1. Introduction

The hypothalamus is a regulator center involved in the integration of multiple factors and in the regulation of numerous homeostatic functions. Among them, the control of energy balance is one of the most complex hypothalamic tasks, as it also requires the coordinated participation of other brain regions and substances secreted by peripheral organs, such as the gastrointestinal tract or the adrenal glands. These peripheric signals send information to the central nervous system about the state of the energy stores, affecting the energy intake and expenditure [1,2,3]. For example, it was reported that gastric distension has a satiating effect [3]. In the control of food intake, a short-term regulation determines the beginning and the end of a meal; a long-term regulation helps to regulate the energy depots, and satiety regulates the interval between meals [3]. The balance between food intake and energy expenditure determines long-term energy homeostasis [1].

The regulation of feeding behavior is a complex mechanism exerted mainly by neuropeptides and neurotransmitters at the hypothalamic level, and the activity of certain hypothalamic neuronal groups sets the balance for maintaining proper homeostasis. In this regard, the activity of neurons located in the arcuate nucleus is particularly important. A group of neurons in this nucleus contain neuropeptide Y (NPY) and agouti-related peptide (AgRP) and are orexigenic, i.e., they promote food intake. These neurons are inhibitory for another population of neurons located in the arcuate nucleus that contain pro-opiomelanocortin (POMC) and cocaine- and amphetamine-regulated transcript (CART), are anorexigenic, and inhibit feeding; see [4,5] for review. The interaction of both systems, POMC/CART and NPY/AgRP, is the basis for the regulation of energy homeostasis. These neuronal groups are under the influence of substances produced by the gastrointestinal tract, such as ghrelin, which activates NPY/AgRP neurons, and insulin or leptin, which activate POMC/CART neurons and inhibit NPY/AgRP neurons [1] (Figure 1).

In addition, other hypothalamic regions and neuropeptides exert different effects on these neuronal groups [2] (Figure 2).

In this regard, it was reported that orexins A and B, synthesized by neurons of the lateral hypothalamus, activate NPY/AgRP neurons located in the hypothalamic arcuate nucleus and that this projection is reciprocal [3,5]. Simultaneously, orexins inhibit POMC/CART neurons [1]. The orexigenic effects of orexins are mainly mediated by NPY/AgRP neurons of the arcuate nucleus [2]. Orexins stimulate food intake and NPY expression (but not AgRP) in the arcuate nucleus when administered centrally, and their production is influenced by the nutritional state of the animal and respond to feeding status [1,2,6]; thus, the hypothalamic expression of the orexin precursor is increased during fasting [2,7,8]. Orexinergic neurons perceive rapidly the body’s nutritional status and respond to metabolic signals, such as leptin and ghrelin levels or peripheral blood glucose, since orexin neurons are glucose-sensitive neurons excited by reduced blood glucose levels. Thus, orexin neurons can translate energy status into neural signals [1]; acting on this hypothalamic circuit, they can exert homeostatic regulation [8,9,10]. In addition, due to their extensive extrahypothalamic projections mainly to the limbic system, forebrain, and midbrain, orexins are involved in the regulation of complex behaviors that regulate food consumption, including motivation [7,8,11]. The participation of orexins in the stimulation of excessive intake of palatable sweet and fatty foods suggests that these peptides could also promote non-homeostatic dysregulated food intake [8,9,11].

It was suggested that the primary role of orexins is to promote foraging behavior, with a minimal role in the reinstatement of seeking for food that may be no longer available. In fact, during food deprivation, elevated levels of orexins are detected as well as progressively shorter episodes of sleep and increased locomotor activity as a part of survival strategy [7,8,12]. Thus, orexins participate in the regulation of numerous functions [10,13], being the control of food intake and associated behaviors especially relevant within this wide range of activities. Therefore, the aim of this review is to evaluate the role of orexins in this complex mechanism.

2. Orexins

Orexins A (hypocretin 1: 33 amino acids) and B (hypocretin 2: 28 amino acids) are excitatory neuropeptides (C-terminally amidated and showing 46% homology), produced in the lateral hypothalamus/perifornical region and are involved in energy homeostasis, feeding (promote food intake: orexin A has a higher action than orexin B), reward-related appetitive behaviors (mesolimbic pathway), glucose metabolism, motor function, sleep, and wakefulness (during sleep orexin neurons are silent) [14,15,16,17] (Table 1).

Orexin A increases food intake, especially diets that are rich in saturated fat [34] (Table 1), whereas orexin B is less stable and lipophilic than orexin A, which is consistently observed in the cerebrospinal fluid of healthy human individuals [15]. It is known that the orexinergic system stimulates the hypothalamus–pituitary–adrenal axis and that this system regulates intestinal motility and insulin secretion [14] (Table 1). Orexin was also observed in the enteric nervous system and endocrine cells in the gut [20] and it is known that orexin A decreases tumor development [21], exerts an excitatory effect on hippocampal neurons through the orexin 1 receptor [22], and is involved in immunomodulatory mechanisms (e.g., by decreasing the level of pro-inflammatory cytokines) [20] (Table 1). It was reported that orexin deficiency regulates cognitive flexibility (ability to adapt behaviors in response to environment changes) in a sex-dependent manner; this means that the peptide plays an important sexually dimorphic role [24] (Table 1). Orexin is involved in the integration of metabolism and sleep: a recent review focused on this topic [19]. It is also known that animals carrying null mutations of the transcription factor named early B-cell factor 2 showed a decrease in the expression of orexin [40]. Recently, the orexinergic system was reviewed in mammalian and non-mammalian species, and it there were reported orexin diurnal variations in the brain of mammals [15] (Table 1).

The lateral hypothalamus regulates metabolism/food intake and integrates hedonic/homeostatic circuits [41]. In the human lateral hypothalamus, cell bodies (50,000–80,000) containing orexin display fusiform/multipolar morphology (20–30 µm in diameter) and show 2–4 dendrites [29]. The hypothalamic distribution of orexin neurons was widely reported in mammals (rat, mouse, hamster, cat, sheep, pig, monkey, and humans) as well as in chicken, amphibians and zebrafish [15,29,42]. Neurons containing orexin show heterogeneity in neuronal connectivity and gene expression; this means that mammalian hypothalamic orexin-producing neurons can be segregated into anatomically, genetically, and functionally distinct subpopulations, which are involved in the diverse actions played by these neurons (e.g., reward, stress, emotions, feeding, sleep, and arousal) [25] (Table 1). In this sense, neurochemical heterogeneity (e.g., glutamate, GABA, pro-dynorphin, neuronal activity-regulated pentraxin II, and insulin-like growth factor-binding protein 3) were demonstrated in the hypothalamic neurons expressing orexin [25,26]. These neurons also contain the protein delta-like homolog 1 and coexpress several receptors, such as mu opioid, 5-hydroxytryptamine (HT)_1A, adenosine A1, leptin, gamma-aminobutyric acid (GABA)_A, pancreatic polypeptide Y4 and cholecystokinin A [25,29,43]. To know in-depth this neurochemical diversity is crucial to understand how different neuronal populations are involved in the regulation and coordination of diverse physiological actions (e.g., feeding, and sleep).

In the lateral hypothalamus, neurons expressing orexin receive inputs from arcuate neurons containing NPY/AgRP [27], whereas orexinergic neurons send inputs to ventral tegmental neurons expressing orexin 1 and 2 receptors, and hence orexin activates the mesolimbic pathway [13,28] (Table 1). Moreover, orexinergic lateral hypothalamic neurons send projections to the paraventricular thalamic nucleus, activating the thalamocortical-projecting neurons located in the latter nucleus (Table 1, Figure 2). Thus, the neuroanatomical connections suggest that orexin regulates attention/arousal to promote reward-related behaviors. In this sense, it is known that orexin controls the rewarding aspect of male sexual reward [44]. Moreover, cell bodies containing orexin project to the posterior hypothalamus (involved in hormone secretion and feeding behavior), medial thalamus, ventral forebrain, amygdala, neocortex, periaqueductal gray matter, locus coeruleus, dorsal raphe, raphe magnus, ventrolateral medulla, spinal cord and brain regions involved in sleep–wake and respiratory/cardiovascular regulation [29] (Table 1, Figure 2).

Thus, orexigenic peptides regulate food intake targeting hypothalamic and extrahypothalamic (e.g., mesolimbic reward circuitry) regions, increasing the complexity to well understand the mechanisms involved in feeding behavior [30]. Orexins or their receptors, in addition to the central nervous system, are located in numerous peripheral tissues, including adipocytes, thyroid, reproductive tract, pancreas, parathyroid, adrenal gland, testis, ovary, pituitary and intestines [14] (Table 1).

2.1. Orexin Precursor

In mammals (e.g., rat, dog, pig, human), orexins are derived from the precursor named prepro-orexin (130–131 amino acids); in humans, the prepro-orexin gene is encoded on chromosome 17q21-q24 and show two exons and one intron distributed over 1432 bp [14,29] (Table 1). It is suggested that the gene arose early in the chordate lineage and that it originated from the secretin gene through three genetic rearrangements [45]. Prepro-orexin (130 residues) contains a signal sequence and two well-conserved places for proteolytic maturation followed by a modification of the carboxy-terminal glycines mediated by the peptidylglycine alpha-amidating monooxygenase [46]. At present, the enzymes that cleave the prepro-orexin to originate orexins A and B are unknown, although it is suggested that the prohormone convertase 1 could be involved in the processing of the precursor [29]. Orexins A and B show two adjacent alpha-helices (9–14 and 6–7 amino acids long) separated by a short 2–3 amino acids turn; the longer helix is the identity region for both peptides [18] (Table 1). The 19 residues of the C-terminal region of both orexins share 13 identical amino acids [29]. During fasting, an upregulation in the prepro-orexin mRNA expression was reported [6] (Table 1). Finally, it is known that the promoter region of the prepro-orexin gene has two early B-cell factor 2 binding sites, named olf-1 sites, that a deletion of the olf1-site proximal to the transcription start site of the gene increases the expression of the prepro-orexin gene, and that a deletion of the distal olf1-like site decreases its expression [40].

2.2. Orexin Receptor

Two orexin receptors highly conserved across species are described: orexin 1 and orexin 2. Rat and human orexin 1 and 2 receptors show, respectively, 94% and 95% homology. Orexin B shows a higher affinity for orexin receptor 2 than for orexin receptor 1, whereas orexin A shows equal affinity for both receptors [30] (Table 1). Both orexin receptors are G protein-coupled receptors (Table 1): orexin 1 receptor is abundant in the spinal cord, laterodorsal tegmentum, locus coeruleus, dorsal raphe, hypothalamus (ventromedial region), paraventricular thalamic nucleus, hippocampus (CA2 region) and prefrontal cortex, whereas the orexin 2 receptor is prominent in the neocortex, central amygdala, hippocampus (CA3 region), septum, thalamus, and hypothalamus (dorsomedial region) [29]. The orexin receptor can form homodimers, heterodimers or oligomers and it was reported that orexin A increased the dimerization/oligomerization, whereas antagonists decreased both processes [31] (Table 1). For example, orexin 1 and corticotropin-releasing factor receptor dimerization and orexin 1 receptor and kappa opioid receptor heteromerization were reported [31]. In general, the distribution of orexin receptors and fibers containing the peptide was similar, and it is known that the distribution of the orexin receptors was similar to that observed for the melanin-concentrating hormone receptor [29,32] (Table 1). Orexinergic terminals show two bouton types: large (ovoid, diameter: > 1.4 µm) or small (spherical, <1.4 µm) [15].

It is known that animals without the orexin 2 receptor had slow cessations of movements (sleep attacks), whereas those lacking the orexin 1 receptor showed disrupted sleep but fewer signs of sleep attacks [47]. In the medulla oblongata, it was reported that chronic aldosterone exposure and salt intake did not change the expression of both orexin 1 and 2 receptors; however, in the hypothalamus, the expression of the latter receptor was increased [48]. It is also known that orexin 1 and 2 receptors are involved in the control of body weight and energy metabolism [14]. During the estrus cycle, it was reported that the expression of orexin receptors was increased exclusively during proestrus and that the administration of orexin receptor antagonists blocked ovulation as well as the effects mediated by the follicle-stimulating and luteinizing hormones [49]. The administration of orexin 1 receptor antagonists inhibited behavioral satiety and hyperphagia mediated by orexin B [33], and the inhibition of the orexin A signaling decreased overfeeding from a high fat diet under the condition of satiation. This means that orexin A regulates unconditioned reward-based high fat feeding, and that the peptide is involved in the modulation of cognitive–emotional mechanisms [34] (Table 1). Recently, a subtype-selective orexin 1 receptor antagonist was developed, showing the potential of structure-based drug designs to obtain new selective ligands for the orexin receptors [50] and it was reported that the neural depolarization mediated by orexin A depended on non-selective cation channels [51]. It was demonstrated that an enhanced orexin 2 receptor signaling improved leptin sensitivity and prevented diet-induced obesity [35] (Table 1).

It is known that dynein light chain Tctex-type 1 and beta-arrestin are coupled to the C-terminus of the orexin receptor and it seems that the extracellular portion of the receptor contributes to the binding of the peptide [31,52,53,54]. The signaling pathways activated by the orexinergic system remains obscure, although it is known that proteins Gq, Gs and Gi are activated and that an increase in the level of Ca²⁺ occurs [36] (Table 1). Orexin 1 receptor activates adenylyl cyclase via a high potency phospholipase C/protein kinase C coupling and a low potency Gs coupling [38] (Table 1). In fact, the response of orexin was blocked when inhibitors of phospholipase C or protein kinase C were used [55]. The orexin 1 receptor is also coupled to diacylglycerol lipase (DAGL) and phospholipase A2 leading to the production of 2-arachidonoyl glycerol [37] (Table 1). Orexin A increased the levels of both cAMP (cyclic adenosine monophosphate) and IP3 (inositol triphosphate) and the labeling of Gi/Gs/Gq but not Go [39] (Table 1). Orexin B also increased the level of cAMP and it was reported that food deprivation exerted a differential effect regarding the coupling that occurred between different G proteins and orexin receptors [14]. The action mediated by orexin was sensitive to inhibitors of protein kinase A mediating the cAMP effect [29]. The activation of both receptors activated the mitogen-activated protein kinase (MAPK) pathway, promoting p38 kinase and extracellular signal-regulated protein kinases (ERK) 1 and 2 phosphorylation [31] (Table 1).

2.3. Physiological Actions Mediated by Orexins

The administration of orexin increases food intake and wakefulness, regulates locomotor activity, hormone secretion, emotional states (anxiety, panic), cognition and blood pressure and suppresses rapid eye movement sleep [15,29] (Table 2).

Orexins are involved in endocrine (controlling the release of luteinizing hormone, and corticotropin-releasing hormone), autonomic (blood pressure, body temperature, heart rate, and breathing) and pain (decrease) actions [29]. In addition, orexin is involved in placental development and growth [15] and in the release of glucocorticoids [31]. Orexins regulate the brain reward function, and it seems that this is mediated by opioids involved in motivational mechanisms [29]. Narcolepsy occurs when the orexin 2 receptor gene is inactivated; in humans, individuals suffering from narcolepsy show a decrease in the level of orexin in the cerebrospinal fluid, and no or a few orexinergic neurons are observed in the hypothalamus [29] (Table 2).

In the adipose tissue, both orexins A and B increased PPAR (peroxisome proliferator-activated receptor)-gamma-2 expression, which is involved in adipose differentiation and decreased the expression of the hormone-sensitive lipase enzyme [56] (Table 2). In addition, orexin A decreased the release of glycerol, suggesting that the peptide regulates fat metabolism by inhibiting lipolysis [56] (Table 2). It is also important to note that orexins A and B promoted and inhibited, respectively, the proliferation of 3T3-L1 cells, which show an adipocyte-like phenotype [14] (Table 2). It was reported that the distribution of orexins in the central nervous system of obese animals lacking the leptin receptor was more widespread than that observed in lean animals [58] (Table 2). This is due to the lack of leptin receptors since leptin negatively regulates the expression of orexin and hence, the orexin tone is augmented in obese individuals [66]. It is also known that a fat diet and triglycerides stimulate orexin tone [57] (Table 2).

It was reported that orexins increase the motility of the gastrointestinal tract, that are involved in glucose metabolism, and that in neurons expressing orexin, fasting increased the level of pCREB (phosphorylated cAMP response binding protein) [59,60] (Table 2). It is also known that orexin A promoted the acid secretion and decreased the rate of gastric emptying and plasma leptin level [14] (Table 2). It was demonstrated that the neuroendocrine regulatory peptide-2 regulated both gastric emptying and secretion and that these mechanisms were mediated by the orexin system [67].

Orexin A increased the plasma level of adrenocorticotropic hormone and corticosterone, but this effect was not observed with orexin B [61] (Table 2). Both orexins increased the plasma level of norepinephrine, suggesting that the peptides stimulated the adrenal medulla [14] (Table 2). Orexin A increased the release of cortisol and mRNA levels of CYP11B1/B2, CYP21 and HSD3B2 (steroidogenic enzymes), but the levels of other enzymes, such as CYP11A and CYP17, were not affected [62] (Table 2). Protein kinase C and ERK 1/2 (extracellular signal-regulated protein kinases 1 and 2) are also involved in these mechanisms mediated by orexin A. This orexin also decreases the level of circulating TSH (thyroid-stimulating hormone), although several studies have shown that orexin A does not exert a significant action on the thyroid–pituitary axis [14]. In avian liver, it was reported that hepatocytes express/secrete orexin and that orexin A regulates hepatic lipogenesis via activation of the ERK1/2 signaling pathway [68].

In humans, orexin A is colocalized with insulin in the pancreatic islets, and the release of orexin A is dependent on a low glucose level; this means that the peptide regulates the secretion of the pancreatic hormones and glucose modulation [60] (Table 2). Orexin plays an important role in the maintenance of normal insulin sensitivity with advanced age, and the data show that the peptide is crucial in maintaining the hypothalamic insulin signaling that is responsible for the prevention of the onset of peripheral insulin resistance, which tends to increase with age [63] (Table 2). This could explain why diabetes (type 2) incidence is augmented in normal weight individuals showing a deficiency in orexin. Hyperglycemia blocks the expression of orexin, and it was reported that the circadian clock of the suprachiasmatic nucleus could be reset through arousal promoting signals from neurons containing orexin [60] (Table 2). In hypoglycemic animals, the hypothalamic level of orexin B was higher than in control animals [64] (Table 2).

Orexins A and B increase food consumption and, in fasting animals, the level of prepro-orexin also increased in the hypothalamus [6] (Table 2). The administration of orexin A into the perifornical area or lateral hypothalamus increased food intake. It is known that neurons containing orexin are sensitive to the levels of triglyceride, leptin, and glucose [29] (Table 2). It is important to note that a long-term administration of orexin A did not modify daily food intake, the level of glucose in blood, and body weight, suggesting that the actions of orexin A could be limited to the short-term, due to increased wakefulness [29] (Table 2). In this sense, orexin knockout animals showed very modest differences in food intake, and animals depleted of neurons expressing orexin showed obesity and hypolocomotion [69,70]. However, other studies showed contradictory results since the genetic ablation of the lateral hypothalamic neurons containing orexin led to hyperphagia and obesity; this means that orexin is a key regulator to maintain a stable energy homeostasis [69]. These and other data suggest that the food effects mediated by orexins result from arousal rather than from a direct feeding pressure [29].

Orexins A and B increase energy expenditure. It was reported that orexin A increased more the metabolic rate than orexin B, and that the stimulation of the metabolic rate by orexin A was lower during the light cycle than during the dark ones [65] (Table 2). Moreover, the administration of orexin A into the paraventricular hypothalamic nucleus increased energy expenditure and physical activity [65]. Orexin A controls the operant that responds to palatable food rewards [71], and it is known that the action of orexin in the mesolimbic system is needed for an opioid-induced high-fat diet [72]. There are data suggesting that orexin A modulates emotional/cognitive processes (e.g., motivation to obtain food) and it was reported that expectation for food reward (both palatable (chocolate) and general (chow)) activated lateral hypothalamic neurons containing orexin and other brain regions involved in feeding control [34] (Table 2). Finally, it is known that orexin A is involved in compulsive behaviors indicating that the orexin 1 receptor is implicated in obsessive-compulsive disorders [73] (Table 2).

3. Orexins and Food Intake in Experimental Animal Models

3.1. Rat

In male and female rats, the administration of genistein (a phytoestrogen) from postnatal days 6 to 13 was studied regarding the expression of orexin in the hypothalamus (lateral, dorsomedial, and perifornical areas) [74]. No alteration in orexin expression was observed, and hence it seems that genistein does not regulate such expression in both sexes. However, sex differences in the demand for highly palatable food (higher in females than in males) were demonstrated; it seems that these differences are related with sexual dimorphism in the actions exerted by the orexinergic system [75] (Table 3).

In the central nucleus of the amygdala, the administration of orexin A increases gastric motility and palatable food intake; in addition, the lateral hypothalamus, nucleus accumbens and ventral tegmental area are also involved in the intake [81] (Table 3). It was reported that orexin, in the posterior paraventricular thalamus (which receives a strong orexinergic innervation), regulates hunger-related signals in the nucleus accumbens core [82] and that the peptide increases the release of dopamine in the nucleus accumbens shell by sucrose feeding [83] (Table 3). It is known that a palatable high-fat diet promotes time-dependent synaptic plasticity in the neurons expressing orexin or melanin-concentrating hormone located in the lateral hypothalamus [76] (Table 3). After the administration of this diet, orexin neurons show a transient increase in spontaneous excitatory transmission, which return to control levels with prolonged feeding, whereas melanin-concentrating hormone neurons show a delayed increase in excitatory synaptic transmission, which progressively increase as the palatable high-fat diet becomes chronic [76]. It seems that the changes observed in the synaptic properties of these neurons are due to the number of active synaptic contacts/altered postsynaptic sensitivity depending on feeding duration and cell type [76]. However, this diet does not induce changes in the inhibitory transmission in both nerve cell types at any time point [76]. The results suggest that the actions of a palatable high-fat diet on feeding-related nerve cells are dynamic and specific for each type of neuron. However, it was also demonstrated that orexinergic neurons (orexin A) shows an endocannabinoid-mediated disinhibition due to an increase in the inhibitory cannabinoid receptor type 1 positive puncta versus the excitatory ones [96]. In obese animals, the activation of the cannabinoid receptor type 1 decreases the inhibition of the orexinergic neurons and hence increases the release of orexin A, promoting hyperphagia and body weight [96]. The latter study showed that obesity-driven synaptic remodeling affects the endocannabinoid control of neurons containing orexin [96]. It was also reported that a perinatal maternal high-fat diet increases the hypothalamic projections (e.g., from the ventromedial hypothalamus) to the lateral hypothalamus containing neurons expressing orexin A as well as the basal activation of these neurons [41] (Table 3). A responsiveness of lateral hypothalamic neurons to leptin was also observed [41]. Because nerve cells located in the lateral hypothalamus send projections to dopaminergic neurons located in the ventral tegmental area, it seems that these hypothalamic nerve cells are involved in early dietary programming of the mesocorticolimbic reward circuits.

In rats, it was reported that the intestinal electrical stimulation modifies the hypothalamic expression of orexin in the lateral hypothalamus and ameliorates diet-induced obesity [77] (Table 3). Electrical stimulation decreases food intake, body weight and the expression of orexin and improves insulin sensitivity and glucose tolerance. Lateral hypothalamic neurons expressing orexin send projections to the medial prefrontal cortex, and it was demonstrated that for a cue-potentiated feeding, it is necessary the activation of the orexin 1 receptors located in the medial prefrontal cortex, the connectivity of the latter region with the lateral hypothalamus and the development of the medial prefrontal cortex neural plasticity [97]. The data show the involvement of the medial prefrontal cortex in the cognitive motivation to eat, suggesting that this cortical region is a potential target for the treatment of excessive appetite/overeating. It was reported that the administration of orexin A into the hindbrain increased both meal size and feeding; these effects were inhibited with the orexin 1 receptor antagonist SB-334,867; and hypothalamic neurons containing orexin send projections to hindbrain centers (e.g., area postrema, and nucleus of the solitary tract) in which the expression of the orexin 1 receptor was reported [87]. The study showed that, via the hindbrain orexin 1 receptors, hypothalamic neurons expressing orexin decrease the sensitivity to gastrointestinal nutrient load and hence, more food is consumed [87] (Table 3).

In female rats, it was reported that a cafeteria diet promoted changes in the hypothalamic mechanisms involved in food consumption at different periods (short-, medium- and long-term) [78]. A short-term period (4 weeks of cafeteria diet) did not affect the expression of orexin in the hypothalamus; a medium-term period (11 weeks) increased the expression of orexin and body weight, and a long-term period (20 weeks) increased more such expression [78]. The alteration in mRNA orexin level was associated to epigenetic modifications in the promoter region. Thus, the data indicate that during the development of obesity, the expression of orexin varies, and hence the alterations observed show the differential roles played by orexin in food consumption at different feeding periods (Table 3). Moreover, the administration of sea buckthorn seed oil was studied regarding the cisplatin-induced vomiting and the role played by orexin A [88]. The plasma level of orexin A and mRNA/protein expressions of the orexin 1 receptor were measured in the brainstem/hypothalamus as well as the expression of orexin A in the lateral hypothalamus. In all cases, the administration of sea buckthorn seed oil increased significantly all the parameters studied and prevented cisplatin-induced vomiting. Thus, it seems that this prevention was mediated by an increase in the central and peripheral levels of orexin A and in the expression of the orexin 1 receptor in both the hypothalamus and brainstem [88] (Table 3). A high-fat diet activates neurons expressing orexin, which in turn, increases the consumption of a high-fat diet by activating the mesolimbic reward pathway [79] (Table 3). It was reported that under a palatable high-fat Western diet (short-term), excitatory synapses to orexin neurons became amenable to long-term depression after one week of high-fat diet feeding; the effect was reversed after four weeks of a high-fat diet [79]. It seems that this mechanism is a homeostatic response that occurs to prevent the overactivation of such neurons and to decrease high-fat diet consumption and obesity. The long-term depression depends on the retrograde endocannabinoid signaling and on the postsynaptic metabotropic glutamate receptor 5 [79]. In free-feeding animals, it was demonstrated that the administration into the median raphe nucleus of prazosin (α1-adrenoceptor antagonist) increased food intake and the expression of fos in the lateral hypothalamic neurons containing orexin [91]. It was also demonstrated that the latter neurons are targeted by axons arising from cell bodies located in the median raphe nucleus [91]. The findings suggest that prazosin, through the orexinergic system, promotes a motivational response regarding food consumption (Table 3).

It was reported that a chronic intake of fructose increases the level of orexin A in the hypothalamus and ventral tegmental area [84] (Table 3). This means that hypothalamic orexinergic neurons are activated by this consumption. It is known that melatonin decreased adiposity, body weight and food intake [93]. In pinealectomized animals, it was found that the hypothalamic expression of orexin was increased, but when these animals were treated with melatonin, such expression was reduced [93] (Table 3). In bilateral nephrectomized rats, food intake decreased significantly, and it was reported that hypothalamic mRNA level of orexin was lower in bilateral nephrectomized rats than in sham-operated animals [95]. This finding suggests that orexin could be involved in the development of anorexia in bilateral nephrectomized rats (Table 3). In rats suffering from type 2 diabetes, glucose regulation was improved after a chronic treatment with orexin A [94]. In addition, the peptide attenuated the loss of pancreatic β-cells by apoptotic mechanisms, increased insulin sensitivity and decreased plasma tumor necrosis factor-α and non-esterified fatty acid levels [94]. In sum, orexin A improved glucose control by protecting beta-cells from apoptosis and by increasing the sensitivity to insulin (Table 3).

During the rest phase, it was reported that feeding decreased the activation of the hypothalamic lateral neuron expressing orexin in the light [85] (Table 3). It is known that aging is related to homeostatic changes (e.g., food innate) and to a dysregulation/loss of the orexinergic system [90]. Aged rats had slower feeding latencies, and this was ameliorated when the orexin expression was upregulated [90]. In the insular cortex of aged rats, this upregulation did not restore deficits in feeding-elicited release of neurotransmitters (e.g., GABA, glutamate, and acetylcholine) but enhanced basal neurotransmitter levels. This means that the orexinergic system mediates age-related deficits in the behavioral/neurochemical mechanisms of feeding and that an increase in the action of this system is a potential strategy to improve both cognitive/physiological functions in age-related disorders (Table 3).

3.2. Mouse

In mice lacking dynorphin peptides, a significant decrease in the hypothalamic level of orexin A was reported; this decrease was particularly observed in animals that received a high-fat diet and were under ad libitum condition [92] (Table 3). Orexin 1 receptor-deficient animals were resistant to diet-induced obesity and food consumption was similar between high-fat and chow food, whereas orexin 2 receptor-deficient animals showed less energy expenditure when they consumed a high-fat diet [89] (Table 3). The latter study also demonstrated that nerve cells expressing orexin are involved in the interactive action of exercise and diet on body weight gain and that orexin-deficient mice have normal brown adipose tissue. The results suggest that orexin 1 and 2 receptors exert a unique role in energy metabolism (Table 3).

It was reported that after four weeks of time-restricted feeding regimen, the plasma level of orexin A decreased; this means that this regimen regulated the expression of orexin A [86] (Table 3). In the lateral hypothalamus, no altered mRNA expression of orexin was observed in mice exposed to transient peripubertal diet-induced obesity [98]. In obese animals, a deficiency in orexins could be the cause of behavioral changes (decreased reward seeking, altered stress response, and lowered arousal) [80]. In fact, the activity of neuronal networks (hippocampus and lateral hypothalamus) was impaired when a decrease in the action mediated by orexin occurred [80] (Table 3). Finally, in mice, it was reported that orexin A decreased adiposity, intraperitoneal fat deposit and the expression of several receptors in the brain but did not affect glucose metabolism and energy expenditure [21] (Table 3).

The relationships between eating and orexinergic neurons were studied [99]. It was suggested that, when these neurons are active, eating is less likely to occur. It was reported that after eating onset, the activity of the orexinergic neurons decreased, and during eating, they remained in a down state [99]. This was observed in fasted and fed mice that received calorie-free food and foods of diverse textures/tastes, suggesting that the inactivation of the orexinergic neurons was due to the act of eating itself [99]. In the same study, the authors reported that in orexinergic-neuron-deficient mice, overweight was observed and the weight gain was prevented by mild caloric restriction [99]. The authors concluded that the activity of the orexinergic neurons can be regulated by a voluntary action, such as eating, and that it is irrespective of the food nature.

3.3. Nonhuman Primates

Maternal high-fat diet consumption resulted in increased hedonic feeding that was associated with decreased dopaminergic fibers and receptors in the prefrontal cortex, but the post-weaning consumption of high-fat diet also altered the reward neurocircuitry in nonhuman primates [100]. It was reported a decrease in the orexinergic hypothalamic projections to the rostral ventral tegmental area; this alteration may be programmed developmentally, although the possible alteration of the dopaminergic signal by orexigenic projections remains to be established [100]. In sum, both maternal and post-weaning consumption of high-fat diet may alter the neural circuits regulating reward and increase hedonic feeding in offspring, possibly through the contribution of multiple organ systems [100].

4. Orexins and Food Intake in Humans

In humans, feeding behavior is complex since some hypothalamic nuclei are involved in the regulation of food intake, stress response and rewards and, in addition, exert effects on the reward system, cortex or brainstem [4,5,101] (Table 4).

Some of these hypothalamic nuclei form a bridge toward the appetite-regulating orexigenic system [101], and reward signaling is encoded in part by neuropeptides, such as orexins [100]; thus, a link between overweight and psychological problems is very frequent (Table 4). Stress is one of the most common problems since it can cause a weight/fat increase, but also a decrease in these parameters in individuals who keep their stress response with less energy intake. Two important stress systems are the hypothalamic–pituitary–adrenal axis and the autonomic nervous system. The prolonged activation of these systems by chronical stress leads to detrimental physiological consequences, often associated with diet alterations. Chronic psychosocial stress may cause uncontrolled eating ranging from emotional eating in response to negative emotions to disinhibition or external eating (eating because food is available) up to binge eating (recurrently eating too much food because of perceiving a lack of control), all of them leading to overweight [101]. These behaviors are also dependent on age; a higher prevalence of stress-eating behaviors was reported in youths compared to adults, being that adolescence is the critical period for the onset of eating disorders [101].

In humans, it was reported that the level of orexin in the cerebrospinal fluid varies; thus, it is higher at night-time and lowest at midday [102] (Table 4). In this fluid, the level of orexin A is correlated negatively with body weight, but it is not related to body adiposity [103] (Table 4). Concerning the plasmatic levels, the diurnal levels of orexin A varied greatly between subjects. In healthy male volunteers, it was reported that orexin A peaked once or more during the whole day within different subjects with no discernible pattern with eating, wake or sleep when compared between subjects [103] (Table 4). It seems that acute feeding does not affect the plasma concentrations of orexin A in healthy subjects; thus, it is unclear if plasma orexin may have physiological significance as related to autonomic and neuroendocrine rhythms [103]. In obese individuals, the plasma level of orexin A was lower than that found in lean individuals [104] (Table 4). Plasma levels of orexin A correlated positively to body mass index (BMI), and intermittent daily fasting increased these plasmatic levels during fasting hours in healthy male volunteers [103] (Table 4).

Feeding and waking are closely associated with one another. Night eating syndrome, which predicts body weight gain, is believed to have a genetic component. Southwestern American Indians exhibit an elevated risk of obesity; with a group of this population in a clinical setting for night eating, a genetic variant of the HCRTR1 locus was reported [106]. This gene is linked to sleep regulation and feeding, and it was suggested that the HCRTR1/hypocretin (orexin receptor/orexin) system might regulate the hypothalamic–pituitary–adrenal axis. Thus, a disruption in this axis produced by variants of the above-mentioned gene could be involved in high cortisol levels and overeating as well as in night eating syndrome [106], although further studies with more participants are needed to confirm this hypothesis (Table 4).

Patients suffering from advanced Alzheimer’s disease showed an important decrease (40%) in the number of hypothalamic neurons containing orexin and in the level of orexin in the cerebrospinal fluid (14%) [107] (Table 4). Similar results were found in Parkinson’s disease: 25% reduction in the cerebrospinal fluid and 40% in the number of cell bodies [107] (Table 4). In fact, the prepro-orexin gene might be a candidate for a group of neurodegenerative disorders collectively called “chromosome 17-linked dementia”, including the disinhibition–dementia–parkinsonism–amyotrophy complex and pallido-ponto-nigral degeneration [6].

On the other hand, the orexin system seems to be associated with clinical symptoms of patients with other mental disorders; in this sense, it was reported that patients with depression showed lower levels of orexin A in the cerebrospinal fluid, higher depression scores, and lowest levels of orexin A [105] (Table 4). It was described that the levels of orexin A are positively correlated with the BMI of the subjects, and that schizophrenic patients displayed significantly higher levels of orexin A, compared to controls [105] (Table 4). In Chinese patients with chronic schizophrenia, the BMIs were positively related with orexin A levels and negatively related with negative symptoms, suggesting that the level of orexin A might modify metabolic indexes (obese patients have a higher incidence of dyslipidemia) to increase the rates of overweight and obesity observed in these inpatients [105] (Table 4). The exact influence of antipsychotic drugs on orexin A levels and obesity remains to be established, although no relationship was found between BMI and different antipsychotic treatments [105].

5. Relationships between Orexins and Other Substances

Many substances (e.g., neuropeptides) are in a constant cross talk in the feeding brain pathways, including the hypothalamic nerve cell populations expressing orexin [108,109]. In this sense, it is known that nerve cells expressing orexin are inhibited by adenosine and GABA and are excited by acetylcholine, noradrenaline, thyrotropin-releasing hormone, glutamate and corticotropin-releasing factor [25]. In this section, the relationships between orexin and other substances (e.g., AgRP, ghrelin, leptin, NPY, opioids, GABA, and glutamate) are mentioned (Table 5, Figure 3).

5.1. Agouti-Related Peptide (AgRP)

Neurons containing orexin located in the lateral hypothalamus are activated after the administration of AgRP (which increases food intake), and it is known that orexin A stimulates AgRP neurons placed in the mediobasal hypothalamus; this finding suggests that orexin is crucial for the release of AgRP and the maintenance of long-term energy balance [110] (Table 5). Moreover, the effect mediated by orexin A is blocked by neuropeptide Y receptor antagonists [111] (Table 5). The feeding mechanisms mediated by the three mentioned peptides must be studied in depth.

5.2. Neuropeptide Y

In the rat hypothalamic paraventricular nucleus, orexin A facilitates food intake and regulates the spontaneous firing of glucose-sensitive neurons [112]. Both effects were inhibited when the orexin 1 receptor antagonist SB-334,867 was administered and were weakened after treatment with a NPY 1 receptor antagonist (BMS-193,885) [112]. In addition, the administration of orexin A in the hypothalamic paraventricular nucleus induced the activation of the arcuate nucleus neurons expressing NPY [112]. This means that orexin A promotes food consumption via the NPY pathway (Table 5). Moreover, it is known that neurons containing orexin received projections from arcuate neurons expressing NPY and this means that food intake mechanisms mediated by orexins are regulated by NPY [113] (Table 5). As indicated above, the effects mediated by orexin A were blocked when a NPY receptor antagonist was administered [111].

5.3. Opioids

In obesity, opioids and orexin A located in the basomedial amygdala are involved in feeding behavior and in the control of gastric distension neuronal excitability [114]. In a diet-induced obesity rat model, the expressions of both μ-opioid receptors and orexin A were increased in the basomedial amygdala [114] (Table 5). In the same experimental model, the administration of orexin A in the latter region augmented both the firing of basomedial amygdala gastric distension neurons and food consumption [114] (Table 5). Thus, these effects could be inhibited with orexin 1 receptor antagonists (e.g., SB-334,867) and could also be somewhat attenuated by the co-administration of naloxone [114].

It is known that dynorphin and orexin peptides are co-released; in the ventral tegmental area, dynorphin inhibits the reward behavior promoted by orexins; and in the paraventricular hypothalamic nucleus, dynorphin, but not orexin, increases hedonic intake [115] (Table 5). It is also known that obesity modifies the expression of both dynorphin and orexin receptors [115] (Table 5). The administration of DYN-A_1-13 into the paraventricular hypothalamic nucleus increases hedonic intake as well as the injection of orexin A into the ventral tegmental area [115] (Table 5). In the paraventricular hypothalamic nucleus, orexin A blunted the increase (hedonic intake) mediated by DYN-A_1-13; when an opioid receptor antagonist was administered in the same nucleus; a decrease in hedonic intake was observed but the administration of orexin A did not increase the hedonic intake. This means that in the paraventricular hypothalamic nucleus, the action mediated by orexin A is not regulated by opioids and that both peptides control the hedonic intake in an opposing manner (Table 5). It was reported that the administration of a non-opioid peptide (dynorphin A_2-17) in the paraventricular hypothalamic nucleus augmented the short-term food intake and energy expenditure [116]. The DYN-A_1-13 opioid peptide increased palatable food intake, whereas orexin-A and DYN-A_2-17 decreased this intake [116]. Moreover, orexin A increased chow intake [116]. The findings suggest that orexin, opioid and non-opioid peptides play different roles in food intake/choice when non-palatable and palatable food possibilities are available (Table 5). Finally, it was reported that orexin A, via the orexin 1 receptor, blocked satiety-inducing pro-opiomelanocortin neurons [117,118] (Table 5).

5.4. Neurotensin

Neurotensinergic neurons located in the lateral hypothalamus regulate body weight via orexin mechanisms [119] (Table 5). The activation of these neurons is also needed for regulating energy balance. A downregulation of orexin was observed when a complete loss of lateral hypothalamic neurons containing neurotensin was performed [119]. Thus, neurotensinergic neurons are needed to regulate the activity of the lateral hypothalamic neurons expressing orexin (Table 5).

5.5. Cannabinoids

It is known that orexin and cannabinoid receptors form heterodimers and that the activation of the orexin receptor promotes the synthesis of 2-arachidonoyl glycerol, an endocannabinoid [37] (Table 5). Thus, a functional interaction between both systems occurred. The peripheral administration of rimonabant (a cannabinoid 1 receptor antagonist) blocked the orexinergic action of orexin A when administered intracerebroventricularly; this means that endocannabinoids regulate the expression of orexin and, hence, control food intake [120] (Table 5).

RVD-hemopressin(α) is, respectively, a positive and negative allosteric modulator of the cannabinoid 2 and 1 receptors and it is known that the endocannabinoid system is involved in feeding behavior [121]. The central administration of RVD-hemopressin(α) blocked food intake and decreased the hypothalamic expression of orexin A [121] (Table 5). Thus, the anorexigenic effect mediated by RVD-hemopressin(α) is associated to a decrease in the hypothalamic orexin A signaling. The findings suggest that orexin A could be a new pharmacological strategy for targeting the endocannabinoid system (Table 5). In addition, it was reported that in obese animals, both endocannabinoid and orexin A systems regulate feeding behavior and arcuate glucose-responsive neurons [122]. The firing of these neurons was altered after the administration of AM-251 (a cannabinoid 1 receptor antagonist) or after the administration of orexin A [122]. The antagonist decreased feeding, whereas orexin A augmented food intake and, in addition, in the arcuate nucleus, both orexin and cannabinoid 1 receptor expressions of protein/mRNA were observed [122]. Thus, the results suggest that in the arcuate nucleus, both the endocannabinoid and orexin A systems are involved in the control of food intake and in the excitability of the glucose-responsive neurons in obese individuals (Table 5).

5.6. Ghrelin

Central administration of ghrelin activates the orexigenic neurons located in the lateral hypothalamus [123]; in animals lacking orexin, the appetite stimulatory action mediated by ghrelin is blocked [130]. It is known that the capacity of ghrelin to facilitate an operant performance for a diet rich in fat is attenuated in animals without orexin [124] (Table 5). The data suggest that the modulation of food reward and feeding by ghrelin is mediated by orexins located in lateral hypothalamic neurons. Another study showed that the central administration of ghrelin activates both non-orexinergic and orexinergic pathways involved in feeding regulation [131]. Thus, ghrelin is a potential anti-obesity therapeutic target due to the orexigenic properties of this hormone.

A new ventral hippocampus-lateral hypothalamus–laterodorsal tegmental nucleus pathway regulating meal size control was demonstrated [125]. Orexin neurons, located in the lateral hypothalamus, project to the hindbrain laterodorsal tegmental nucleus, and hence through this pathway, orexin and ghrelin interact [125]. Thus, ventral hippocampus ghrelin signaling augments meal size through a downstream orexin receptor signaling in the laterodorsal tegmental nucleus (Table 5).

5.7. Leptin

This adipocyte-derived substance decreases food intake, and it is known that orexin lateral hypothalamic neurons express leptin receptors [132]. Leptin decreases the increase in prepro-orexin during fasting and the expression of the hypothalamic orexin 1 receptor [66]. However, another study showed that the administration of leptin into the lateral hypothalamus increased the level of orexin mRNA [133]. The discrepancy could be due to the time in which the expression of orexin was studied or to the experimental animal model used [30]. In addition to the direct action of leptin on the lateral hypothalamic orexinergic neurons, indirect network mechanisms were also reported [134]. Thus, it is known that leptin, acting on neurotensinergic lateral hypothalamic neurons, inhibits orexinergic neurons by two GABA-independent mechanisms (opening of K_ATP channels, and presynaptic inhibition of the excitatory neurotransmission) [134].

It is known that the peripheral orexin A decreases the level of leptin [20] (Table 5). Leptin regulates lateral hypothalamic neurons involved in the maintenance of energy homeostasis and in the regulation of food intake [126]. It was reported that leptin blocked the excitatory synaptic inputs to the lateral hypothalamic neurons expressing melanin-concentrating hormone or orexin that sends projections to the ventral tegmental area [126] (Table 5). Thus, it seems that leptin, by regulating the synaptic transmission, plays an important role in the maintenance of the energy homeostasis. This synaptic regulation is sensitive to energy states since both excessive energy storage (high-fat diet-induced obesity) and energy deficiency (acute fasting) attenuated leptin actions.

In lean and satiated mice that consumed a highly palatable food, an activation of the orexinergic neuros located in the lateral hypothalamus was observed; this activation was maintained even when the anorexigenic hormone leptin was administered [127]. In lean animals, it is also known that the overeating of palatable foods diminished when the galanin 2 receptor was activated in the lateral hypothalamus [127]. Thus, the inhibitory action on leptin on the lateral hypothalamic neurons containing orexin was blocked when a hedonically loaded food was administered, and during hedonic overeating, the blunted leptin sensitivity was reinstated when the galanin 2 receptor was activated (Table 5).

5.8. GABA

It is known that GABA neurons send projections to the lateral hypothalamus and that food intake increases the level of GABA in the same nucleus [128]. The administration of muscimol (GABA_A receptor agonist) decreases hypothalamic prepro-orexin mRNA and blocks food consumption [128] (Table 5). It was also reported that food consumption activated the GABAergic function in the lateral hypothalamus [128]. This activation, via GABA_A receptors, terminates feeding, and it seems that GABA decreases food intake by inhibiting orexinergic neurons located in the lateral hypothalamus [128] (Table 5).

5.9. Glutamate

In the ventral tegmental area, it was reported that the lateral hypothalamic orexin glucose-inhibited neurons control reward-based feeding by regulating the transmission mediated by glutamate [129] (Table 5). Fasting augmented the activation of lateral hypothalamic orexin glucose-inhibited neurons in low glucose, whereas glucose blocked lateral hypothalamic neurons expressing orexin [129] (Table 5). In low glucose (after weight loss), an increased activation of lateral hypothalamic orexin glucose-inhibited neurons was observed; this was associated with increased glutamate signaling on ventral tegmental area dopaminergic neurons and eating rewarding food, leading to weight regain [129] (Table 5).

6. Therapeutic Strategies

Unfortunately, no effective pharmacological treatment for obesity was reported, and when these treatments were applied, important side effects were observed. It is also important to note that comorbidity between mood disorders and abnormal eating behaviors is frequent.

Orexin receptor antagonists are divided into DORAs (dual orexin1 and 2 receptor antagonists, e.g., suvorexant, and lemobrexant), SORA1s (selective orexin 1 receptor antagonists, e.g., SB-334,867) and SORA2s (selective orexin a receptor antagonists, e.g., seltorexant) [135]. Many studies used orexin receptor antagonists for the treatment of sleep disorders, depression, panic, anxiety, and drug addiction [135]. Concerning feeding disorders, it is known that orexin 1 receptor antagonists block hyperphagia [33] and that SB-334,867 (an orexin 1 receptor antagonist) inhibits meal size/feeding increase and the spontaneous firing of glucose-sensitive neurons mediated by orexin A [87,112]. Orexin receptors are a potential target for the development of anti-obesity drugs that antagonize the orexinergic system; in this sense, it was suggested that a pharmacotherapy targeting the orexin receptor 1 could selectively affect binge eating of palatable food while leaving basic appetite undiminished [7]. However, as mentioned above, the orexinergic system is involved in many physiological actions, making orexins an unspecific target against obesity since serious adverse effects can occur. Thus, due to the widespread distribution of neuropeptides in the central and peripheral nervous systems and the numerous physiological actions that these substances exert, therapeutic agents based on neuropeptides showed low efficacy; hence, drug development is complicate when targeting peptidergic systems (e.g., orexin). In addition, these systems are related with redundancy and for this reason, in general, the therapies applied are ineffective when they are directed against a single target. Thus, more preclinical/clinical studies must be performed to show clearly the beneficial effects mediated by the orexin receptor antagonists. For example, in feeding behavior, the effects of these antagonists must be studied in depth since it is known that each orexin receptor (1 and 2) plays a unique role in energy metabolism and, hence, each receptor exerts a differential function in obesity [89]. Accordingly, it seems that combination therapies are the best options for successful anti-obesity treatments. In these therapies, the physiological roles played by heterodimers or oligodimers of the orexin receptor must be fully investigated since, for example, heteromers (receptor–receptor interaction) are potential targets for food intake dysregulation. Hence a promising line of research is to understand in-depth these interactions as potential therapeutic targets in the hypothalamic nuclei, playing an important role in feeding behavior.

7. Conclusions

The orexinergic system is widely studied in mammals, birds, amphibians, reptiles and fish and the connectivity of this system is widely known. However, although some data are known, the signaling pathways activated by the orexinergic system must be fully demonstrated. Orexigenic peptides A and B originate from prepro-orexin, but the enzymes implicated in this mechanism are unknown. Orexinergic neurons are classified in different neurochemical subpopulations involved in the coordination and regulation of diverse physiological actions. These neurons project to different hypothalamic and extrahypothalamic regions, and thus, the complexity to fully understand the mechanisms involved in feeding behavior and motivation to consume food is increased, and a link between psychological problems and overweight is frequent.

The metabolic status controls the action of orexins on the intake of food. Diurnal variations in orexin levels were reported, and the expression of orexin varied during the development of obesity, indicating the differential roles played by orexin, at different feeding periods, in food consumption. There are contradictory data regarding the action of orexin A on the thyroid–pituitary axis; this must be solved by performing new experiments, as well as the sexually dimorphic role played by orexins. Moreover, the potentiation of the orexinergic system is a promising strategy for the improvement of cognitive/physiological actions in age-related disorders, although the concrete fluctuations of orexins observed in neurodegenerative diseases must be studied in depth. In addition, orexin A could be a new pharmacological strategy for targeting the endocannabinoid system.

The development of anti-obesity therapies must be focused on combination therapies, due to the widespread physiological actions exerted by the orexinergic system. For this reason, is crucial to understand in depth the relationships between orexins and other substances. It seems that the combination of different types of therapies is the best approach for the treatment of obesity and hence, this research line must be developed in the future.

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Figure 1. Schematic representation of the main hypothalamic regions implicated in the control of food intake. Neuroactive substances involved in feeding regulation are represented at the right side of the image, and receptors are represented at the left part of the schema. Abbreviations: 3V—third ventricle; AgRP—agouti-related peptide; Arc—arcuate hypothalamic nucleus; α-MSH—alpha-melanocyte stimulating hormone; CART—cocaine and amphetamine regulated transcript; DMN—dorsomedial hypothalamic nucleus; Enk—enkephalins; GABA—gamma-aminobutyric acid; GAL—galanin; GALP—galanin-like peptide; GalR1—galanin receptor type 1; GalR2—galanin receptor type 2; GalR3—galanin receptor type 3; GHRF—growth hormone-releasing factor; Glut—glutamate; GHS-R—growth hormone secretagogue receptor; LH—lateral hypothalamus; MC3R—melanocortin receptor type 3; MC4R—melanocortin receptor type 4; MCH—melanin-concentrating hormone; NPY—neuropeptide Y; OX1R—orexin receptor 1; OX2R—orexin receptor 2; OXTR—oxytocin receptor; POMC—pro-opiomelanocortin; PVH—paraventricular hypothalamic nucleus; SON—supraoptic nucleus; VMN—ventromedial hypothalamic nucleus; Y1—NPY receptor type 1; Y2—NPY receptor type 2; Y5—NPY receptor type 5.

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Figure 2. Relationships between different hypothalamic and extrahypothalamic regions involved in the control of feeding. Orexinergic neurons of the lateral hypothalamus send direct projections to other hypothalamic nuclei (posterior hypothalamus), different regions of the brainstem and spinal cord as well as forebrain structures and receive inputs from the median raphe or the ventromedial hypothalamus. Green arrows represent direct activation exerted from the orexinergic neurons to thalamo-cortical neurons, the ventral tegmental area or the NPY/AgRP neurons of the arcuate nucleus, and the red arrow represents the inhibitory projection from orexigenic neurons to POMC/CART neurons of the arcuate nucleus. Abbreviations: Acb—accumbens nucleus; Arc—arcuate hypothalamic nucleus; LC—locus coeruleus; LH—lateral hypothalamus; NPY/AgRP—neurons of the arcuate nucleus containing neuropeptide Y and agouti-related peptide; PAG—periaqueductal gray matter; POMC/CART—neurons of the arcuate nucleus containing pro-opiomelanocortin and cocaine- and amphetamine-regulated transcript; PVH—paraventricular hypothalamic nucleus; VTA—ventral tegmental area.

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Figure 3. Interactions of orexin with other substances. Green arrows represent activation and red arrows represent inhibition. Blue arrows mean related actions: glucose activates the secretion of orexin by neurons of the lateral hypothalamus, and this activation leads to an increase in glutamate in dopaminergic neurons of the ventral tegmental area. Abbreviations: AgRP—agouti-related protein; Arc—arcuate hypothalamic nucleus; DA—dopamine; Dyn-A—dynorphin-A; GABA—gamma-aminobutyric acid; Glut—glutamate; LH—lateral hypothalamus; NPY—neuropeptide Y; NT—neurotensin; POMC—pro-opiomelanocortin; VTA—ventral tegmental area.

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