep disturbances affect glucose metabolism which, in turn, leads to bone loss. 95 96
Diurnal variations in bone cells and bone markers as well as the knockout clock gene in animal models have clearly shown that circadian rhythmicity is vital for bone health. Nowadays, an increasing number of individuals experience sleep disturbances due to working shifts and jet lag due to constant travel. This contributes to an increased risk of osteoporosis, which could be attenuated by a novel intervention targeting the circadian timing system. The application of chronotherapy, which is a method of medication administration coordinated with the biological clock, is an effective intervention to improve the efficacy of osteoporosis treatment. The circadian clock gene can be a therapeutic target for researchers to study on the prevention and treatment of bone diseases. This indirectly reduces osteoporosis and fracture cases in the future.describes a list of studies on bone disorders and their relationships with circadian rhythm. Table 1
5. Nutritional Strategies for Musculoskeletal Health
Nutritional status plays an important aspect in bone health. Malnutrition appears as a strong predictor of bone osteoporosis and impaired bone healing, especially in the elderly. Hence, a balanced diet rich in nutrients, vitamins, and minerals is essential for the prevention and treatment of bone disorders [112].
Besides bone health, muscle disorders that are usually associated with pain are also the leading causes of disability and decreased quality of life among adults worldwide. Their prevalence was recorded at approximately 30% (ranging from 13.5% to 47%) in 23 population studies conducted in 15 different countries (the United States, United Kingdom, Germany, Sweden, Denmark, Norway, Italy, Spain, The Netherlands, Kuwait, Japan, Austria, Malaysia, Brazil, and Cuba). As practitioners struggle to curb the problems, it is proposed that the modifiable factor related to nutrition be included in the assessment, advice, and intervention, which may provide a new perspective on the solution [113]. Multiple disorders of the musculoskeletal system are related to inflammatory factors; hence, they exert the sensation of pain. A diet containing protein, specifically soy protein, has been found to have a pain-relieving effect among an aging population with osteoarthritis [114]. Several studies have suggested that anti-inflammatory foods, such as those found in the Mediterranean diet (vegetables, fruits, fish, fish oils, legumes, olive oil, and plant-based proteins), are best for relieving the inflammation and pain associated with chronic musculoskeletal disorders and diseases [113]. On the contrary, an excessive fat diet was found to increase nociceptive responsiveness and enhance pain sensation in an animal study on knee arthritis [115].
Calcium and vitamin D are two established nutrients related to bone health. Deficiencies in calcium and vitamin D are major risk factors for osteoporosis and compromised bone repair [116]. An adequate intake of these nutrients is essential; however, the global prevalence of deficiencies is notably high [117]. Because calcium intake influences peak bone mass from a young age, it is critical to increase childrenâs consumption of dairy foods and calcium sources in food or supplements. Previous meta-analyses reported that calcium or dairy intervention in children has a significant effect on bone density [118,119]. Although it is uncertain whether these effects could reduce fracture, adequate intake of calcium at a young age is shown to be related to bone mineral accretion in adulthood as well. Recent research updates highlighted on the importance of chronotherapy as a strategy to improve the therapeutic efficacy of osteoporosis because bone metabolism demonstrates potent circadian regulations. In addition, the main regulators of calcium homeostasis, namely osteocalcin and vitamin D, also demonstrate a diurnal rhythm in humans. Thus, the appropriate timing for the supplementation of calcium may have a significant impact on bone resorption. There are studies suggesting that evening calcium intake may suppress bone resorption. On the contrary, no significant impact was found when the supplementation was given in the morning [120,121]. However, up to date, the optimal time for antiresorptive treatment is still scarce. Despite the fact that calcium supplementation and therapy based on the biological clock seems to be a promising strategy, more data from randomised clinical trials are needed prior to its implementation.
Vitamin D on the other hand, is essential to maintain the concentration of calcium [122]. It can be obtained from sunlight exposure and food fortification. The deficiencies are worldwide issues which are mainly associated with bone diseases [123]. Eventually, a recent study among shift workers showed that low serum calcium levels might be associated with circadian dysregulation as well as sleep disturbance [124]. Individuals with irregular sleep schedules may obtain less sun exposure, which contributes to vitamin D deficiency. Due to inevitably low exposure to sunlight in certain populations owing to various limitations, there are suggestions for vitamin D supplementation. A few studies have suggested that the supplement be taken after meal to maximize absorption [125]. Similar to calcium supplementation, the intake of vitamin D supplements at a certain time of the day is the future direction of study to be explored.
Nutritional strategies for bone health in circadian dysregulation population may include promoting an adequate intake of calcium and vitamin D from a young age for the promotion of bone development. It should be in accordance with physical activity for improvement in bone mineral density [126]. School-based nutrition intervention may be effective in implementing the strategy [127]. In adults, as they may be exposed to circadian regulation, a balanced diet emphasising calcium is necessary to maintain bone health. Fortified vitamin D foods, milk intake, and calcium supplementation are also suggested [128]. Although adult intervention is questionable in terms of feasibility and sustainability, such studies are required in order to suggest ways to improve intake among vulnerable populations. It is critical to improve the nutritional status of the elderly, who are more prone to bone fractures. As malnutrition is very prevalent among elders with bone or hip fractures, proper nutrition assessment and intervention are needed.
Another interesting view in maintaining musculoskeletal health is the timing of intake for specific types of nutrients in assuring optimal uptake that benefits its function. For example, the intake of carbohydrates influences insulin release. Insulin influences the transport of tryptophan across the blood brain barrier after each carbohydrate-rich meal, and facilitates the uptake of large neutral amino acids by muscle [129]. According to research, different carbohydrate intake times have different metabolic effects. In accord with carbohydrates, the intake of important nutrients for muscle, such as tryptophan-rich proteins, at different times of the day also showed variability in the bodyâs response [130]. However, the majority of these studies did not explore the direct impact of the different timings of intake on musculoskeletal functions.
6. Conclusions and Future Directions of Research
The musculoskeletal system is the main system that influences daily activities; hence, any disorders or limitations on its function generally affect an individualâs quality of life. We found that growing interest in the individual circadian regulation associated with disease progression has produced various insights into the reciprocal relationships in the field of nutrition [131]. However, most studies on the musculoskeletal system related to nutrition focus on finding the specific type of nutrients or food with potential benefits for health. The concern that is still scarce relates to the type of food consumed at which specific time of day that may have a specific impact on the system. Furthermore, for those who are overweight or obese, losing weight has always been part of the clinical recommendation to address the problem of musculoskeletal disorders. Particularity on the timing of nutritional intake in accordance with circadian rhythm also exerts an effect on calorie intake, which subsequently affects body weight [113]. Given that circadian regulation influences the times at which various physiological processes are optimised, taking into account individual differences in circadian regulation, which recent studies have labelled as âchronotype,â is critical for personalised nutrition recommendations in populations with musculoskeletal disorders. Similar to the approach of chrononutrition, this also applies to nutritional supplements, with the idea that specific supplements may provide better effectiveness during certain times of the day. The specific timing when supplements should be consumed relates to individual sleep and energy patterns [121]. However, the only setback is the lack of conclusive evidence on the specific timing.
The evolution of chronobiological studies has recently left pressing questions to be explored. As described in Figure 1, recommendations on body response are based on the 24 h clock with a specific sunrise time of around 6 am. However, sunrise times vary across the globe; as a result, these differences affect the sleep and wake timing of populations, as well as the onset of dim light melatonin [132]. These variations further affect the best time for daily activities and their relationship with musculoskeletal health. Hypothetically, the bodyâs 24 h chronological events may be best described in terms of hours and minutes from wake time, rather than being assigned to a specific 24 h time of day. Thus, the body response of those living in regions with different seasons can be better understood. With respect to specific food and supplement intake, this area of study must be further explored to allow effective interventions. Collaborations between nutritionists and physiologists in this chronobiological and chrononutrition field will further clarify these interactions and ultimately lead to successful interventions to reduce morbidity due to musculoskeletal disorders.