scholarly journals TRESK is a key regulator of nocturnal suprachiasmatic nucleus dynamics and light adaptive responses

2020 ◽  
Vol 11 (1) ◽  
Author(s):  
Tatjana Lalic ◽  
Aiste Steponenaite ◽  
Liting Wei ◽  
Sridhar R. Vasudevan ◽  
Alistair Mathie ◽  
...  

Abstract The suprachiasmatic nucleus (SCN) is a complex structure dependent upon multiple mechanisms to ensure rhythmic electrical activity that varies between day and night, to determine circadian adaptation and behaviours. SCN neurons are exposed to glutamate from multiple sources including from the retino-hypothalamic tract and from astrocytes. However, the mechanism preventing inappropriate post-synaptic glutamatergic effects is unexplored and unknown. Unexpectedly we discovered that TRESK, a calcium regulated two-pore potassium channel, plays a crucial role in this system. We propose that glutamate activates TRESK through NMDA and AMPA mediated calcium influx and calcineurin activation to then oppose further membrane depolarisation and rising intracellular calcium. Hence, in the absence of TRESK, glutamatergic activity is unregulated leading to membrane depolarisation, increased nocturnal SCN firing, inverted basal calcium levels and impaired sensitivity in light induced phase delays. Our data reveals TRESK plays an essential part in SCN regulatory mechanisms and light induced adaptive behaviours.

2017 ◽  
Vol 112 (3) ◽  
pp. 244a
Author(s):  
Matteo M. Ottaviani ◽  
Vincenzo Mastrolia ◽  
Laura Guarina ◽  
Emilio Carbone ◽  
Petronel Tuluc

2017 ◽  
Vol 284 (1857) ◽  
pp. 20170800 ◽  
Author(s):  
Akira Yamawo ◽  
Hiromi Mukai

Numerous organisms integrate information from multiple sources and express adaptive behaviours, but how they do so at different developmental stages remains to be identified. Seeds, which are the embryonic stage of plants, need to make decisions about the timing of emergence in response to environmental cues related to survival. We investigated the timing of emergence of Plantago asiatica (Plantaginaceae) seed while manipulating the presence of Trifolium repens seed and the relatedness of neighbouring P. asiatica seed. The relatedness of neighbouring P. asiatica seed and the presence of seeds of T. repens did not on their own influence the timing of P. asiatica emergence. However, when encountering a T. repens seed, a P. asiatica seed emerged faster in the presence of a sibling seed than in the presence of a non-sibling seed. Water extracts of seeds gave the same result. We show that P. asiatica seeds integrate information about the relatedness of neighbouring P. asiatica seeds and the presence of seeds of a different species via water-soluble chemicals and adjust their emergence behaviour in response. These findings suggest the presence of kin-dependent interspecific interactions.


Author(s):  
Rae Silver

We live in an approximately 24-hour world and circadian rhythms have evolved to adapt organisms to the opportunities presented by Earth’s 24-hour cycle of light and dark. A “master clock” located in the suprachiasmatic nucleus (SCN) of the brain orchestrates daily rhythms in all manner of behavioral, endocrine, metabolic, autonomic, and homeostatic systems in our bodies. The SCN is comprised of about 20,000 neurons and about one third as many astroglia. How can so few neurons and astroglia guide so many rhythms? How do neurons time out an interval as long as a day? The answers are a case study in understanding how genes within cells, and cells within circuits, function together to perform complex activities and optimize bodily functions. While individual clock cells are found in virtually all bodily tissues, the unique connectome of the SCN, its specialized afferent inputs from the retinohypothalamic tract, and its neural and humoral outputs enable its “babel” of neuronal types to synchronize their activity and signal time to the rest of the body. At the molecular-cellular level, circadian rhythms are regulated by a 24-hour transcriptional–translational feedback loop. At the SCN tissue level, individual SCN neurons coordinate their gene expression and electrical activity, working together in circuits that sustain coherent rhythms. The SCN has many distinct cell types based on their neurotransmitters, neuropeptides, and afferent and efferent connections. There has been much progress in unraveling the dynamic network organization that underlies the SCN network’s communications. Though the precise anatomical connections underlying interneuronal communication in the SCN are not completely understood, key signaling mechanisms that sustain the SCN’s intrinsic rhythmicity have been tackled using intersectional genomic tools. Transgenic animals that permit the visualization of clock gene–protein expression have enabled analysis of SCN network activity over time. Availability of animals bearing mutations in clock genes or proteins enable the determination of changes within neurons, among neurons in networks, and their impact on behavior. The use of continuous readouts of circadian activity that track behavior, or clock gene expression, or electrical activity changes over time, within an SCN or a single neuron, leads the way to unraveling mechanisms sustaining the circadian timing system. Because the results of circadian studies generate huge amounts of data, the entry of mathematical modelers and statisticians into the field has begun to yield useful and testable predictions on how these multiplexed systems work to adapt to our 24-hour world.


1996 ◽  
Vol 157 ◽  
pp. 242-243
Author(s):  
C. G. Mundell ◽  
A. Pedlar ◽  
D. L. Shone ◽  
M. W. Asif ◽  
A. Robinson ◽  
...  

Bars are thought to play a crucial role in the fueling of AGN (see e.g., Mundell et al., in these proceedings and references therein), and as part of a project to investigate this, we have studied the neutral hydrogen structure in the bar of the Seyfert 1.5 galaxy NGC 4151.High-sensitivity VLA observations have enabled us to image the neutral hydrogen emission from the bar of NGC 4151 in unprecedented detail, and is a continuation of the work by Pedlar et al. (1992).Figure 1 shows images of integrated neutral hydrogen emission. The large scale emission extends over approximately 20 kpc and the outer part consists of a well-defined two-armed spiral which originates from a fat bar at a radius of about 5 kpc. The bar shows complex structure, including two sharp features which are reminiscent of the shocks seen in many simulations, e.g., Athanassoula (1992). These features appear to join the central 1-kpc ring discovered by Vila-Vilaró et al. (1994), and for which there appears a partial counterpart in neutral hydrogen emission.


Author(s):  
Anush Tumanyan ◽  
Narine Tadevosyan ◽  
Aleksandr Khachunts ◽  
Ira Tadevosyan

The features of heart rate variability before, during and after a brief mental load in three age groups (17–21, 22–35 and 36–60 years old) were studied. It is shown that for all groups during the mental load some tension of central regulatory mechanisms of heart is typical. The highest degree of tension is found in subjects from the III group (36–60 years old). In these subjects the recovery of regulatory systems up to the baseline took more time. These changes of regulatory systems that occur in older age group, most probably, are connected with a decrease of adaptive responses and some limitation of functional capabilities. Refs 16. Figs 2. Tables 2.


2015 ◽  
Vol 112 (13) ◽  
pp. 4140-4145 ◽  
Author(s):  
Yesser H. Belgacem ◽  
Laura N. Borodinsky

Sonic hedgehog (Shh) is a morphogenic protein that operates through the Gli transcription factor-dependent canonical pathway to orchestrate normal development of many tissues. Because aberrant levels of Gli activity lead to a wide spectrum of diseases ranging from neurodevelopmental defects to cancer, understanding the regulatory mechanisms of Shh canonical pathway is paramount. During early stages of spinal cord development, Shh specifies neural progenitors through the canonical signaling. Despite persistence of Shh as spinal cord development progresses, Gli activity is switched off by unknown mechanisms. In this study we find that Shh inverts its action on Gli during development. Strikingly, Shh decreases Gli signaling in the embryonic spinal cord by an electrical activity- and cAMP-dependent protein kinase-mediated pathway. The inhibition of Gli activity by Shh operates at multiple levels. Shh promotes cytosolic over nuclear localization of Gli2, induces Gli2 and Gli3 processing into repressor forms, and activates cAMP-responsive element binding protein that in turn represses gli1 transcription. The regulatory mechanisms identified in this study likely operate with different spatiotemporal resolution and ensure effective down-regulation of the canonical Shh signaling as spinal cord development progresses. The developmentally regulated intercalation of electrical activity in the Shh pathway may represent a paradigm for switching from canonical to noncanonical roles of developmental cues during neuronal differentiation and maturation.


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