Effects of Metabolic Energy on Synaptic Transmission and Dendritic Integration in Pyramidal Neurons

As a sophisticated computing unit, the pyramidal neuron requires sufficient metabolic energy to fuel its powerful computational capabilities. However, the majority of previous works focus on nonlinear integration and energy consumption in individual pyramidal neurons but seldom on the effects of metabolic energy on synaptic transmission and dendritic integration. Here, we developed biologically plausible models to simulate the synaptic transmission and dendritic integration of pyramidal neurons, exploring the relations between synaptic transmission and metabolic energy and between dendritic integration and metabolic energy. We find that synaptic energy not only drives synaptic vesicle cycle, but also participates in the regulation of this cycle. Release probability of synapses adapts to synaptic energy levels by regulating the speed of synaptic vesicle cycle. Besides, we also find that to match neural energy levels, only a part of the synapses receive presynaptic signals during a given period so that neurons have a low action potential frequency. That is, the number of simultaneously active synapses over a period of time should be adapted to neural energy levels

Human metabolic adaptations and prolonged expensive neurodevelopment: A review

1.	After weaning, human hunter-gatherer juveniles receive substantial (≈3.5-7 MJ day^-1^), extended (≈15 years) and reliable (kin and nonkin food pooling) energy provision.
2.	The childhood (pediatric) and the adult human brain takes a very high share of both basal metabolic rate (BMR) (child: 50-70%; adult: ≈20%) and total energy expenditure (TEE) (child: 30-50%; adult: ≈10%).
3.	The pediatric brain for an extended period (≈4-9 years-of-age) consumes roughly 50% more energy than the adult one, and after this, continues during adolescence, at a high but declining rate. Within the brain, childhood cerebral gray matter has an even higher 1.9 to 2.2-fold increased energy consumption. 
4.	This metabolic expensiveness is due to (i) the high cost of synapse activation (74% of brain energy expenditure in humans), combined with (ii), a prolonged period of exuberance in synapse numbers (up to double the number present in adults). Cognitive development during this period associates with volumetric changes in gray matter (expansion and contraction due to metabolic related size alterations in glial cells and capillary vascularization), and in white matter (expansion due to myelination). 
5.	Amongst mammals, anatomically modern humans show an unique pattern in which very slow musculoskeletal body growth is followed by a marked adolescent size/stature spurt. This pattern of growth contrasts with nonhuman primates that have a sustained fast juvenile growth with only a minor period of puberty acceleration. The existence of slow childhood growth in humans has been shown to date back to 160,000 BP. 
6.	Human children physiologically have a limited capacity to protect the brain from plasma glucose fluctuations and other metabolic disruptions. These can arise in adults, during prolonged strenuous exercise when skeletal muscle depletes plasma glucose, and produces other metabolic disruptions upon the brain (hypoxia, hyperthermia, dehydration and hyperammonemia). These are proportional to muscle mass.
7.	Children show specific adaptations to minimize such metabolic disturbances. (i) Due to slow body growth and resulting small body size, they have limited skeletal muscle mass. (ii) They show other adaptations such as an exercise specific preference for free fatty acid metabolism. (iii) While children are generally more active than adolescents and adults, they avoid physically prolonged intense exertion. 
8.	Childhood has a close relationship to high levels of energy provision and metabolic adaptations that support prolonged synaptic neurodevelopment. 
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Inhibition and Brain Work

The major part of the brain's energy budget (∼60%–80%) is devoted to its communication activities. While inhibition is critical to brain function, relatively little attention has been paid to its metabolic costs. Understanding how inhibitory interneurons contribute to brain energy consumption (brain work) is not only of interest in understanding a fundamental aspect of brain function but also in understanding functional brain imaging techniques which rely on measurements related to blood flow and metabolism. Herein we examine issues relevant to an assessment of the work performed by inhibitory interneurons in the service of brain function

Human metabolic adaptations and prolonged expensive neurodevelopment: A review

1.	After weaning, human hunter-gatherer juveniles receive substantial (≈3.5-7 MJ day^-1^), extended (≈15 years) and reliable (kin and nonkin food pooling) energy provision.
2.	The childhood (pediatric) and the adult human brain takes a very high share of both basal metabolic rate (BMR) (child: 50-70%; adult: ≈20%) and total energy expenditure (TEE) (child: 30-50%; adult: ≈10%).
3.	The pediatric brain for an extended period (≈4-9 years-of-age) consumes roughly 50% more energy than the adult one, and after this, continues during adolescence, at a high but declining rate. Within the brain, childhood cerebral gray matter has an even higher 1.9 to 2.2-fold increased energy consumption. 
4.	This metabolic expensiveness is due to (i) the high cost of synapse activation (74% of brain energy expenditure in humans), combined with (ii), a prolonged period of exuberance in synapse numbers (up to double the number present in adults). Cognitive development during this period associates with volumetric changes in gray matter (expansion and contraction due to metabolic related size alterations in glial cells and capillary vascularization), and in white matter (expansion due to myelination). 
5.	Amongst mammals, anatomically modern humans show an unique pattern in which very slow musculoskeletal body growth is followed by a marked adolescent size/stature spurt. This pattern of growth contrasts with nonhuman primates that have a sustained fast juvenile growth with only a minor period of puberty acceleration. The existence of slow childhood growth in humans has been shown to date back to 160,000 BP. 
6.	Human children physiologically have a limited capacity to protect the brain from plasma glucose fluctuations and other metabolic disruptions. These can arise in adults, during prolonged strenuous exercise when skeletal muscle depletes plasma glucose, and produces other metabolic disruptions upon the brain (hypoxia, hyperthermia, dehydration and hyperammonemia). These are proportional to muscle mass.
7.	Children show specific adaptations to minimize such metabolic disturbances. (i) Due to slow body growth and resulting small body size, they have limited skeletal muscle mass. (ii) They show other adaptations such as an exercise specific preference for free fatty acid metabolism. (iii) While children are generally more active than adolescents and adults, they avoid physically prolonged intense exertion. 
8.	Childhood has a close relationship to high levels of energy provision and metabolic adaptations that support prolonged synaptic neurodevelopment. 
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The Ghrelin Receptor Regulates Dendritic Spines and the NMDA Receptor–Mediated Synaptic Transmission in the Hippocampus

Increasing evidence suggests the involvement of ghrelin (an orexigenic hormone) and its cognate receptor growth hormone secretagogue receptor (GHSR1a, also known as the ghrelin receptor) in extra‐hypothalamic functions such as hippocampal learning and memory. However, cellular and molecular mechanisms underlying the ghrelin‐regulated hippocampal neuron activity are poorly understood. In this chapter, we show the following: (1) ghrelin promoted phosphorylation of the N‐methyl‐d‐aspartate receptor (NMDAR) subunit 1 (GluN1) in a PKC/PKA‐dependent manner and amplified NMDAR‐mediated excitatory postsynaptic currents, (2) ghrelin stimulated phosphorylation of CREB (cAMP response‐element‐binding protein), and (3) ghrelin increased phalloidin binding to F‐actin, suggesting possible reorganization of dendritic spines; all occurred through the activation of GHSR1a in the CA1 pyramidal cell of the hippocampus in cultured slice preparations. Interestingly, the ghrelin’s effects on GluN1 and CREB phosphorylation were negatively modulated by exogenous application of endocannabinoids, 2‐arachidonoylglycerol (2‐AG), and anandamide (ANE), in type 1 cannabinoid receptor (CB1R)‐dependent and ‐independent manners, respectively. It is suggested that ghrelin and the ghrelin receptor regulate synaptic transmission and plasticity in the hippocampus, interacting with the endogenous cannabinoid system, which may be essential and necessary for successful acquisition of metabolic state–dependent learning and adaptive appetitive behavior

Influence of the dentritic morphology on electrophysiological responses of thalamocortical neurons

Les neurones thalamiques de relai ont un rôle exclusif dans la transformation et de transfert de presque toute l'information sensorielle dans le cortex. L'intégration synaptique et la réponse électrophysiologique des neurones thalamiques de relai sont déterminées non seulement par l’état du réseau impliqué, mais ils sont également contrôlés par leurs propriétés intrinsèques tels les divers canaux ioniques voltage-dépendants ainsi que l’arborisation dendritique élaboré. Par conséquent, investiguer sur le profil complexe de morphologie dendritique et sur les propriétés dendritiques actives révèle des renseignements importants sur la fonction d'entrée-sortie de neurones thalamiques de relai. Dans cette étude, nous avons reconstruit huit neurones thalamocorticaux (TC) du noyau VPL de chat adulte. En se basant sur ces données morphologiques complètes, nous avons développé plusieurs modèles multicompartimentaux afin de trouver un rôle potentiellement important des arbres dendritiques des neurones de TC dans l'intégration synaptique et l’intégration neuronale. L'analyse des caractéristiques morphologiques des neurones TC accordent des valeurs précises à des paramètres géométriques semblables ou différents de ceux publiés antérieurement. En outre, cette analyse fait ressortir de tous nouveaux renseignements concernant le patron de connectivité entre les sections dendritiques telles que l'index de l'asymétrie et la longueur de parcours moyen (c'est-à-dire, les paramètres topologiques). Nous avons confirmé l’étendue des valeurs rapportée antérieurement pour plusieurs paramètres géométriques tels que la zone somatique (2956.24±918.89 m2), la longueur dendritique totale (168017.49±4364.64 m) et le nombre de sous-arbres (8.3±1.5) pour huit neurones TC. Cependant, contrairement aux données rapportées antérieurement, le patron de ramification dendritique (avec des cas de bifurcation 98 %) ne suit pas la règle de puissance de Rall 3/2 pour le ratio géométrique (GR), et la valeur moyenne de GR pour un signal de propagation est 2,5 fois plus grande que pour un signal rétropropagé. Nous avons également démontré une variabilité significative dans l'index de symétrie entre les sous-arbres de neurones TC, mais la longueur du parcours moyen n'a pas montré une grande variation à travers les ramifications dendritiques des différents neurones. Nous avons examiné la conséquence d’une distribution non-uniforme des canaux T le long de l'arbre dendritique sur la réponse électrophysiologique émergeante, soit le potentiel Ca 2+ à seuil bas (low-threshold calcium spike, LTS) des neurones TC. En appliquant l'hypothèse du «coût minimal métabolique», nous avons constaté que le neurone modélisé nécessite un nombre minimal de canaux-T pour générer un LTS, lorsque les canaux-T sont situés dans les dendrites proximales. Dans la prochaine étude, notre modèle informatique a illustré l'étendue d'une rétropropagation du potentiel d'action et de l'efficacité de la propagation vers des PPSEs générés aux branches dendritiques distales. Nous avons démontré que la propagation dendritique des signaux électriques est fortement contrôlée par les paramètres morphologiques comme illustré par les différents paliers de polarisation obtenus par un neurone à équidistance de soma pendant la propagation et la rétropropagation des signaux électriques. Nos résultats ont révélé que les propriétés géométriques (c.-à-d. diamètre, GR) ont un impact plus fort sur la propagation du signal électrique que les propriétés topologiques. Nous concluons que (1) la diversité dans les propriétés morphologiques entre les sous-arbres d'un seul neurone TC donne une capacité spécifique pour l'intégration synaptique et l’intégration neuronale des différents dendrites, (2) le paramètre géométrique d'un arbre dendritique fournissent une influence plus élevée sur le contrôle de l'efficacité synaptique et l'étendue du potentiel d'action rétropropagé que les propriétés topologiques, (3) neurones TC suivent le principe d’optimisation pour la distribution de la conductance voltage-dépendant sur les arbres dendritiques.Thalamic relay neurons have an exclusive role in processing and transferring nearly all sensory information into the cortex. The synaptic integration and the electrophysiological response of thalamic relay neurons are determined not only by a state of the involved network, but they are also controlled by their intrinsic properties; such as diverse voltage-dependent ionic channels as well as by elaborated dendritic arborization. Therefore, investigating the complex pattern of dendritic morphology and dendritic active properties reveals important information on the input-output function of thalamic relay neurons. In this study, we reconstructed eight thalamocortical (TC) neurons from the VPL nucleus of adult cats. Based on these complete morphological data, we developed several multi-compartment models in order to find a potentially important role for dendritic trees of TC neurons in the synaptic integration and neuronal computation. The analysis of morphological features of TC neurons yield precise values of geometrical parameters either similar or different from those previously reported. In addition, this analysis extracted new information regarding the pattern of connectivity between dendritic sections such as asymmetry index and mean path length (i.e., topological parameters). We confirmed the same range of previously reported value for several geometric parameters such as the somatic area (2956.24±918.89 m2), the total dendritic length (168017.49±4364.64 m) and the number of subtrees (8.3±1.5) for eight TC neurons. However, contrary to previously reported data, the dendritic branching pattern (with 98% bifurcation cases) does not follow Rall’s 3/2 power rule for the geometrical ratio (GR), and the average GR value for a forward propagation signal was 2.5 times bigger than for a backward propagating signal. We also demonstrated a significant variability in the symmetry index between subtrees of TC neurons, but the mean path length did not show a large variation through the dendritic arborizations of different neurons. We examined the consequence of non-uniform distribution of T-channels along the dendritic tree on the prominent electrophysiological response, the low-threshold Ca2+ spike (LTS) of TC neurons. By applying the hypothesis of “minimizing metabolic cost”, we found that the modeled neuron needed a minimum number of T-channels to generate low-threshold Ca2+ spike (LTS), when T-channels were located in proximal dendrites. In the next study, our computational model illustrated the extent of an action potential back propagation and the efficacy of forward propagation of EPSPs arriving at the distal dendritic branches. We demonstrated that dendritic propagation of electrical signals is strongly controlled by morphological parameters as shown by different levels of polarization achieved by a neuron at equidistance from the soma during back and forward propagation of electrical signals. Our results revealed that geometrical properties (i.e. diameter, GR) have a stronger impact on the electrical signal propagation than topological properties. We conclude that (1) diversity in the morphological properties between subtrees of a single TC neuron lead to a specific ability for synaptic integration and neuronal computation of different dendrites, (2) geometrical parameter of a dendritic tree provide higher influence on the control of synaptic efficacy and the extent of the back propagating action potential than topological properties, (3) TC neurons follow the optimized principle for distribution of voltage-dependent conductance on dendritic trees

Miro1-dependent Mitochondrial Dynamics in Parvalbumin Interneurons

Parvalbumin interneurons are fast-spiking inhibitory cells that have been implicated in the generation of rhythmic network activity in the γ-frequency band (30-80Hz) by coordinating principal cell activity. In order to sustain their high firing rates, parvalbumin interneurons have a high mitochondrial content reflecting their large energy utilization. Therefore, parvalbumin interneurons are more susceptible to incidents of mitochondrial impairment as mitochondria provide the predominant source of energy. Miro1 is a Ca²⁺-sensing adaptor protein that links mitochondria to the trafficking apparatus, for their microtubule-dependent transport along axons and dendrites, in order to meet the metabolic needs of the cell. Here, we explore the role of Miro1 in parvalbumin interneurons and how changes in the mitochondrial distribution could alter network activity. To investigate mitochondrial dynamics we generated a mouse line where mitochondria are specifically labelled in parvalbumin interneurons. The Cre- recombinase is expressed exclusively in parvalbumin interneurons and excises a termination signal upstream of a fluorescent reporter allowing for the visualisation of mitochondria only in these cells. We further crossed this line with the Miro1(f/f) mouse, generating a transgenic mouse where Miro1 was conditionally knocked-out exclusively in parvalbumin interneurons. Specifically we investigated the conditional removal of Miro1 in mitochondrial dynamics in parvalbumin interneurons. Using live-imaging of ex-vivo organotypic brain cultures, we demonstrated a reduction in mitochondrial trafficking in parvalbumin interneurons in the hippocampus under basal conditions. This lead to accumulation of mitochondria in the soma and their depletion from synaptic terminals. Loss of Miro1 resulted in alterations in axonal but not dendritic branching in parvalbumin interneurons. This was accompanied by altered synaptic transmission and increased frequency of γ-oscillations in hippocampal brain slices. In this study, we show for the first time that Miro1 and Miro1-dependent mitochondrial positioning are essential for correct parvalbumin interneuron function and network activity

Uncertainty and stress: Why it causes diseases and how it is mastered by the brain

The term 'stress' - coined in 1936 - has many definitions, but until now has lacked a theoretical foundation. Here we present an information-theoretic approach - based on the 'free energy principle' - defining the essence of stress; namely, uncertainty. We address three questions: What is uncertainty? What does it do to us? What are our resources to master it? Mathematically speaking, uncertainty is entropy or 'expected surprise'. The 'free energy principle' rests upon the fact that self-organizing biological agents resist a tendency to disorder and must therefore minimize the entropy of their sensory states. Applied to our everyday life, this means that we feel uncertain, when we anticipate that outcomes will turn out to be something other than expected - and that we are unable to avoid surprise. As all cognitive systems strive to reduce their uncertainty about future outcomes, they face a critical constraint: Reducing uncertainty requires cerebral energy. The characteristic of the vertebrate brain to prioritize its own high energy is captured by the notion of the 'selfish brain'. Accordingly, in times of uncertainty, the selfish brain demands extra energy from the body. If, despite all this, the brain cannot reduce uncertainty, a persistent cerebral energy crisis may develop, burdening the individual by 'allostatic load' that contributes to systemic and brain malfunction (impaired memory, atherogenesis, diabetes and subsequent cardio- and cerebrovascular events). Based on the basic tenet that stress originates from uncertainty, we discuss the strategies our brain uses to avoid surprise and thereby resolve uncertainty