Your search keyword '"SUPRACHIASMATIC nucleus"' showing total 15,038 results

1. Neuronal and glial vulnerability of the suprachiasmatic nucleus in tauopathies: evidence from human studies and animal models.

Author

Son, Gowoon, Neylan, Thomas, and Grinberg, Lea

Subjects

“Alzheimer’s disease”, “Amyloid”, “Astrocyte”, “Circadian clock”, “Circadian dysregulation”, “Microglia”, “Neurodegenerative disease”, “Progressive supranuclear palsy”, “Suprachiasmatic nucleus”, “Tau”, Animals, Humans, Neuroglia, Tauopathies, Suprachiasmatic Nucleus, Alzheimer Disease, Models, Animal

Abstract

Tauopathies, a group of neurodegenerative diseases that includes Alzheimers disease, commonly lead to disturbances in sleep-wake patterns and circadian rhythm disorders. The circadian rhythm, a recurring 24-hour cycle governing human biological activity, is regulated by the hypothalamic suprachiasmatic nucleus (SCN) and endogenous transcriptional-translational feedback loops. Surprisingly, little attention has been given to investigating tauopathy-driven neuropathology in the SCN and the repercussions of SCN and circadian gene dysfunction in the human brain affected by tauopathies. This review aims to provide an overview of the current literature on the vulnerability of the SCN in tauopathies in humans. Emphasis is placed on elucidating the neuronal and glial changes contributing to the widespread disruption of the molecular circadian clock. Furthermore, this review identifies areas of knowledge requiring further investigation.

Published

2024

2. Crosstalk between the subiculum and sleep–wake regulation: A review.

Author

Rahimi, Sadegh, Joyce, Leesa, Fenzl, Thomas, and Drexel, Meinrad

Subjects

*RAPID eye movement sleep, *SUPRACHIASMATIC nucleus, *LOCUS coeruleus, *HIPPOCAMPUS (Brain), *RAPHE nuclei, *PROSENCEPHALON, *PREOPTIC area

Abstract

Summary: The circuitry underlying the initiation, maintenance, and coordination of wakefulness, rapid eye movement sleep, and non‐rapid eye movement sleep is not thoroughly understood. Sleep is thought to arise due to decreased activity in the ascending reticular arousal system, which originates in the brainstem and awakens the thalamus and cortex during wakefulness. Despite the conventional association of sleep–wake states with hippocampal rhythms, the mutual influence of the hippocampal formation in regulating vigilance states has been largely neglected. Here, we focus on the subiculum, the main output region of the hippocampal formation. The subiculum, particulary the ventral part, sends extensive monosynaptic projections to crucial regions implicated in sleep–wake regulation, including the thalamus, lateral hypothalamus, tuberomammillary nucleus, basal forebrain, ventrolateral preoptic nucleus, ventrolateral tegmental area, and suprachiasmatic nucleus. Additionally, second‐order projections from the subiculum are received by the laterodorsal tegmental nucleus, locus coeruleus, and median raphe nucleus, suggesting the potential involvement of the subiculum in the regulation of the sleep–wake cycle. We also discuss alterations in the subiculum observed in individuals with sleep disorders and in sleep‐deprived mice, underscoring the significance of investigating neuronal communication between the subiculum and pathways promoting both sleep and wakefulness. [ABSTRACT FROM AUTHOR]

Published

2024

3. Fabrication of S-g-C3N4/Ni-CuS nanocomposites: assessing the influence of S-g-C3N4 concentration on electrocatalytic performance for HER/OER activities.

Author

Mehrose, Qamar, Muhammad Azam, Ali, Syed Kashif, Imran, Mohd, Farhan, Ahmad, Hakami, Othman, Zelai, Taharh, Madkhali, O., Alathlawi, Hussain J., and Amri, Nasser

Subjects

*CLEAN energy, *OXYGEN evolution reactions, *COPPER sulfide, *SCANNING electron microscopy, *GLOBAL warming, *SUPRACHIASMATIC nucleus

Abstract

The shortage of fossil fuels and global warming are the two main issues facing the world today and these can be overcome by the usage of H2 as a sustainable energy. The study's primary objective is to fabricate an efficient electrocatalyst for electrochemical water splitting. This study uses CuS, Ni-doped CuS and Ni/CuS/S-g-C3N4 (NCS/SCN) composites for the electrochemical water-splitting. NCS/SCN composites were produced via the co-precipitation method with different S-g-C3N4 contents (10, 30, 50, 70, and 90 wt.%) to study the impact of S-g-C3N4 on the electrochemical water splitting performance of NCS. Characterization techniques SEM, EDX, FTIR, and XRD evaluated the electrocatalysts' size, shape, and morphology. Electrochemical studies were performed employing a three-electrode system using KOH as the electrolyte. Results from LSV, CV, and EIS show that the development of composite material NCS/SCN enhances the electrocatalytic water-splitting activity of NCS in 1 M KOH solution. Results show that NCS/50%SCN exhibits the best OER and HER and thus can be utilized as a commercial electrocatalyzer for water splitting. [ABSTRACT FROM AUTHOR]

Published

2024

4. Hypothyroidism alters the rhythmicity of the central clock, body temperature and metabolism: evidence of Bmal1 transcriptional regulation by T3.

Author

Emrich, Felipe, Gomes, Bruno Henrique, Selvatici‐Tolentino, Letícia, Lopes, Roberta Araújo, Secio‐Silva, Ayla, Carvalho‐Moreira, João Pedro, Bittencourt‐Silva, Paloma Graziele, Guarnieri, Leonardo de Oliveira, Silva, Ana Bárbara de Paula, Drummond, Lucas Rios, da Silva, Glauber Santos Ferreira, Szawka, Raphael Escorsim, Moraes, Márcio Flávio Dutra, Coimbra, Cândido Celso, Peliciari‐Garcia, Rodrigo Antonio, and Bargi‐Souza, Paula

Subjects

*HYPOTHYROIDISM, *CIRCADIAN rhythms, *SUPRACHIASMATIC nucleus, *PITUITARY gland, *THYROID gland

Abstract

In mammals, the central circadian oscillator is located in the suprachiasmatic nucleus (SCN). Hypothalamus–pituitary–thyroid axis components exhibit circadian oscillation, regulated by both central clock innervation and intrinsic circadian clocks in the anterior pituitary and thyroid glands. Thyroid disorders alter the rhythmicity of peripheral clocks in a tissue‐dependent response; however, whether these effects are influenced by alterations in the master clock remains unknown. This study aimed to characterize the effects of hypothyroidism on the rhythmicity of SCN, body temperature (BT) and metabolism, and the possible mechanisms involved in this signalling. C57BL/6J adult male mice were divided into Control and Hypothyroid groups. Profiles of spontaneous locomotor activity (SLA), BT, oxygen consumption (V̇O2${{\dot{V}}_{{{{\mathrm{O}}}_{\mathrm{2}}}}}$) and respiratory quotient (RQ) were determined under free‐running conditions. Clock gene expression, and neuronal activity of the SCN and medial preoptic nucleus (MPOM) area were investigated in light–dark (LD) conditions. Triiodothyronine (T3) transcriptional regulation of Bmal1 promoter activity was evaluated in GH3‐transfected cells. Hypothyroidism delayed the rhythmicity of SLA and BT, and altered the expression of core clock components in the SCN. The activity of SCN neurons and their outputs were also affected, as evidenced by the loss of circadian rhythmicity in V̇O2${{\dot{V}}_{{{{\mathrm{O}}}_{\mathrm{2}}}}}$ and RQ and alterations in the neuronal activity pattern of MPOM. In GH3 cells, T3 increased Bmal1 promoter activity in a time‐dependent manner. Thyroid hormone may act as a temporal cue for the central circadian clock, and the uncoupling of central and peripheral clocks might contribute to a wide range of metabolic and thermoregulatory impairments observed in hypothyroidism. Key points: Hypothyroidism alters clock gene expression in the suprachiasmatic nucleus (SCN).Thyroid hypofunction alters the phase of spontaneous locomotor activity and body temperature rhythms.Thyroid hormone deficiency alters the daily pattern of SCN and medial preoptic nucleus neuronal activities.Hypothyroidism alterations are extended to daily oscillations of oxygen consumption and metabolism, which might contribute to the development of metabolic syndrome.Triiodothyronine increases Bmal1 promoter activity acting as temporal cue for the central circadian clock. [ABSTRACT FROM AUTHOR]

Published

2024

5. PERfect Day: reversible and dose‐dependent control of circadian time‐keeping in the mouse suprachiasmatic nucleus by translational switching of PERIOD2 protein expression.

Author

McManus, David, Patton, Andrew P., Smyllie, Nicola J., Chin, Jason W., and Hastings, Michael H.

Subjects

*SYNTHETIC proteins, *BIOLOGICAL rhythms, *PROTEIN expression, *CRYPTOCHROMES, *SYNTHETIC biology, *SUPRACHIASMATIC nucleus

Abstract

The biological clock of the suprachiasmatic nucleus (SCN) orchestrates circadian (approximately daily) rhythms of behaviour and physiology that underpin health. SCN cell‐autonomous time‐keeping revolves around a transcriptional/translational feedback loop (TTFL) within which PERIOD (PER1,2) and CRYPTOCHROME (CRY1,2) proteins heterodimerise and suppress trans‐activation of their encoding genes (Per1,2; Cry1,2). To explore its contribution to SCN time‐keeping, we used adeno‐associated virus–mediated translational switching to express PER2 (tsPER2) in organotypic SCN slices carrying bioluminescent TTFL circadian reporters. Translational switching requires provision of the non‐canonical amino acid, alkyne lysine (AlkK), for protein expression. Correspondingly, AlkK, but not vehicle, induced constitutive expression of tsPER2 in SCN neurons and reversibly and dose‐dependently suppressed pPer1‐driven transcription in PER‐deficient (Per1,2‐null) SCN, illustrating the potency of PER2 in negative regulation within the TTFL. Constitutive expression of tsPER2, however, failed to initiate circadian oscillations in arrhythmic PER‐deficient SCN. In rhythmic, PER‐competent SCN, AlkK dose‐dependently reduced the amplitude of PER2‐reported oscillations as inhibition by tsPER2 progressively damped the TTFL. tsPER2 also dose‐dependently lengthened the period of the SCN TTFL and neuronal calcium rhythms. Following wash‐out of AlkK to remove tsPER2, the SCN regained TTFL amplitude and period. Furthermore, SCN retained their pre‐washout phase: the removal of tsPER2 did not phase‐shift the TTFL. Given that constitutive tsCRY1 can regulate TTFL amplitude and period, but also reset TTFL phase and initiate rhythms in CRY‐deficient SCN, these results reveal overlapping and distinct properties of PER2 and CRY1 within the SCN, and emphasise the utility of translational switching to explore the functions of circadian proteins. [ABSTRACT FROM AUTHOR]

Published

2024

6. Proper Frequency of Perinatal Retinal Waves Is Essential for the Precise Wiring of Visual Axons in Nonimage-Forming Nuclei.

Author

Negueruela, Santiago, Morenilla-Palao, Cruz, Sala, Salvador, Ordoño, Patricia, Herrera, Macarena, Coca, Yaiza, López-Cascales, Maria Teresa, Florez-Paz, Danny, Gomis, Ana, and Herrera, Eloísa

Subjects

*LATERAL geniculate body, *RETINAL ganglion cells, *PHYSIOLOGY, *SUPERIOR colliculus, *SUPRACHIASMATIC nucleus

Abstract

The development of the visual system is a complex and multistep process characterized by the precise wiring of retinal ganglion cell (RGC) axon terminals with their corresponding neurons in the visual nuclei of the brain. Upon reaching primary image-forming nuclei (IFN), such as the superior colliculus and the lateral geniculate nucleus, RGC axons undergo extensive arborization that refines over the first few postnatal weeks. The molecular mechanisms driving this activity-dependent remodeling process, which is influenced by waves of spontaneous activity in the developing retina, are still not well understood. In this study, by manipulating the activity of RGCs in mice from either sex and analyzing their transcriptomic profiles before eye-opening, we identified the Type I membrane protein synaptotagmin 13 (Syt13) as involved in spontaneous activity-dependent remodeling. Using these mice, we also explored the impact of spontaneous retinal activity on the development of other RGC recipient targets such as nonimageforming (NIF) nuclei and demonstrated that proper frequency and duration of retinal waves occurring prior to visual experience are essential for shaping the connectivity of the NIF circuit. Together, these findings contribute to a deeper understanding of the molecular and physiological mechanisms governing activity-dependent axon refinement during the assembly of the visual circuit. [ABSTRACT FROM AUTHOR]

Published

2024

7. Transcriptomic Plasticity of the Circadian Clock in Response to Photoperiod: A Study in Male Melatonin-Competent Mice.

Author

Cox, Olivia H., Gianonni-Guzmán, Manuel A., Cartailler, Jean-Philippe, Cottam, Matthew A., and McMahon, Douglas G.

Subjects

*GABA, *GENE expression, *SUPRACHIASMATIC nucleus, *ION channels, *RNA sequencing, *PHYSIOLOGY, *MOLECULAR clock

Abstract

Seasonal daylength, or circadian photoperiod, is a pervasive environmental signal that profoundly influences physiology and behavior. In mammals, the central circadian clock resides in the suprachiasmatic nuclei (SCN) of the hypothalamus where it receives retinal input and synchronizes, or entrains, organismal physiology and behavior to the prevailing light cycle. The process of entrainment induces sustained plasticity in the SCN, but the molecular mechanisms underlying SCN plasticity are incompletely understood. Entrainment to different photoperiods persistently alters the timing, waveform, period, and light resetting properties of the SCN clock and its driven rhythms. To elucidate novel candidate genes for molecular mechanisms of photoperiod plasticity, we performed RNA sequencing on whole SCN dissected from mice raised in long (light:dark [LD] 16:8) and short (LD 8:16) photoperiods. Fewer rhythmic genes were detected in mice subjected to long photoperiod, and in general, the timing of gene expression rhythms was advanced 4-6 h. However, a few genes showed significant delays, including Gem. There were significant changes in the expression of the clock-associated gene Timeless and in SCN genes related to light responses, neuropeptides, gamma aminobutyric acid (GABA), ion channels, and serotonin. Particularly striking were differences in the expression of the neuropeptide signaling genes Prokr2 and Cck, as well as convergent regulation of the expression of 3 SCN light response genes, Dusp4, Rasd1, and Gem. Transcriptional modulation of Dusp4 and Rasd1 and phase regulation of Gem are compelling candidate molecular mechanisms for plasticity in the SCN light response through their modulation of the critical NMDAR-MAPK/ERK-CREB/CRE light signaling pathway in SCN neurons. Modulation of Prokr2 and Cck may critically support SCN neural network reconfiguration during photoperiodic entrainment. Our findings identify the SCN light response and neuropeptide signaling gene sets as rich substrates for elucidating novel mechanisms of photoperiod plasticity. Data are also available at http://circadianphotoperiodseq.com/, where users can view the expression and rhythmic properties of genes across these photoperiod conditions. [ABSTRACT FROM AUTHOR]

Published

2024

8. Exploration of the white matter bundles connected to the pineal gland: A DTI study.

Author

Kiani, Pejman, Hassanzadeh, Gholamreza, Jameie, Seyed Behnamedin, and Batouli, Seyed Amir Hossein

Subjects

*DIFFUSION tensor imaging, *PINEAL gland, *WHITE matter (Nerve tissue), *SUPRACHIASMATIC nucleus, *DIFFUSION magnetic resonance imaging

Abstract

Purpose: Pineal gland (PG) is a structure located in the midline of the brain, and is considered as a main part of the epithalamus. There are reports on the role of this area for brain function by hormone secretion, as well as few reports on its role in brain cognition. However, little knowledge is available on the PG, and in particular on the structural connectivity of this region with the other brain structures. Methods: Using diffusion-weighted images collected by a 3T MRI scanner, and using a sample of 61 (29 F) mentally and physically healthy young individuals in the age range of 20–30 years old, we tried to extract the white matter bundles connected to the PG. Based on prior knowledge, seven target bundles were suggested to be between the PG body and the PG roots, Pons, Periventricular region, thalamus, caudate, lentiform, suprachiasmatic nuclei, and the supercervical ganglia. Results: Nearly all the target bundles were successfully extracted, with the exception of the lentiform. Rate of identification of the tracts was different, with the bundle between the PG body and roots having the highest identification rate (97%); then it was with the Pons (70%), Periventricular region (57%), SCN (55%), left thalamus (52%), right thalamus (47%), left caudate (27%) and right caudate (22%). Conclusion: This study is an attempt to expand our knowledge on the neuroanatomy of the PG, which might help for identifying further roles for it in brain functionality, and also be a help for the treatment of some disorders in the future. [ABSTRACT FROM AUTHOR]

Published

2024

9. Blunted Melatonin Circadian Rhythm in Parkinson's Disease: Express Bewilderment.

Author

Turkistani, Areej, Al-kuraishy, Hayder M., Al-Gareeb, Ali I., Negm, Walaa A., Bahaa, Mostafa M., Metawee, Mostafa E., and El-Saber Batiha, Gaber

Subjects

*PARKINSON'S disease, *PINEAL gland, *LIGHT transmission, *NEURODEGENERATION, *DYSAUTONOMIA, *SUPRACHIASMATIC nucleus, *CIRCADIAN rhythms

Abstract

Melatonin (MTN) is a neuro-hormone released from the pineal gland. MTN secretion is regulated by different neuronal circuits, including the retinohypothalamic tract and suprachiasmatic nucleus (SCN), which are affected by light. MTN is neuroprotective in various neurodegenerative diseases, including Parkinson's disease (PD). MTN circulating level is highly blunted in PD. However, the underlying causes were not fully clarified. Thus, the present review aims to discuss the potential causes of blunted MTN levels in PD. Distortion of MTN circadian rhythmicity in PD patients causies extreme daytime sleepiness. The underlying mechanism for blunted MTN response may be due to reduction for light exposure, impairment of retinal light transmission, degeneration of circadian pacemaker and dysautonomia. In conclusion, degeneration of SCN and associated neurodegeneration together with neuroinflammation and activation of NF-κB and NLRP3 inflammasome, induce dysregulation of MTN secretion. Therefore, low serum MTN level reflects PD severity and could be potential biomarkers. Preclinical and clinical studies are suggested to clarify the underlying causes of low MTN in PD. [ABSTRACT FROM AUTHOR]

Published

2024

10. Accessibility of Patients With Special Healthcare Needs to Dental Care in the Eastern Province of Saudi Arabia: A Multicentre Study From Perspective of Caregiver and Dental Care Providers.

Author

Ezzeldin, Tarek, Algahtani, Mazin, Alghannam, Nadia Abdulrahman, Alsafran, Faisal Abdulkareem, Siddiqui, Intisar Ahmad, Al-Ghanim, Hebah Zaki, Bader, Basma Mohamed, Alshubat, Abdullah Abdulatif, Almarry, Adnan Hamad, IbnAhmed, Hussein Hejji, Kanakri, Sarah Abdulhadi, Eltayeb, Reem Babiker, Almuaybid, Mohammed Ibrahim, Al-Wasi, Khalaf Ali, and SoonMin, Ho

Subjects

CAREGIVER attitudes, CAREGIVERS, PATIENT compliance, DENTAL hygiene, DENTAL care, SUPRACHIASMATIC nucleus, CHI-squared test

Abstract

Dental care accessibility is subject to a dentist's qualification, practice and intention to treat patients, regardless of whether those patients have special healthcare needs (SCN) and should receive treatment in a dental setting. This multicentre study aimed to evaluate the characteristics of patients with SCN, their access to dental care and behaviour towards dental care from their caregiver's perspective. In addition, the perspective of dental care providers who care for patients with SCN and the factors affecting the provision of treatment was also appraised. The Eastern Province of Saudi Arabia served as the site of this cross‐sectional study from 1 February 2020 to 31 January 2022. Caregivers of 272 patients with SCN, regardless of age and gender, were recruited in the study. The caregiver's proforma sought information on the demographic characteristics, type of disability, cooperation, medical history, occupation of the parent and patient's behaviour towards oral hygiene and dental healthcare. The second proforma had the dental care provider's perspective about the common disabilities, factors that affect the decision to provide treatment, difficulties patients face in getting their dental treatment and, from the dentist's experience, recommendations to improve the access to dental care for patients with SCN. Statistical analysis was carried out by using SPSS version 22.0. The demographic features, caregiver's perception about oral healthcare accessibility and dental professional's point of view were presented as frequencies and percentages. Chi‐square test was applied to compare the proportions. The majority of the caregivers were satisfied with the dental service providers (91.9%) for their patients with SCN. The dental care provider's survey results indicated a shortage of dentists (54.7%) in the region and other factors that pose challenges to special care, like the severity of the disability of patients with SCN (50%), family structure (46.7%), treatment cost (35.6%) and transportation (32.8%). Patients with SCN in Saudi Arabia had a high appraisal of access to dental care and were very satisfied with dental treatment results. However, the presence of a dental care provider in the same rehabilitation centre was a major concern. The severity of the disability and the patient's cooperation were the major factors that may have affected the decision of the dental care provider. [ABSTRACT FROM AUTHOR]

Published

2024

11. Neural network architecture of a mammalian brain.

Author

Swanson, Larry W., Hahn, Joel D., and Sporns, Olaf

Subjects

*CENTRAL nervous system, *NEURAL circuitry, *SUPRACHIASMATIC nucleus, *GRAY matter (Nerve tissue), *BIOLOGICAL rhythms

Abstract

Connectomics research is making rapid advances, although models revealing general principles of connectional architecture are far from complete. Our analysis of 106 published connection reports indicates that the adult rat brain interregional connectome has about 76,940 of a possible 623,310 axonal connections between its 790 gray matter regions mapped in a reference atlas, equating to a network density of 12.3%. We examined the sexually dimorphic network using multiresolution consensus clustering that generated a nested hierarchy of interconnected modules/subsystems with three first-order modules and 157 terminal modules in females. Top-down hierarchy analysis suggests a mirror-image primary module pair in the central nervous system's rostral sector (forebrain-midbrain) associated with behavior control, and a single primary module in the intermediate sector (rhombicbrain) associated with behavior execution; the implications of these results are considered in relation to brain development and evolution. Bottom-up hierarchy analysis reveals known and unfamiliar modules suggesting strong experimentally testable hypotheses. Global network analyses indicate that all hubs are in the rostral module pair, a rich club extends through all three primary modules, and the network exhibits small-world attributes. Simulated lesions of all regions individually enabled ranking their impact on global network organization, and the visual path from the retina was used as a specific example, including the effects of cyclic connection weight changes from the endogenous circadian rhythm generator, suprachiasmatic nucleus. This study elucidates principles of interregional neuronal network architecture for a mammalian brain and suggests a strategy for modeling dynamic structural connectivity. [ABSTRACT FROM AUTHOR]

Published

2024

12. Enhancing Bioluminescence Imaging of Cultured Tissue Explants Using Optical Telecompression.

Author

Myung, Jihwan

Subjects

*NUMERICAL apertures, *OPTICAL apertures, *SUPRACHIASMATIC nucleus, *DIGITAL photography, *TISSUE culture, *BIOLUMINESCENCE

Abstract

Long-term observation of single-cell oscillations within tissue networks is now possible by combining bioluminescence reporters with stable tissue explant culture techniques. This method is particularly effective in revealing the network dynamics in systems with slow oscillations, such as circadian clocks. However, the low intensity of luciferase-based bioluminescence requires signal amplification using specialized cameras (e.g., I-CCDs and EM-CCDs) and prolonged exposure times, increasing baseline noise and reducing temporal resolution. To address this limitation, we implemented a cost-effective optical enhancement technique called telecompression, first used in astrophotography and now commonly used in digital photography. By combining a high numerical aperture objective lens with a magnification-reducing relay lens, we significantly increased the collection efficiency of the bioluminescence signal without raising the baseline CCD noise. This method allows for shorter exposure times in time-lapse imaging, enhancing temporal resolution and enabling more precise period estimations. Our implementation demonstrates the feasibility of telecompression for enhancing bioluminescence imaging for the tissue-level network observation of circadian clocks. [ABSTRACT FROM AUTHOR]

Published

2024

13. Invited Speaker Abstracts.

Subjects

*SLEEP latency, *SUPRACHIASMATIC nucleus, *MELANOPSIN, *GENETIC risk score, *RAPID eye movement sleep, *SLEEP duration, *SLEEP interruptions, *NON-REM sleep

Abstract

This document contains abstracts from a sleep research conference covering various topics. The first abstract discusses the long-term effects of perinatal stress exposure on adult health, particularly in relation to sleep disturbances. The second abstract proposes a new definition of sleep cycles based on fractal neural activity. The third abstract explores the different features of obstructive sleep apnea (OSA) in women, including differences in symptoms, co-morbidities, and treatment. The fourth abstract discusses the subtyping of insomnia disorder based on objective sleep measures and its implications for treatment. Other abstracts cover topics such as sleep bruxism in pediatric OSA, the role of dental medicine in sleep medicine, the effects of sleep deprivation on the circadian clock, the retinal mechanisms underlying caffeine effects on sleep-wake regulation, and the phosphorylation hypothesis of sleep. The document also highlights the increased risk of sleep problems and impaired cardiovascular control in children born preterm and growth restricted, as well as the challenges in diagnosing and managing pediatric OSA due to arousals. It further discusses Upper Airway Resistance Syndrome (UARS) in children, including its symptoms, diagnosis, and treatment options. The text emphasizes the importance of early diagnosis and intervention for UARS in children to prevent long-term complications. [Extracted from the article]

Published

2024

14. Pharmacologic blockade of nicotinic receptors in the suprachiasmatic nucleus increases ovarian atresia and inhibits follicular growth.

Author

Vieyra, Elizabeth, Calderón, Roberto, Linares, Rosa, Rosas, Gabriela, Ramírez, Deyra A., Espinoza, Julieta A., Chaparro, Andrea, Silva, Carlos‐Camilo, Domínguez, Roberto, and Morales‐Ledesma, Leticia

Subjects

*OVARIAN atresia, *ESTRUS, *NICOTINIC receptors, *OVARIAN follicle, *SUPRACHIASMATIC nucleus

Abstract

Reproduction in all mammalian species depends on the growth and maturation of ovarian follicles, that is, folliculogenesis. Follicular development can culminate with the rupture of mature follicles and the consequent expulsion of their oocytes (ovulation) or in atresia, characterized by the arrest of development and eventual degeneration. These processes are regulated by different neuroendocrine signals arising at different hypothalamic nuclei, including the suprachiasmatic nucleus (SCN). In the later, the activation of muscarinic receptors (mAChRs) and nicotinic receptors (nAChRs) by acetylcholine is essential for the regulation of the pre‐ovulatory signals that stimulate the rupture of mature follicles. To evaluate the participation of the nAChRs in the SCN throughout the oestrous cycle in the regulation of the hypothalamic–pituitary–ovarian axis. For this purpose, 90‐day‐old adult female rats in metoestrus, dioestrus, proestrus or oestrus were microinjected into the left‐ or right‐SCN with 0.3 μL of saline solution as vehicle or with 0.225 μg of mecamylamine (Mec), a non‐selective antagonist of the nicotinic receptors, diluted in 0.3 μL of vehicle. The animals were sacrificed when they presented vaginal cornification, indicative of oestrus stage, and the effects of the unilateral pharmacological blockade of the nAChRs in the SCN on follicular development, ovulation and secretion of oestradiol and follicle‐stimulating hormone (FSH) were evaluated. The microinjection of Mec decreased the serum levels of FSH, which resulted in a lower number of growing and healthy follicles and an increase in atresia. The higher percentage of atresia in pre‐ovulatory follicles was related to a decrease in the number of ova shed and abnormalities in oestradiol secretion. We also detected asymmetric responses between the left and right treatments that depended on the stage of the oestrous cycle. The present results allow us to suggest that during all the stages of the oestrous cycle, cholinergic signals that act on the nAChRs in the SCN are pivotal to modulate the secretion of gonadotropins and hence the physiology of the ovaries. Further research is needed to determine if such signals are generated by the cholinergic neurons in the SCN or by cholinergic afferents to the SCN. [ABSTRACT FROM AUTHOR]

Published

2024

15. Peripheral clock gene oscillations are perturbed in neonatal and adult rat offspring raised under adverse limited bedding conditions.

Author

Delorme, Tara, Kiessling, Silke, Long, Hong, Cermakian, Nicolas, and Walker, Charles

Subjects

Female, Rats, Animals, Circadian Rhythm, Corticosterone, ARNTL Transcription Factors, Circadian Clocks, Suprachiasmatic Nucleus

Abstract

Circadian (24-h) rhythms in the suprachiasmatic nucleus (SCN) are established in utero in rodents, but rhythmicity of peripheral circadian clocks appears later in postnatal development. Since peripheral oscillators can be influenced by maternal feeding and behavior, we investigated whether exposure to the adverse environmental conditions of limited bedding (LB) during postnatal life would alter rhythmicity in the SCN, adrenal gland and liver in neonatal (postnatal day PND10), juvenile (PND28) and adult rats. We also examined locomotor activity in adults. Limited bedding increased nursing time and slightly increased fragmentation of maternal behavior. Exposure to LB reduced the amplitude of Per2 in the SCN on PND10. Adrenal clock gene expression (Bmal1, Per2, Cry1, Rev-erbα, Dbp) and corticosterone secretion were rhythmic at all ages in NB offspring, whereas rhythmicity of Bmal1, Cry1 and corticosterone was abolished in neonatal LB pups. Circadian gene expression in the adrenal and liver was well established by PND28. In adults, liver expression of several circadian genes was increased at specific daytimes by LB and the microstructure of locomotor behavior was altered. Thus, changes in maternal care and behavior might provide important signals to the maturing peripheral oscillators and modify, in particular their output functions in the long-term.

Published

2023

16. An intricate relationship between circadian rhythm dysfunction and psychiatric diseases

Author

Saptadip Samanta and Debasis Bagchi

Subjects

suprachiasmatic nucleus, circadian rhythm dysfunction, psychiatric disorders, melatonin, cortisol, antipsychotic treatment, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

There is a complex relationship between circadian rhythm dysfunctions and various psychiatric disorders. Circadian (~24 h) rhythms indicate the rhythmic change of different physiological activities in relation to the environmental light-dark cycle. Shift work, light exposure at night, and chronic and acute jet lag affect circadian rhythm that have a negative impact on psychological functions, and behaviors. Additionally, professional stress, mental instability, and social disintegration influence psychiatric disorders. PubMed/MEDLINE, Springer Nature, Science Direct (Elsevier), Wiley Online, ResearchGate, and Google Scholar databases were searched to collect relevant articles. Circadian rhythm disruption causes impaired neurotransmitter release, impaired melatonin and cortisol rhythm, metabolic dysfunctions, neuroinflammation, and neural apoptosis; collectively these factors influence the development of psychiatric disorders. Circadian dysfunction also alters the expression of several clock control genes in the mesolimbic areas that are associated with pathologies of psychiatric disorders. Additionally, chronotherapy and applications of anti-psychotic medicine can improve psychiatric diseases. This review focuses on the effects of circadian clock dysfunction on the vulnerability of psychiatric disorders and the implications of chronotherapy.

Published

2024

17. Efferent pathways from the suprachiasmatic nucleus to the horizontal limbs of diagonal band promote NREM sleep during the dark phase in mice

Author

Lei Chen, Changfeng Chen, Qiaoling Jin, Yue Liang, Jian Wu, Pingping Zhang, Juan Cheng, and Liecheng Wang

Subjects

Suprachiasmatic nucleus, Basal forebrain, Sleep–wake, Non–rapid eye movement sleep, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurophysiology and neuropsychology, QP351-495

Abstract

Abstract The regulation of circadian rhythms and the sleep–wake states involves in multiple neural circuits. The suprachiasmatic nucleus (SCN) is a circadian pacemaker that controls the rhythmic oscillation of mammalian behaviors. The basal forebrain (BF) is a critical brain region of sleep–wake regulation, which is the downstream of the SCN. Retrograde tracing of cholera toxin subunit B showed a direct projection from the SCN to the horizontal limbs of diagonal band (HDB), a subregion of the BF. However, the underlying function of the SCN–HDB pathway remains poorly understood. Herein, activation of this pathway significantly increased non–rapid eye movement (NREM) sleep during the dark phase by using optogenetic recordings. Moreover, activation of this pathway significantly induced NREM sleep during the dark phase for first 4 h by using chemogenetic methods. Taken together, these findings reveal that the SCN–HDB pathway participates in NREM sleep regulation and provides direct evidence of a novel SCN-related pathway involved in sleep–wake states regulation.

Published

2024

18. Diurnal modulations of neuropeptides ‘cocaine- and amphetamine- regulated transcript’ and ‘Neuropeptide Y’ in the brain of <italic>E. cyanophlyctis</italic>.

Author

Koli, Sunil, Shetye, Ketaki, Bhargava, Shobha, and Sagarkar, Sneha

Subjects

*NEUROPEPTIDE Y, *PREOPTIC area, *SUPRACHIASMATIC nucleus, *RAPHE nuclei, *NEUROPEPTIDES

Abstract

Cocaine- and amphetamine- regulated transcript (CART) and Neuropeptide Y (NPY) primarily regulate energy homeostasis. Anurans exhibit diurnal behavioral rhythm, but the response of central neuropeptides to the Day-Night cycle is not elucidated. In this study, we have examined the profile of CART and NPY in the brain of Euphlyctis cyanophlyctis from 6:00 h to 24:00 h. Although expressions of CART and NPY changed with time of the day, circadian oscillation was observed only in expression of CART in anteroventral tegmentum (AV). CART exhibited a single peak in preoptic area (POA), Edinger-Westphal nucleus (EW), nucleus isthmus (NI) and raphe nucleus (Ra); two peaks in ventral hypothamalus (vHy), habenula (Hb) and torus semicircularis (TS). NPY exhibited single peak in TS and suprachiasmatic nucleus (SCN); two peaks in POA, vHy, AV and EW. The daily modulations of these neuropeptides may contribute to their physiological activities and are evolutionarily conserved. [ABSTRACT FROM AUTHOR]

Published

2024

19. Circadian disruptions and their role in the development of hypertension.

Author

Crowthers, Raymond, Trinh Thi Mong Nguyen, and Martinez, Diana

Subjects

AUTONOMIC nervous system, BLOOD pressure, SUPRACHIASMATIC nucleus, CIRCADIAN rhythms, CHRONOBIOLOGY disorders

Abstract

Circadian fluctuations in physiological setpoints are determined by the suprachiasmatic nucleus (SCN) which exerts control over many target structures within and beyond the hypothalamus via projections. The SCN, or central pacemaker, orchestrates synchrony between the external environment and the internal circadian mechanism. The resulting cycles in hormone levels and autonomic nervous system (ANS) activity provide precise messages to specific organs, adjusting, for example, their sensitivity to approaching hormones or metabolites. The SCN responds to both photic (light) and non-photic input. Circadian patterns are found in both heart rate and blood pressure, which are linked to daily variations in activity and autonomic nervous system activity. Variations in blood pressure are of great interest as several cardiovascular diseases such as stroke, arrhythmias, and hypertension are linked to circadian rhythm dysregulation. The disruption of normal day-night cycles, such as in shift work, social jetlag, or eating outside of normal hours leads to desynchronization of the central and peripheral clocks. This desynchronization leads to disorganization of the cellular processes that are normally driven by the interactions of the SCN and photic input. Here, we review autonomic system function and dysfunction due to regulation and interaction between different cardiorespiratory brain centers and the SCN, as well as social, lifestyle, and external factors that may impact the circadian control of blood pressure. [ABSTRACT FROM AUTHOR]

Published

2024

20. The role of N6‐methyladenosine RNA methylation in the crosstalk of circadian clock and neuroinflammation in rodent suprachiasmatic nuclei.

Author

Filipovská, Eva, Čočková, Zuzana, Černá, Barbora, Kubištová, Aneta, Spišská, Veronika, Telenský, Petr, and Bendová, Zdeňka

Subjects

*PRIMARY cell culture, *SUPRACHIASMATIC nucleus, *RNA methylation, *REACTIVE oxygen species, *CELL nuclei, *CLOCK genes, *MOLECULAR clock

Abstract

N6‐methyladenosine (m6A) is the most abundant epitranscriptomic mark that regulates the fate of RNA molecules. Recent studies have revealed a bidirectional interaction between m6A modification and the circadian clock. However, the precise temporal dynamics of m6A global enrichment in the central circadian pacemaker have not been fully elucidated. Our study investigates the relationship between FTO demethylase and molecular clocks in primary cells of the suprachiasmatic nucleus (SCN). In addition, we examined the effects of lipopolysaccharide (LPS) on Fto expression and the role of FTO in LPS‐induced reactive oxygen species (ROS) production in primary SCN cell culture. We observed circadian rhythmicity in the global m6A levels, which mirrored the rhythmic expression of the Fto demethylase. Silencing FTO using siRNA reduced the mesor of Per2 rhythmicity in SCN primary cells and extended the period of the PER2 rhythm in SCN primary cell cultures from PER2::LUC mice. When examining the immune response, we discovered that exposure to LPS upregulated global m6A levels while downregulating Fto expression in SCN primary cell cultures. Interestingly, we found a loss of circadian rhythmicity in Fto expression following LPS treatment, indicating that the decrease of FTO levels may contribute to m6A upregulation without directly regulating its circadian rhythm. To explore potential protective mechanisms against neurotoxic inflammation, we examined ROS production following LPS treatment in SCN primary cell cultures pretreated with FTO siRNA. We observed a time‐dependent pattern of ROS induction, with significant peak at 32 h but not at 20 h after synchronization. Silencing the FTO demethylase abolished ROS induction following LPS exposure, supporting the hypothesis that FTO downregulation serves as a protective mechanism during LPS‐induced neuroinflammation in SCN primary cell cultures. [ABSTRACT FROM AUTHOR]

Published

2024

21. Resistance of Pseudomonas aeruginosa and Staphylococcus aureus to the airway epithelium oxidative response assessed by a cell-free in vitro assay.

Author

Petithomme-Nanrocki, Maïwenn, Nicolau-Guillaumet, Nathan, Borie, Nicolas, Haudrechy, Arnaud, Renault, Jean-Hugues, Moussalih, Sophie, Muggeo, Anaëlle, and Guillard, Thomas

Subjects

*REACTIVE oxygen species, *PSEUDOMONAS aeruginosa, *STAPHYLOCOCCUS aureus, *HIGH throughput screening (Drug development), *HYDROGEN peroxide, *SUPRACHIASMATIC nucleus

Abstract

The antibacterial oxidative response, which relies on the production of hydrogen peroxide (H2O2) and hypothiocyanite (OSCN-), is a major line of defense protecting the human airway epithelium (HAE) from lesions when infected. The in vitro studies of the oxidative responses are performed mainly by one-shot H2O2 exposure that does not recapitulate the complex H2O2/LPO/SCN- system releasing the reactive oxygen species in airway secretions. A cell-free in vitro assay mimicking this system has been described but was not fully characterized. Here, we comprehensively characterized the hourly H2O2/OSCN- concentrations produced within this in vitro assay and assessed the resistance of Pseudomonas aeruginosa and Staphylococcus aureus clinical strains to the HAE oxidative response. We found that H2O2/OSCN- were steadily produced from 7h and up to 25h, but OSCN- was detoxified in 15 minutes by bacteria upon exposure. Preliminary tests on PA14 showed survival rates at 1-hour post-exposure (hpe) to H2O2 of roughly 50% for 105 and 107 colony-forming unit (CFU)/mL inocula, while 102 and 104 CFU/mL inocula were cleared after one hpe. Thirteen clinical strains were then exposed, highlighting that conversely to P. aeruginosa, S. aureus showed resistance to oxidative stress independently of its antibiotic resistance phenotype. Our results demonstrated how this in vitro assay can be helpful in assessing whether pathogens can resist the antibacterial oxidative HAE response. We anticipate these findings as a starting point for more sophisticated in vitro models that could serve as high-throughput screening for molecules targeting the bacterial antioxidant response. [ABSTRACT FROM AUTHOR]

Published

2024

22. Sweetened caffeine drinking revealed behavioral rhythm independent of the central circadian clock in male mice.

Author

Tahara, Yu, Ding, Jingwei, Ito, Akito, and Shibata, Shigenobu

Subjects

CIRCADIAN rhythms, MICE, CHRONOTYPE, CAFFEINE, HYPOTHALAMUS, SUPRACHIASMATIC nucleus

Abstract

Caffeine consumption is associated with the evening chronotype, and caffeine administration in mice results in prolonged period of the circadian rhythm in locomotor activity. However, as caffeine is bitter, sweetened caffeine is preferred by humans and mice; yet, its impact on the circadian clock has not been explored. In this study, mice were provided with freely available sweetened caffeine to investigate its effects on behavioral rhythms and peripheral clocks. Mice that freely consumed sweetened caffeine shifted from nocturnal to diurnal activity rhythms. In addition to the light-dark entrained behavioral rhythm component, some animals exhibited free-running period longer than 24-h. Intraperitoneal administration of caffeine at the beginning of the light phase also acutely induced diurnal behavior. The behavioral rhythms with long period (26–30 h) due to sweetened caffeine were observed even in mice housed under constant light or with a lesioned central circadian clock located in the suprachiasmatic nucleus of the hypothalamus; however, the rhythmicity was unstable. PER2::LUCIFERASE rhythms in peripheral tissues, such as the kidney, as measured via in vivo whole-body imaging during caffeine consumption, showed reduced amplitude and desynchronized phases among individuals. These results indicate that consumption of sweetened caffeine induces diurnal and long-period behavioral rhythms irrespective of the central clock, causing desynchronization of the clock in the body. [ABSTRACT FROM AUTHOR]

Published

2024

23. Loss of Cldn5 -and increase in Irf7-in the hippocampus and cerebral cortex of diabetic mice at the early symptomatic stage.

Author

Carús-Cadavieco, Marta, González de la Fuente, Sandra, Berenguer López, Inés, Serrano-Lope, Miguel A., Aguado, Begoña, Guix, Francesc, Palomer, Ernest, and Dotti, Carlos G.

Subjects

CEREBRAL cortex, HIPPOCAMPUS (Brain), INTERFERON regulatory factors, TRANSFORMING growth factors, TYPE 2 diabetes, SUPRACHIASMATIC nucleus

Abstract

Analyzing changes in gene expression within specific brain regions of individuals with Type 2 Diabetes (T2DM) who do not exhibit significant cognitive deficits can yield valuable insights into the mechanisms underlying the progression towards a more severe phenotype. In this study, transcriptomic analysis of the cortex and hippocampus of mice with long-term T2DM revealed alterations in the expression of 28 genes in the cerebral cortex and 15 genes in the hippocampus. Among these genes, six displayed consistent changes in both the cortex and hippocampus: Interferon regulatory factor 7 (Irf7), Hypoxia-inducible factor 3 alpha (Hif-3α), period circadian clock 2 (Per2), xanthine dehydrogenase (Xdh), and Transforming growth factor β-stimulated clone 22/TSC22 (Tsc22d3) were upregulated, while Claudin-5 (Cldn5) was downregulated. Confirmation of these changes was achieved through RT-qPCR. At the protein level, CLDN5 and IRF7 exhibited similar alterations, with CLDN5 being downregulated and IRF7 being upregulated. In addition, the hippocampus and cortex of the T2DM mice showed decreased levels of IκBα, implying the involvement of NF-κB pathways as well. Taken together, these results suggest that the weakening of the blood-brain barrier and an abnormal inflammatory response via the Interferon 1 and NF-κB pathways underlie cognitive impairment in individuals with long-standing T2DM [ABSTRACT FROM AUTHOR]

Published

2024

24. Circadian rhythms and breast cancer: unraveling the biological clock's role in tumor microenvironment and ageing.

Author

Yalan Yan, Lanqian Su, Shanshan Huang, Qihui He, Jiaan Lu, Huiyan Luo, Ke Xu, Guanhu Yang, Shangke Huang, and Hao Chi

Subjects

VASOACTIVE intestinal peptide, CIRCADIAN rhythms, COMBINATION drug therapy, CLOCK genes, SUPRACHIASMATIC nucleus

Abstract

Breast cancer (BC) is one of the most common and fatal malignancies among women worldwide. Circadian rhythms have emerged in recent studies as being involved in the pathogenesis of breast cancer. In this paper, we reviewed the molecular mechanisms by which the dysregulation of the circadian genes impacts the development of BC, focusing on the critical clock genes, brain and muscle ARNT-like protein 1 (BMAL1) and circadian locomotor output cycles kaput (CLOCK). We discussed how the circadian rhythm disruption (CRD) changes the tumor microenvironment (TME), immune responses, inflammation, and angiogenesis. The CRD compromises immune surveillance and features and activities of immune effectors, including CD8+ T cells and tumor-associated macrophages, that are important in an effective anti-tumor response. Meanwhile, in this review, we discuss bidirectional interactions: age and circadian rhythms, aging further increases the risk of breast cancer through reduced vasoactive intestinal polypeptide (VIP), affecting suprachiasmatic nucleus (SCN) synchronization, reduced ability to repair damaged DNA, and weakened immunity. These complex interplays open new avenues toward targeted therapies by the combination of clock drugs with chronotherapy to potentiate the immune response while reducing tumor progression for better breast cancer outcomes. This review tries to cover the broad area of emerging knowledge on the tumor-immune nexus affected by the circadian rhythm in breast cancer. [ABSTRACT FROM AUTHOR]

Published

2024

25. A high-light therapy restores the circadian clock and corrects the pathological syndrome generated in restricted-fed mice.

Author

Damara, Manohar, Misra, Nisha, and Chambon, Pierre

Subjects

*SUPRACHIASMATIC nucleus, *METABOLIC syndrome, *PHOTOTHERAPY, *MEMORY loss, *NIGHT work

Abstract

Time-restricted feeding (RF) is known to shift the phasing of gene expression in most primary metabolic tissues, whereas a time misalignment between the suprachiasmatic nucleus circadian clock (SCNCC) and its peripheral CCs (PCC's) is known to induce various pathophysiological conditions, including a metabolic syndrome. We now report that a unique "light therapy," involving different light intensities (TZT0-ZT12150-TZT0-ZT12700 lx, TZT0-ZT1275-TZT0-ZT12150 lx, and TZT0-ZT12350-TZT0-ZT12700 lx), realigns the RF-generated misalignment between the SCNCC and the PCC's. Using such high-light regime, we show that through shifting the SCNCC and its activity, it is possible in a RF and "night-shifted mouse model" to prevent/correct pathophysiologies (e.g., a metabolic syndrome, a loss of memory, cardiovascular abnormalities). Our data indicate that such a "high-light regime" could be used as a unique chronotherapy, for those working on night shifts or suffering from jet-lag, in order to realign their SCNCC and PCC's, thereby preventing the generation of pathophysiological conditions. [ABSTRACT FROM AUTHOR]

Published

2024

26. Dysfunction of large‐scale brain networks underlying cognitive impairments in shift work disorder.

Author

Zhao, Yan, Feng, Sitong, Dong, Linrui, Wu, Ziyao, and Ning, Yanzhe

Subjects

*LARGE-scale brain networks, *SHIFT systems, *COGNITION disorders, *FUNCTIONAL connectivity, *SHORT-term memory, *SUPRACHIASMATIC nucleus

Abstract

Summary: It has been demonstrated that shift work can affect cognitive functions. Several neuroimaging studies have revealed altered brain function and structure for patients with shift work disorder (SWD). However, knowledge on the dysfunction of large‐scale brain networks underlying cognitive impairments in shift work disorder is limited. This study aims to identify altered functional networks associated with cognitive declines in shift work disorder, and to assess their potential diagnostic value. Thirty‐four patients with shift work disorder and 36 healthy controls (HCs) were recruited to perform the Repeatable Battery for the Assessment of Neuropsychological Status (RBANS) and resting‐state functional scans. After surface‐based preprocessing, we calculated within‐ and between‐network functional connectivity (FC) using the Dosenbach atlas. Moreover, correlation analysis was done between altered functional connectivity of large‐scale brain networks and scores of cognitive assessments in patients with shift work disorder. Finally, we established a classification model to provide features for patients with shift work disorder concerning the disrupted large‐scale networks. Compared with healthy controls, increased functional connectivity within‐networks across the seven brain networks, and between‐networks involving ventral attention network (VAN)‐subcortical network (SCN), SCN‐frontoparietal network (FPN), and somatosensory network (SMN)‐SCN were observed in shift work disorder. Decreased functional connectivity between brain networks was found in shift work disorder compared with healthy controls, including visual network (VN)‐FPN, VN‐default mode network (DMN), SMN‐DMN, dorsal attention network (DAN)‐DMN, VAN‐DMN, and FPN‐DMN. Furthermore, the altered functional connectivity of large‐scale brain networks was significantly correlated with scores of immediate memory, visuospatial, and delayed memory in patients with shift work disorder, respectively. Abnormal functional connectivity of large‐scale brain networks may play critical roles in cognitive dysfunction in shift work disorder. Our findings provide new evidence to interpret the underlying neural mechanisms of cognitive impairments in shift work disorder. [ABSTRACT FROM AUTHOR]

Published

2024

27. Exercise entrainment of musculoskeletal connective tissue clocks.

Author

Steffen, Danielle, Kjaer, Michael, and Yeung, Ching-Yan Chloé

Subjects

*CONNECTIVE tissues, *INTERVERTEBRAL disk, *MUSCULOSKELETAL system, *SUPRACHIASMATIC nucleus, *CIRCADIAN rhythms, *EXTRACELLULAR matrix

Abstract

The musculoskeletal system, crucial for movement and support, relies on the delicate balance of connective tissue homeostasis. Maintaining this equilibrium is essential for tissue health and function. There has been increasing evidence in the past decade that shows the circadian clock as a master regulator of extracellular matrix (ECM) homeostasis in several connective tissue clocks. Very recently, exercise has emerged as a significant entrainment factor for cartilage and intervertebral disk circadian rhythms. Understanding the implications of exercise on connective tissue peripheral clocks holds promise for enhancing tissue health and disease prevention. Exercise-induced factors such as heat, glucocorticoid release, mechanical loading, and inter-tissue cross talk may play pivotal roles in entraining the circadian rhythm of connective tissues. This mini review underscores the importance of elucidating the mechanisms through which exercise influences circadian rhythms in connective tissues to optimize ECM homeostasis. Leveraging exercise as a modulator of circadian rhythms in connective tissues may offer novel therapeutic approaches to physical training for preventing musculoskeletal disorders and enhancing recovery. [ABSTRACT FROM AUTHOR]

Published

2024

28. Adrenergic Agonists Activate Transcriptional Activity in Immortalized Neuronal Cells From the Mouse Suprachiasmatic Nucleus.

Author

Langiu, Monica, Dehghani, Faramarz, Hohmann, Urszula, Bechstein, Philipp, Rawashdeh, Oliver, Rami, Abdelhaq, and Maronde, Erik

Subjects

*SUPRACHIASMATIC nucleus, *VASOACTIVE intestinal peptide, *ADRENERGIC agonists, *BIOLOGICAL rhythms, *PEPTIDES

Abstract

The suprachiasmatic nucleus of the hypothalamus (SCN) houses the central circadian oscillator of mammals. The main neurotransmitters produced in the SCN are γ‐amino‐butyric acid, arginine‐vasopressin (AVP), vasoactive intestinal peptide (VIP), pituitary‐derived adenylate cyclase‐activating peptide (PACAP), prokineticin 2, neuromedin S, and gastrin‐releasing peptide (GRP). Apart from these, catecholamines and their receptors were detected in the SCN as well. In this study, we confirmed the presence of β‐adrenergic receptors in SCN and a mouse SCN‐derived immortalized cell line by immunohistochemical, immuno‐cytochemical, and pharmacological techniques. We then characterized the effects of β‐adrenergic agonists and antagonists on cAMP‐regulated element (CRE) signaling. Moreover, we investigated the interaction of β‐adrenergic signaling with substances influencing parallel signaling pathways. Our findings have potential implications on the role of stress (elevated adrenaline) on the biological clock and may explain some of the side effects of β‐blockers applied as anti‐hypertensive drugs. [ABSTRACT FROM AUTHOR]

Published

2024

29. Dysregulation of the Suprachiasmatic Nucleus Disturbs the Circadian Rhythm and Aggravates Epileptic Seizures by Inducing Hippocampal GABAergic Dysfunction in C57BL/6 Mice.

Author

Liang, Xiaoshan, Liang, Xiaotao, Zhao, Yunyan, Ding, Yuewen, Zhu, Xiaoyu, Zhou, Jieli, Qiu, Jing, Shen, Xiaoqin, and Xie, Wei

Subjects

*TEMPORAL lobe epilepsy, *SUPRACHIASMATIC nucleus, *EPILEPSY, *CIRCADIAN rhythms, *GENE expression

Abstract

The interplay between circadian rhythms and epilepsy has gained increasing attention. The suprachiasmatic nucleus (SCN), which acts as the master circadian pacemaker, regulates physiological and behavioral rhythms through its complex neural networks. However, the exact role of the SCN and its Bmal1 gene in the development of epilepsy remains unclear. In this study, we utilized a lithium–pilocarpine model to induce epilepsy in mice and simulated circadian disturbances by creating lesions in the SCN and specifically knocking out the Bmal1 gene in the SCN neurons. We observed that the pilocarpine‐induced epileptic mice experienced increased daytime seizure frequency, irregular oscillations in core body temperature, and circadian gene alterations in both the SCN and the hippocampus. Additionally, there was enhanced activation of GABAergic projections from the SCN to the hippocampus. Notably, SCN lesions intensified seizure activity, concomitant with hippocampal neuronal damage and GABAergic signaling impairment. Further analyses using the Gene Expression Omnibus database and gene set enrichment analysis indicated reduced Bmal1 expression in patients with medial temporal lobe epilepsy, potentially affecting GABA receptor pathways. Targeted deletion of Bmal1 in SCN neurons exacerbated seizures and pathology in epilepsy, as well as diminished hippocampal GABAergic efficacy. These results underscore the crucial role of the SCN in modulating circadian rhythms and GABAergic function in the hippocampus, aggravating the severity of seizures. This study provides significant insights into how circadian rhythm disturbances can influence neuronal dysfunction and epilepsy, highlighting the therapeutic potential of targeting SCN and the Bmal1 gene within it in epilepsy management. [ABSTRACT FROM AUTHOR]

Published

2024

30. Mouse Models in Circadian Rhythm and Melatonin Research.

Author

Korf, Horst‐Werner and von Gall, Charlotte

Subjects

*SUPRACHIASMATIC nucleus, *CIRCADIAN rhythms, *TRANSGENIC mice, *GENETIC transcription regulation, *CEREBROSPINAL fluid

Abstract

This contribution reviews the role of inbred and transgenic mouse strains for deciphering the mammalian melatoninergic and circadian system. It focusses on the pineal organ as melatonin factory and two major targets of the melatoninergic system, the suprachiasmatic nuclei (SCN) and the hypophysial pars tuberalis (PT). Mammalian pinealocytes sharing molecular characteristics with true pineal and retinal photoreceptors synthesize and secrete melatonin into the blood and cerebrospinal fluid night by night. Notably, neuron‐like connections exist between the deep pinealocytes and the habenular/pretectal region suggesting direct pineal‐brain communication. Control of melatonin biosynthesis in rodents involves transcriptional regulation including phosphorylation of CREB and upregulation of mPer1. In the SCN, melatonin acts upon MT1 and MT2 receptors. Melatonin is not necessary to maintain the rhythm of the SCN molecular clockwork, but it has distinct effects on the synchronization of the circadian rhythm by light, facilitates re‐entrainment of the circadian system to phase advances in the level of the SCN molecular clockwork by acting upon MT2 receptors and plays a stabilizing role in the circadian system as evidenced from locomotor activity recordings. While the effects in the SCN are subtle, melatonin is essential for PT functions. Via the MT1 receptor it drives the PT‐intrinsic molecular clockwork and the retrograde and anterograde output pathways controlling seasonal rhythmicity. Although inbred and transgenic mice do not show seasonal reproduction, the pathways from the PT are fully intact if the animals are melatonin proficient. Thus, only melatonin‐proficient strains are suited to investigate the circadian and melatoninergic systems. [ABSTRACT FROM AUTHOR]

Published

2024

31. Computational modeling of the synergistic role of GCN2 and the HPA axis in regulating the integrated stress response in the central circadian timing system.

Author

Li, Yannuo, Lu, Lingjun, Levy, Jordan L., Anthony, Tracy G., and Androulakis, Ioannis P.

Subjects

*HYPOTHALAMIC-pituitary-adrenal axis, *PHYSIOLOGICAL stress, *CIRCADIAN rhythms, *LIFE change events, *NUTRITIONAL status, *SUPRACHIASMATIC nucleus, *CLOCK genes

Abstract

The circadian timing system and integrated stress response (ISR) systems are fundamental regulatory mechanisms that maintain body homeostasis. The central circadian pacemaker in the suprachiasmatic nucleus (SCN) governs daily rhythms through interactions with peripheral oscillators via the hypothalamus-pituitary-adrenal (HPA) axis. On the other hand, ISR signaling is pivotal for preserving cellular homeostasis in response to physiological changes. Notably, disrupted circadian rhythms are observed in cases of impaired ISR signaling. In this work, we examine the potential interplay between the central circadian system and the ISR, mainly through the SCN and HPA axis. We introduce a semimechanistic mathematical model to delineate SCN's capacity for indirectly perceiving physiological stress through glucocorticoid-mediated feedback from the HPA axis and orchestrating a cellular response via the ISR mechanism. Key components of our investigation include evaluating general control nonderepressible 2 (GCN2) expression in the SCN, the effect of physiological stress stimuli on the HPA axis, and the interconnected feedback between the HPA and SCN. Simulation revealed a critical role for GCN2 in linking ISR with circadian rhythms. Experimental findings have demonstrated that a Gcn2 deletion in mice leads to rapid re-entrainment of the circadian clock following jetlag as well as to an elongation of the circadian period. These phenomena are well replicated by our model, which suggests that both the swift re-entrainment and prolonged period can be ascribed to a reduced robustness in neuronal oscillators. Our model also offers insights into phase shifts induced by acute physiological stress and the alignment/misalignment of physiological stress with external light-dark cues. Such understanding aids in strategizing responses to stressful events, such as nutritional status changes and jetlag. NEW & NOTEWORTHY: This study is the first theoretical work to investigate the complex interaction between integrated stress response (ISR) sensing and central circadian rhythm regulation, encompassing the suprachiasmatic nucleus (SCN) and hypothalamus-pituitary-adrenal (HPA) axis. The findings carry implications for the development of dietary or pharmacological interventions aimed at facilitating recovery from stressful events, such as jetlag. Moreover, they provide promising prospects for potential therapeutic interventions that target circadian rhythm disruption and various stress-related disorders. [ABSTRACT FROM AUTHOR]

Published

2024

32. From the Pineal Gland to the Central Clock in the Brain: Beginning of Studies of the Mammalian Biological Rhythms in the Institute of Physiology of the Czech Academy of Sciences.

Author

ILLNEROVÁ, Helena

Subjects

BIOLOGICAL rhythms, CHRONOBIOLOGY, SUPRACHIASMATIC nucleus, PINEAL gland, MELATONIN

Abstract

The Institute of Physiology of the Czech Academy of Sciences (CAS) has been involved in the field of chronobiology, i.e., in research on temporal regulation of physiological processes, since 1970. The review describes the first 35 years of the research mostly on the effect of light and daylength, i.e., photoperiod, on entrainment or resetting of the pineal rhythm in melatonin production and of intrinsic rhythms in the central biological clock. This clock controls pineal and other circadian rhythms and is located in the suprachiasmatic nuclei (SCN) of the hypothalamus. During the early chronobiological research, many original findings have been reported, e.g. on mechanisms of resetting of the pineal rhythm in melatonin production by short light pulses or by long exposures of animals to light at night, on modulation of the nocturnal melatonin production by the photoperiod or on the presence of high affinity melatonin binding sites in the SCN. The first evidence was given that the photoperiod modulates functional properties of the SCN and hence the SCN not only controls the daily programme of the organism but it may serve also as a calendar measuring the time of a year. During all the years, the chronobiological community has started to talk about “the Czech school of chronobiology”. At present, the today´s Laboratory of Biological Rhythms of the Institute of Physiology CAS continues in the chronobiological research and the studies have been extended to the entire circadian timekeeping system in mammals with focus on its ontogenesis, entrainment mechanisms and circadian regulation of physiological functions. [ABSTRACT FROM AUTHOR]

Published

2024

33. Therapeutic applications of melatonin in disorders related to the gastrointestinal tract and control of appetite.

Author

Moghadam Fard, Atousa, Goodarzi, Pardis, Mottahedi, Mehran, Garousi, Setareh, Zadabhari, Hamed, Kalantari Shahijan, Mohammad, Esmaeili, Saeedeh, Nabi-Afjadi, Mohsen, and Yousefi, Bahman

Subjects

SUPRACHIASMATIC nucleus, GASTROINTESTINAL system, RESEARCH personnel, MELATONIN, SECRETION

Abstract

Most animals have large amounts of the special substance melatonin, which is controlled by the light/dark cycle in the suprachiasmatic nucleus. According to what is now understood, the gastrointestinal tract (GIT) and other areas of the body are sites of melatonin production. According to recent studies, the GIT and adjacent organs depend critically on a massive amount of melatonin. Not unexpectedly, melatonin's many biological properties, such as its antioxidant, anti-inflammatory, pro-apoptotic, anti-proliferative, anti-metastasis, and antiangiogenic properties, have drawn the attention of researchers more and more. Because melatonin is an antioxidant, it produces a lot of secretions in the GIT's mucus and saliva, which shields cells from damage and promotes the development of certain GIT-related disorders. Melatonin's ability to alter cellular behavior in the GIT and other associated organs, such as the liver and pancreas, is another way that it functions. This behavior alters the secretory and metabolic activities of these cells. In this review, we attempted to shed fresh light on the many roles that melatonin plays in the various regions of the gastrointestinal tract by focusing on its activities for the first time. [ABSTRACT FROM AUTHOR]

Published

2024

34. GABAA receptor subunit composition regulates circadian rhythms in rest-wake and synchrony among cells in the suprachiasmatic nucleus.

Author

Granados-Fuentes, Daniel, Lambert, Peter, Simon, Tatiana, Mennerick, Steven, and Herzog, Erik D.

Subjects

*SUPRACHIASMATIC nucleus, *SPECIFIC gravity, *CELL nuclei, *CIRCADIAN rhythms, *PHENOTYPES

Abstract

The mammalian circadian clock located in the suprachiasmatic nucleus (SCN) produces robust daily rhythms including rest-wake. SCN neurons synthesize and respond to γ-aminobutyric acid (GABA), but its role remains unresolved. We tested the hypothesis that γ2-and δ-subunits of the GABAA receptor in the SCN differ in their regulation of synchrony among circadian cells. We used two approaches: 1) shRNA to knock-down (KD) the expression of either γ2 or δ subunits in the SCN or 2) knock-in mice harboring a point mutation in the M2 domains of the endogenous GABAA γ2 or δ subunits. KD of either γ2 or δ subunits in the SCN increased daytime running and reduced nocturnal running by reducing their circadian amplitude by a third. Similarly, δ subunit knock-in mice showed decreased circadian amplitude, increased duration of daily activity, and decreased total daily activity. Reduction, or mutation of either γ2 or δ subunits halved the synchrony among, and amplitude of, circadian SCN cells as measured by firing rate or expression of the PERIOD2 protein, in vitro. Surprisingly, overexpression of the γ2 subunit rescued these phenotypes following KD or mutation of the δ subunit, and overexpression of the δ subunit rescued deficiencies due to γ2 subunit KD or mutation. We conclude that γ2 and δ GABAA receptor subunits play similar roles in maintaining circadian synchrony in the SCN and amplitude of daily rest-wake rhythms, but that modulation of their relative densities can change the duration and amplitude of daily activities. [ABSTRACT FROM AUTHOR]

Published

2024

35. Spatiotemporal changes in Netrin/ Dscam1 signaling dictate axonal projection direction in Drosophila small ventral lateral clock neurons.

Author

Jingjing Liu, Yuedong Wang, Xian Liu, Junhai Han, and Yao Tian

Subjects

*GLYCOCALYX, *CELL adhesion molecules, *DROSOPHILA, *NEURONS, *NETRINS, *SUPRACHIASMATIC nucleus, *CALYX, *AXONS

Abstract

Axon projection is a spatial- and temporal-specific process in which the growth cone receives environmental signals guiding axons to their final destination. However, the mechanisms underlying changes in axonal projection direction without well-defined landmarks remain elusive. Here, we present evidence showcasing the dynamic nature of axonal projections in Drosophila’s small ventral lateral clock neurons (s-LNvs). Our findings reveal that these axons undergo an initial vertical projection in the early larval stage, followed by a subsequent transition to a horizontal projection in the early-to-mid third instar larvae. The vertical projection of s-LNv axons correlates with mushroom body calyx expansion, while the s-LNv-expressed Down syndrome cell adhesion molecule (Dscam1) interacts with Netrins to regulate the horizontal projection. During a specific temporal window, locally newborn dorsal clock neurons secrete Netrins, facilitating the transition of axonal projection direction in s-LNvs. Our study establishes a compelling in vivo model to probe the mechanisms of axonal projection direction switching in the absence of clear landmarks. These findings underscore the significance of dynamic local microenvironments in the complementary regulation of axonal projection direction transitions. [ABSTRACT FROM AUTHOR]

Published

2024

36. Water‐Stable Lewis Superacids as Precursors for (Pseudo)halogenogallate and ‐indate Salts.

Author

Tölke, Katharina, Porath, Sven, Neumann, Beate, Stammler, Hans‐Georg, and Hoge, Berthold

Subjects

*SUPERACIDS, *SALTS, *GALLIUM, *LEWIS acids, *SOLUBILITY, *SUPRACHIASMATIC nucleus, *GALLIUM alloys

Abstract

Tris(pentafluoroethyl)indane dihydrate, [In(C2F5)3(OH2)2], and the gallium analog, [Ga(C2F5)3(OH2)2], serve as transfer reagents for the In(C2F5)3 and Ga(C2F5)3 units, as illustrated by the preparation of salts of (pseudo)halogenotris(pentafluoroethyl)indate and ‐gallate anions, [M(C2F5)3)X]− (M=Ga, In; X=F, Cl, Br, I, CN, SCN). Due to the water tolerance and water solubility of [In(C2F5)3(OH2)2] and [Ga(C2F5)3(OH2)2], reactions can be performed in the presence of water or even in an aqueous medium. [ABSTRACT FROM AUTHOR]

Published

2024

37. Efferent pathways from the suprachiasmatic nucleus to the horizontal limbs of diagonal band promote NREM sleep during the dark phase in mice.

Author

Chen, Lei, Chen, Changfeng, Jin, Qiaoling, Liang, Yue, Wu, Jian, Zhang, Pingping, Cheng, Juan, and Wang, Liecheng

Subjects

*EFFERENT pathways, *SUPRACHIASMATIC nucleus, *NON-REM sleep, *CHOLERA toxin, *NEURAL circuitry

Abstract

The regulation of circadian rhythms and the sleep–wake states involves in multiple neural circuits. The suprachiasmatic nucleus (SCN) is a circadian pacemaker that controls the rhythmic oscillation of mammalian behaviors. The basal forebrain (BF) is a critical brain region of sleep–wake regulation, which is the downstream of the SCN. Retrograde tracing of cholera toxin subunit B showed a direct projection from the SCN to the horizontal limbs of diagonal band (HDB), a subregion of the BF. However, the underlying function of the SCN–HDB pathway remains poorly understood. Herein, activation of this pathway significantly increased non–rapid eye movement (NREM) sleep during the dark phase by using optogenetic recordings. Moreover, activation of this pathway significantly induced NREM sleep during the dark phase for first 4 h by using chemogenetic methods. Taken together, these findings reveal that the SCN–HDB pathway participates in NREM sleep regulation and provides direct evidence of a novel SCN-related pathway involved in sleep–wake states regulation. [ABSTRACT FROM AUTHOR]

Published

2024

38. Diverse genetic alteration dysregulates neuropeptide and intracellular signalling in the suprachiasmatic nuclei.

Author

Curtis, Lucy and Piggins, Hugh D.

Subjects

*SUPRACHIASMATIC nucleus, *NUCLEOTIDE sequencing, *GENE expression, *MOLECULAR clock, *CLOCK genes, *PROMOTERS (Genetics), *CIRCADIAN rhythms, *GENETIC code

Abstract

In mammals, intrinsic 24 h or circadian rhythms are primarily generated by the suprachiasmatic nuclei (SCN). Rhythmic daily changes in the transcriptome and proteome of SCN cells are controlled by interlocking transcription‐translation feedback loops (TTFLs) of core clock genes and their proteins. SCN cells function as autonomous circadian oscillators, which synchronize through intercellular neuropeptide signalling. Physiological and behavioural rhythms can be severely disrupted by genetic modification of a diverse range of genes and proteins in the SCN. With the advent of next generation sequencing, there is unprecedented information on the molecular profile of the SCN and how it is affected by genetically targeted alteration. However, whether the expression of some genes is more readily affected by genetic alteration of the SCN is unclear. Here, using publicly available datasets from recent RNA‐seq assessments of the SCN from genetically altered and control mice, we evaluated whether there are commonalities in transcriptome dysregulation. This was completed for four different phases across the 24 h cycle and was augmented by Gene Ontology Molecular Function (GO:MF) and promoter analysis. Common differentially expressed genes (DEGs) and/or enriched GO:MF terms included signalling molecules, their receptors, and core clock components. Finally, examination of the JASPAR database indicated that E‐box and CRE elements in the promoter regions of several commonly dysregulated genes. From this analysis, we identify differential expression of genes coding for molecules involved in SCN intra‐ and intercellular signalling as a potential cause of abnormal circadian rhythms. [ABSTRACT FROM AUTHOR]

Published

2024

39. Aryl hydrocarbon receptor impairs circadian regulation in Alzheimer's disease: Potential impact on glymphatic system dysfunction.

Author

Salminen, Antero

Subjects

*ARYL hydrocarbon receptors, *ALZHEIMER'S disease, *TRANSCRIPTION factors, *ALZHEIMER'S patients, *BLOOD-brain barrier, *SUPRACHIASMATIC nucleus, *SLEEP-wake cycle

Abstract

Circadian clocks maintain diurnal rhythms of sleep–wake cycle of 24 h that regulate not only the metabolism of an organism but also many other periodical processes. There is substantial evidence that circadian regulation is impaired in Alzheimer's disease. Circadian clocks regulate many properties known to be disturbed in Alzheimer's patients, such as the integrity of the blood–brain barrier (BBB) as well as the diurnal glymphatic flow that controls waste clearance from the brain. Interestingly, an evolutionarily conserved transcription factor, that is, aryl hydrocarbon receptor (AhR), impairs the function of the core clock proteins and thus could disturb diurnal rhythmicity in the BBB. There is abundant evidence that the activation of AhR signalling inhibits the expression of the major core clock proteins, such as the brain and muscle arnt‐like 1 (BMAL1), clock circadian regulator (CLOCK) and period circadian regulator 1 (PER1) in different experimental models. The expression of AhR is robustly increased in the brains of Alzheimer's patients, and protein level is enriched in astrocytes of the BBB. It seems that AhR signalling inhibits glymphatic flow since it is known that (i) activation of AhR impairs the function of the BBB, which is cooperatively interconnected with the glymphatic system in the brain, and (ii) neuroinflammation and dysbiosis of gut microbiota generate potent activators of AhR, which are able to impair glymphatic flow. I will examine current evidence indicating that activation of AhR signalling could disturb circadian functions of the BBB and impair glymphatic flow and thus be involved in the development of Alzheimer's pathology. [ABSTRACT FROM AUTHOR]

Published

2024

40. Loss of temporal coherence in the circadian metabolome across multiple tissues during ageing in mice.

Author

Buijink, M. Renate, van Weeghel, Michel, Harms, Amy, Murli, Devika S., Meijer, Johanna H., Hankemeier, Thomas, Michel, Stephan, and Kervezee, Laura

Subjects

*SUPRACHIASMATIC nucleus, *MOLECULAR clock, *METABOLOMICS, *TYPE 2 diabetes, *PARAVENTRICULAR nucleus, *CIRCADIAN rhythms, *MICE, *TISSUES

Abstract

Circadian clock function declines with ageing, which can aggravate ageing‐related diseases such as type 2 diabetes and neurodegenerative disorders. Understanding age‐related changes in the circadian system at a systemic level can contribute to the development of strategies to promote healthy ageing. The goal of this study was to investigate the impact of ageing on 24‐h rhythms in amine metabolites across four tissues in young (2 months of age) and old (22–25 months of age) mice using a targeted metabolomics approach. Liver, plasma, the suprachiasmatic nucleus (SCN; the location of the central circadian clock in the hypothalamus) and the paraventricular nucleus (PVN; a downstream target of the SCN) were collected from young and old mice every 4 h during a 24‐h period (n = 6–7 mice per group). Differential rhythmicity analysis revealed that ageing impacts 24‐h rhythms in the amine metabolome in a tissue‐specific manner. Most profound changes were observed in the liver, in which rhythmicity was lost in 60% of the metabolites in aged mice. Furthermore, we found strong correlations in metabolite levels between the liver and plasma and between the SCN and the PVN in young mice. These correlations were almost completely abolished in old mice. These results indicate that ageing is accompanied by a severe loss of the circadian coordination between tissues and by disturbed rhythmicity of metabolic processes. The tissue‐specific impact of ageing may help to differentiate mechanisms of ageing‐related disorders in the brain versus peripheral tissues and thereby contribute to the development of potential therapies for these disorders. [ABSTRACT FROM AUTHOR]

Published

2024

41. Steven A. Brown and the synchronization of circadian rhythms by body temperature cycles.

Author

Schibler, Ueli

Subjects

*BIOLOGICAL rhythms, *CIRCADIAN rhythms, *BODY temperature, *SUPRACHIASMATIC nucleus, *TISSUE culture, *CELLULAR signal transduction, *SYNCHRONIZATION

Abstract

The mammalian circadian timing system has a hierarchical architecture, with a central pacemaker located in the brain's suprachiasmatic nucleus orchestrating rhythms in behaviour and physiology. In cooperation with environmental cycles, it synchronizes the phases of peripheral oscillators operating in most cells of the body. Even cells kept in tissue culture harbour self‐sustained and cell‐autonomous circadian clocks that keep ticking throughout their lifespan. The master pacemaker in the suprachiasmatic nucleus is synchronized primarily by light–dark cycles, whereas peripheral oscillators are phase entrained by a multitude of systemic signalling pathways. These include pathways depending on feeding–fasting cycles, cellular actin polymerization dynamics, endocrine rhythms and, surprisingly, body temperature oscillations. Using tissue culture and murine models, Steve Brown was the first one to demonstrate that shallow rhythms of mammalian body temperature are timing cues (zeitgebers) for peripheral circadian clocks. [ABSTRACT FROM AUTHOR]

Published

2024

42. A critical role of Ca2+/calmodulin‐dependent protein kinase II in coupling between evening and morning circadian oscillators in the suprachiasmatic nucleus.

Author

Yoshikawa, Tomoko, Honma, Ken‐ichi, Shigeyoshi, Yasufumi, Yamagata, Yoko, and Honma, Sato

Subjects

*SUPRACHIASMATIC nucleus, *PROTEIN kinases, *MOLECULAR clock, *CALMODULIN, *MORNING

Abstract

Ca2+/calmodulin‐dependent protein kinase IIα (CaMKIIα) is widely expressed in the brain and is involved in various functions, including memory formation, mood and sleep. We previously reported that CaMKIIα is involved in the circadian molecular clock. Mice lacking functional CaMKIIα (K42R mice) exhibited a gradual increase in activity time (α decompression) of running‐wheel (RW) activity due to a lengthened circadian period (τ) of activity offset under constant darkness (DD). In the present study, to investigate the functional roles of CaMKIIα in behavioural rhythms, we measured RW and general movements simultaneously under prolonged DD. Tau became longer as the relative intensity of behaviour activity within an activity time shifted from activity onset towards activity offset. In some K42R mice, α was gradually expanded with a marked reduction of RW activity, while general movements persisted without noticeable decline, which was followed by an abrupt shortening of α (α compression) with differential phase shifts of the activity onset and offset and recovery of RW activity. These results suggest that an internal coupling between the oscillators controlling activity onset and offset is bidirectional but with different strengths. The α compression occurred recurrently in 38% of K42R mice examined with an average interval of 37 days in association with attenuation of RW activity but never in the wild‐type (WT) mice. Consistent with behavioural rhythms, the circadian period of the PER2::LUC rhythm in the cultured suprachiasmatic nucleus (SCN) slice was significantly longer in K42R than in WT. These findings are best interpreted by assuming that a loss of functional CaMKIIα attenuates the coupling between the onset and offset oscillators. [ABSTRACT FROM AUTHOR]

Published

2024

43. Online Scene Semantic Understanding Based on Sparsely Correlated Network for AR.

Author

Wang, Qianqian, Song, Junhao, Du, Chenxi, and Wang, Chen

Subjects

*STREAMING video & television, *AUGMENTED reality, *PRIOR learning, *SUPRACHIASMATIC nucleus

Abstract

Real-world understanding serves as a medium that bridges the information world and the physical world, enabling the realization of virtual–real mapping and interaction. However, scene understanding based solely on 2D images faces problems such as a lack of geometric information and limited robustness against occlusion. The depth sensor brings new opportunities, but there are still challenges in fusing depth with geometric and semantic priors. To address these concerns, our method considers the repeatability of video stream data and the sparsity of newly generated data. We introduce a sparsely correlated network architecture (SCN) designed explicitly for online RGBD instance segmentation. Additionally, we leverage the power of object-level RGB-D SLAM systems, thereby transcending the limitations of conventional approaches that solely emphasize geometry or semantics. We establish correlation over time and leverage this correlation to develop rules and generate sparse data. We thoroughly evaluate the system's performance on the NYU Depth V2 and ScanNet V2 datasets, demonstrating that incorporating frame-to-frame correlation leads to significantly improved accuracy and consistency in instance segmentation compared to existing state-of-the-art alternatives. Moreover, using sparse data reduces data complexity while ensuring the real-time requirement of 18 fps. Furthermore, by utilizing prior knowledge of object layout understanding, we showcase a promising application of augmented reality, showcasing its potential and practicality. [ABSTRACT FROM AUTHOR]

Published

2024

44. Time-restricted feeding reveals a role for neural respiratory clocks in optimizing daily ventilatory-metabolic coupling in mice.

Author

Jones, Aaron A., Marino, Gabriella M., and Arble, Deanna M.

Subjects

*CIRCADIAN rhythms, *SUPRACHIASMATIC nucleus, *MOLECULAR clock, *MICE, *RHYTHM

Abstract

The master circadian clock, located in the suprachiasmatic nuclei (SCN), organizes the daily rhythm in minute ventilation (V ̇ E). However, the extent that the daily rhythm in V ̇ E is secondary to SCN-imposed O2 and CO2 cycles (i.e., metabolic rate) or driven by other clock mechanisms remains unknown. Here, we experimentally shifted metabolic rate using time-restricted feeding (without affecting light-induced synchronization of the SCN) to determine the influence of metabolic rate in orchestrating the daily V ̇ E rhythm. Mice eating predominantly at night exhibited robust daily rhythms in O2 consumption (V ̇ O2), CO2 production (V ̇ CO2), and V ̇ E with similar peak times (approximately ZT18) that were consistent with SCN organization. However, feeding mice exclusively during the day separated the relative timing of metabolic and ventilatory rhythms, resulting in an approximately 8.5-h advance in V ̇ CO2 and a disruption of the V ̇ E rhythm, suggesting opposing circadian and metabolic influences on V ̇ E. To determine if the molecular clock of cells involved in the neural control of breathing contributes to the daily V_ E rhythm, we examined V ̇ E in mice lacking BMAL1 in Phox2b-expressing respiratory cells (i.e., BKOP mice). The ventilatory and metabolic rhythms of predominantly night-fed BKOP mice did not differ from wild-type mice. However, in contrast to wild-type mice, exclusive day feeding of BKOP mice led to an unfettered daily V̇ E rhythm with a peak time aligning closely with the daily V ̇ CO2 rhythm. Taken together, these results indicate that both daily V ̇ CO2 changes and intrinsic circadian time-keeping within Phox2b respiratory cells are predominant orchestrators of the daily rhythm in ventilation. [ABSTRACT FROM AUTHOR]

Published

2024

45. On the origin and evolution of the dual oscillator model underlying the photoperiodic clockwork in the suprachiasmatic nucleus.

Author

Evans, Jennifer A. and Schwartz, William J.

Subjects

*SUPRACHIASMATIC nucleus, *SUNRISE & sunset, *PHYSIOLOGICAL adaptation

Abstract

Decades have now passed since Colin Pittendrigh first proposed a model of a circadian clock composed of two coupled oscillators, individually responsive to the rising and setting sun, as a flexible solution to the challenge of behavioral and physiological adaptation to the changing seasons. The elegance and predictive power of this postulation has stimulated laboratories around the world in searches to identify and localize such hypothesized evening and morning oscillators, or sets of oscillators, in insects, rodents, and humans, with experimental designs and approaches keeping pace over the years with technological advances in biology and neuroscience. Here, we recount the conceptual origin and highlight the subsequent evolution of this dual oscillator model for the circadian clock in the mammalian suprachiasmatic nucleus; and how, despite our increasingly sophisticated view of this multicellular pacemaker, Pittendrigh's binary conception has remained influential in our clock models and metaphors. [ABSTRACT FROM AUTHOR]

Published

2024

46. Body Composition of Medical Staff Working on Shift Duty and Day Duty: A Cross-sectional Study.

Author

BORKHATARIYA, AVI and PATIL, DEVENDRA MANOHAR

Subjects

*SHIFT systems, *BODY composition, *MEDICAL personnel, *NIGHT work, *SUPRACHIASMATIC nucleus, *DIETARY patterns

Abstract

Introduction: The necessity for 24-hour patient care in the medical field often requires staff to work in shifts, disrupting their circadian rhythms controlled by the hypothalamus’s Suprachiasmatic Nuclei (SCN). This disruption can lead to sleep deprivation, which is linked to significant health issues such as obesity, type 2 diabetes, hypertension, and cardiovascular disease. Sleep deprivation affects body composition by altering fat distribution, muscle mass, and Body Mass Index (BMI), and changes meal preferences towards high-calorie, carbohydraterich foods. Irregular eating patterns due to hormonal and gut microbiome changes can lead to over-eating and weight gain. The sedentary nature of many shift-based jobs exacerbates the imbalance between energy intake and expenditure, promoting obesity. Aim: To address the limited research on how shift work impacts the body composition of medical staff by comparing those on shift duty to those on day duty. Materials and Methods: This study was a cross-sectional study that included medical staff between the age group of 25 to 40 years working in the Parent Institute. The subjects were divided into two equal groups consisting of 100 staff working on shift duty (study group) and 100 staff working on day duty (control group). Subjects were tested for body composition by using Karada Scan. Various parameters of body composition were compared using an unpaired t-test. Results: The day duty group consisted of 36 females and 64 males (N=100) staff with a mean age of 33.0±4.6 years while the shift duty group consisted of 36 females and 64 males (N=100) staff with a mean age of 31.9±4.4 years. The study suggests a significant difference between the two groups for BMI, skeletal muscle mass, and subcutaneous fat with a p-value <0.05. Conclusion: The study showed lower skeletal muscle mass and higher body weight, body fat percentage, visceral fat, BMI, and subcutaneous fat in medical staff working on shift duty. [ABSTRACT FROM AUTHOR]

Published

2024

47. Time-of-day effects on ex vivo muscle contractility following short-term satellite cell ablation.

Author

Kahn, Ryan E., Lieber, Richard L., Meza, Guadalupe, Dinnunhan, Fawzan, Lacham-Kaplan, Orly, Dayanidhi, Sudarshan, and Hawley, John A.

Subjects

*SATELLITE cells, *CLOCK genes, *MOLECULAR clock, *CELL populations, *STEM cells, *MUSCLE physiology, *SUPERIOR colliculus, *SUPRACHIASMATIC nucleus

Abstract

Muscle isometric torque fluctuates according to time-of-day with such variation owed to the influence of circadian molecular clock genes. Satellite cells (SCs), the muscle stem cell population, also express molecular clock genes with several contractile-related genes oscillating in a diurnal pattern. Currently, limited evidence exists regarding the relationship between SCs and contractility, although long-term SC ablation alters muscle contractile function. Whether there are acute alterations in contractility following SC ablation and with respect to the time-of-day is unknown. We investigated whether short-term SC ablation affected contractile function at two times of day and whether any such alterations led to different extents of eccentric contraction-induced injury. Using an established mouse model to deplete SCs, we characterized muscle clock gene expression and ex vivo contractility at two times-of-day (morning: 0700 and afternoon: 1500). Morning-SC+ animals demonstrated ∼25%–30% reductions in tetanic/eccentric specific forces and, after eccentric injury, exhibited ∼30% less force-loss and ∼50% less dystrophinnegative fibers versus SC− counterparts; no differences were noted between Afternoon groups (Morning-SC+: −5.63 ± 0.61, Morning-SC−: −7.93 ± 0.61; N/cm2; P < 0.05) (Morning-SC+: 32 ± 2.1, Morning-SC−: 64 ± 10.2; dystrophinnegative fibers; P < 0.05). As Ca++ kinetics underpin force generation, we also evaluated caffeine-induced contracture force as an indirect marker of Ca++ availability and found similar force reductions in Morning-SC+ vs. SC− mice. We conclude that force production is reduced in the presence of SCs in the morning but not in the afternoon, suggesting that SCs may have a time-of-day influence over contractile function. NEW & NOTEWORTHY: Muscle isometric torque fluctuates according to time-of-day with such variation owed to molecular clock regulation. Satellite cells (SCs) have recently demonstrated diurnal characteristics related to muscle physiology. In our work, force production was reduced in the presence versus absence of SCs in the morning but, not in the afternoon. Morning-SC+ animals, producing lower force, sustained lesser degrees of injury versus SC− counterparts. One potential mechanism underpinning lower forces produced appears to be lower calcium availability. [ABSTRACT FROM AUTHOR]

Published

2024

48. Psychedelics in developmental stuttering to modulate brain functioning: a new therapeutic perspective?

Author

Pasculli, Giuseppe, Busan, Pierpaolo, Jackson, Eric S., Alm, Per A., De Gregorio, Danilo, Maguire, Gerald A., Goodwin, Guy M., Gobbi, Gabriella, Erritzoe, David, and Carhart-Harris, Robin L.

Subjects

SUPRACHIASMATIC nucleus, STUTTERING, HALLUCINOGENIC drugs, SOCIAL anxiety, POST-traumatic stress disorder, BRAIN metabolism

Abstract

Developmental stuttering (DS) is a neurodevelopmental speech-motor disorder characterized by symptoms such as blocks, repetitions, and prolongations. Persistent DS often has a significant negative impact on quality of life, and interventions for it have limited efficacy. Herein, we briefly review existing research on the neurophysiological underpinnings of DS -specifically, brain metabolic and default mode/social-cognitive networks (DMN/SCN) anomaliesarguing that psychedelic compounds might be considered and investigated (e.g., in randomized clinical trials) for treatment of DS. The neural background of DS is likely to be heterogeneous, and some contribution from genetically determinants of metabolic deficiencies in the basal ganglia and speech-motor cortical regions are thought to play a role in appearance of DS symptoms, which possibly results in a cascade of events contributing to impairments in speechmotor execution. In persistent DS, the difficulties of speech are often linked to a series of associated aspects such as social anxiety and social avoidance. In this context, the SCN and DMN (also influencing a series of fronto-parietal, somatomotor, and attentional networks) may have a role in worsening dysfluencies. Interestingly, brain metabolism and SCN/DMN connectivity can be modified by psychedelics, which have been shown to improve clinical evidence of some psychiatric conditions (e.g., depression, post-traumatic stress disorder, etc.) associated with psychological constructs such as rumination and social anxiety, which also tend to be present in persistent DS. To date, while there have been no controlled trials on the effects of psychedelics in DS, anecdotal evidence suggests that these agents may have beneficial effects on stuttering and its associated characteristics. We suggest that psychedelics warrant investigation in DS. [ABSTRACT FROM AUTHOR]

Published

2024

49. Alpha-synuclein expression in oxytocin neurons of young and old bovine brains.

Author

NIYONZIMA, Yvan Bienvenu, Yuuki ASATO, and Hiroya KADOKAWA

Subjects

SYNUCLEINS, NEURONS, BRAIN physiology, SUPRAOPTIC nucleus, PROTEIN expression

Abstract

Understanding of central nervous system mechanisms underlying age-related infertility remains limited. Fibril α-synuclein, distinct from its monomeric form, is implicated in age-related diseases. Notably, fibril α-synuclein spreads among neurons, similar to prions, from damaged old neurons in cortex and hippocampus to healthy neurons. However, less is known whether α-synuclein propagates into oxytocin neurons, which play crucial roles in reproduction. We compared α-synuclein expression in the oxytocin neurons in suprachiasmatic nucleus (SCN), supraoptic nucleus (SON), paraventricular hypothalamic nucleus (PVN), and posterior pituitary (PP) gland of healthy heifers and aged cows to determine its role in age-related infertility. We analyzed mRNA and protein expression, along with Congo red histochemistry and fluorescent immunohistochemistry for oxytocin and α-synuclein, followed by confocal microscopy with Congo red staining. Both mRNA and protein expressions of α-synuclein were confirmed in the bovine cortex, hippocampus, SCN, SON, PVN, and PP tissues. Significant differences in α-synuclein mRNA expressions were observed in the cortex and hippocampus between young heifers and old cows. Western blots showed five bands of α-synuclein, probably reflecting monomers, dimers, and oligomers, in the cortex, hippocampus, SCN, SON, PVN, and PP tissues, and there were significant differences in some bands between the young heifers and old cows. Bright-field and polarized light microscopy did not detect obvious amyloid deposition in the aged hypothalami; however, higher-sensitive confocal microscopy unveiled strong positive signals for Congo red and α-synuclein in oxytocin neurons in the aged hypothalami. α-synuclein was expressed in oxytocin neurons, and some differences were observed between young and old hypothalami. [ABSTRACT FROM AUTHOR]

Published

2024

50. The negative effect on human health due to disruption of circadian rhythm in modern times.

Author

Sharo, Hevind, Amann, Yannick, and Wozniak, Slawomir

Subjects

CIRCADIAN rhythms, CAFFEINE, SUPRACHIASMATIC nucleus, PINEAL gland, MELATONIN

Abstract

Disruptions of the circadian rhythm have shown that it can lead to significant health risks. Factors such as rapid travel across different time zones, increased exposure to artificial light, and the consumption of substances like caffeine contribute to this disruption. Understanding these disruptions and its causes is crucial for improving our health and in finding solutions. [ABSTRACT FROM AUTHOR]

Published

2024