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Query: UMLS:C0028754 (
obesity
)
124,988
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Neuropeptide Y
regulates numerous physiological processes via at least five different Y receptors, but the specific roles of each receptor are still unclear. We previously demonstrated that Y2 receptor knockout results in a lean phenotype, increased cancellous bone volume, and an increase in plasma pancreatic polypeptide (PP), a ligand for Y4 receptors. PP-overexpressing mice are also known to have a lean phenotype. Deletion of the Y4 receptor also produced a lean phenotype and increased plasma PP levels. We therefore hypothesized that part of the Y2 phenotype results from increased PP action on Y4 receptors and tested this in PP transgenic Y4(-/-) and Y2(-/-) Y4(-/-) double knockout mice. Bone mass was not altered in Y4 knockout mice. Surprisingly, despite significant hyperphagia, Y2(-/-) Y4(-/-) mice retained a markedly lean phenotype, with reduced body weight, white adipose tissue mass, leptinemia, and insulinemia. Furthermore, bone volume was also increased threefold in Y2(-/-) Y4(-/-) mice, and this was associated with enhanced osteoblastic activity. These changes were more pronounced than those observed in Y2(-/-) mice, suggesting synergy between Y2 and Y4 receptor pathways. The lack of bone changes in PP transgenic mice suggests that PP alone is not responsible for the bone mass increases but might play a major role in the lean phenotype. However, a synergistic interaction between Y2 and Y4 pathways seems to regulate bone volume and adiposity and could have important implications for possible interventions in
obesity
and for anabolic treatment of osteoporotic bone loss.
...
PMID:Synergistic effects of Y2 and Y4 receptors on adiposity and bone mass revealed in double knockout mice. 1286 Oct 9
Neuropeptide Y
(
NPY
) is a powerful orexigenic neurotransmitter. The
NPY
Y1 and Y5 receptors have been implicated in mediating the appetite-stimulating activity of
NPY
. To further investigate the importance of these two receptors in
NPY
-induced hyperphagia after chronic central administration, we used mice lacking either Npy1r or Npy5r expression.
NPY
infusion into the lateral ventricle of wild-type mice stimulated food intake and induced
obesity
over a 7-d period. Fat pad weight as well as plasma insulin, leptin, and corticosterone levels were strongly increased in
NPY
-treated mice. In addition,
NPY
infusion resulted in a significant decrease in hypothalamic
NPY
and proopiomelanocortin expression. Interestingly, the lack of either Npy1r or Npy5r expression in knockout mice did not affect such feeding response to chronic
NPY
infusion. Moreover, the
obesity
syndrome that developed in these animals was similar to that in wild-type animals. Taken together, these data strongly suggest biological redundancies between Y1 and Y5 receptor signaling in the
NPY
-mediated control of food intake.
...
PMID:Chronic neuropeptide Y infusion into the lateral ventricle induces sustained feeding and obesity in mice lacking either Npy1r or Npy5r expression. 1452 13
Neuropeptide Y
(
NPY
), a 36-amino-acid neuropeptide is the most potent physiological appetite transducer known. Episodic
NPY
neurosecretion in hypothalamic target sites is temporally linked with onset of the daily feeding pattern. Upregulation of
NPY
signaling in the arcuate nucleus-paraventricular nucleus (ARC-PVN) neural axis is responsible for the hyperphagia evoked by dieting, fasting, hormonal and genetic factors, and disruption in intrahypothalamic signaling. Clusters of
NPY
-producing neurons in the ARC that coexpress gamma- amino butyric acid and agouti-related peptide, and those in the brain stem (BS) that coexpress catecholamines and galanin, participate in disparate manners to regulate appetitive behavior.
NPY
receptors, Y1, Y2, and Y5, expressed by various components of the
NPY
network, mediate
NPY
-induced feeding. Imbalance in
NPY
signaling due either to high or low abundance of
NPY
at target sites elicits hyperphagia leading to increased fat accretion and
obesity
. Recent studies show that intermittent, feedback action of opposing afferent hormonal signals-leptin from adipose tissue and ghrelin from stomach-regulate the episodic secretion of orexigenic
NPY
in the PVN-ARC. Apparently, the hypothalamic
NPY
network is the primary common pathway intimately involved in genesis of appetite- stimulating impulses.
...
PMID:Neuropeptide Y: a physiological orexigen modulated by the feedback action of ghrelin and leptin. 1461 Feb 98
Neuropeptide Y
(
NPY
) is present in the hypothalamus, where it is believed to play a key role in the control of food intake. Evidence for this assertion has come from studies demonstrating that acute administration of
NPY
into the hypothalamus or into the brain ventricles leads to increased food intake. In the case of chronic administration, the hyperphagic effects of
NPY
are prolonged, leading to the development of an obese state.
NPY
levels in the hypothalamus are temporally correlated with food intake and are markedly elevated in response to energy depletion. However, attempts to demonstrate an important role for
NPY
in the control of food intake using
NPY
knockout mice,
NPY
antisense oligodeoxynucleotides and anti-
NPY
antibodies has produced equivocal results. Despite this, many pharmaceutical companies have moved ahead with the search for antagonists of
NPY
receptor subtypes as appetite suppressant/anti-
obesity
agents. Antagonists of the
NPY
Y5 subtype seemed initially promising since analogs of
NPY
with high selectivity for this receptor strongly stimulated food intake. However, once again, attempts to inhibit the signaling of
NPY
through the
NPY
Y5 receptor produced equivocal effects on food intake. Many thousands of
NPY
Y5 antagonists have been made which fall into two main categories: those that influence food intake and those that do not. Those compounds that do inhibit food intake appear to do so by interactions with non-
NPY
Y5 related mechanisms. Thus, current evidence would suggest that antagonists of
NPY
acting through the
NPY
Y5 receptor subtype will not be useful appetite suppressant/anti-
obesity
agents.
...
PMID:Neuropeptide Y Y5 receptor antagonists as anti-obesity drugs. 1464 11
Neuropeptide Y
(
NPY
) and galanin have both been implicated in the regulation of body weight, yet mice bearing deletions of either of these molecules have unremarkable metabolic phenotypes. To investigate whether galanin and
NPY
might compensate for one another, we produced mutants lacking both neuropeptides (GAL(-/-)/
NPY
(-/-)). We found that male GAL(-/-)/
NPY
(-/-) mice ate significantly more and were much heavier (30%) than wild-type (WT) controls. GAL(-/-)/
NPY
(-/-) mice responded to a high-fat diet by gaining more weight than WT mice gain, and they were unable to regulate their weight normally after a change in diet. GAL(-/-)/
NPY
(-/-) mice had elevated levels of leptin, insulin, and glucose, and they lost more weight than WT mice during chronic leptin treatment. Galanin mRNA was increased in the hypothalamus of
NPY
(-/-) mice, providing evidence of compensatory regulation in single mutants. The disruption of energy balance observed in GAL(-/-)/
NPY
(-/-) double knockouts is not found in the phenotype of single knockouts of either molecule. The unexpected
obesity
phenotype may result from the dysregulation of the leptin and insulin systems that normally keep body weight within the homeostatic range.
...
PMID:Obesity and endocrine dysfunction in mice with deletions of both neuropeptide Y and galanin. 1502 85
The hypothalamus and other brain regions that control energy homeostasis contain neuronal populations that produce specific neuropeptides which have experimental effects on feeding behavior and body weight. Here, we describe examples of neuropeptides that exert 'anabolic' effects, notably stimulation of feeding and increased body weight.
Neuropeptide Y
(
NPY
) neurons in the hypothalamic arcuate nucleus (ARC) are inhibited by leptin and insulin, and thus are stimulated in states of energy deficit and fat loss, e.g., underfeeding.
NPY
neuronal overactivity contributes to enhanced hunger and food-seeking activity under these conditions. The lateral hypothalamic area (LHA) contains specific neuronal populations that affect feeding in different ways. Neurons expressing the appetite-stimulating peptide orexin A are stimulated by starvation (but not food restriction) and by hypoglycemia, but only if food is withheld. Orexin neurons are apparently activated by low glucose but are promptly inhibited by visceral feeding signals, probably mediated via vagal sensory pathway and the nucleus of the solitary tract (NTS); a short-term role in initiating feeding seems most likely. Other LHA neurons express melanin-concentrating hormone (MCH), which transiently increases food intake when injected centrally. MCH neurons may be regulated by leptin, insulin and glucose. Glucose-sensing neurons in the hypothalamus and elsewhere are sensitive to other cues of nutritional state, including visceral satiety signals (transmitted via the vagus) and orexin A. Thus, long- and short-term humoral and neural signals interact with each other to meet diverse nutritional needs, and anabolic neuropeptides are important in the overall integration of energy homeostasis. Clarifying the underlying mechanisms will be essential to understanding normal energy balance and the pathogenesis and treatment of disorders, such as
obesity
and cachexia.
...
PMID:Anabolic neuropeptides. 1515 68
Neuropeptide Y
(
NPY
) in the central nervous system is a major regulator of food consumption and energy homeostasis. It also regulates blood pressure, induces anxiolysis, enhances memory retention, affects circadian rhythms and modulates hormone release. Five Y receptors (Y1, Y2, Y4, Y5 and Y6) are known to mediate the action of
NPY
and its two other family members, peptide YY (PYY) and pancreatic polypeptide (PP). Increased
NPY
signaling due to elevated
NPY
expression in the hypothalamus leads to the development of
obesity
and its related phenotypes, Type II diabetes and cardiovascular disease. Dysregulation in
NPY
signaling also causes alterations in bone formation, alcohol consumption and seizure susceptibility. The large number of Y receptors has made it difficult to delineate their individual contributions to these physiological processes. However, recent studies analysing
NPY
and Y receptor overexpressing and knockout models have started to unravel some of the different functions of these Y receptors. Particularly, the use of conditional knockout models has made it possible to pinpoint a specific function to an individual Y receptor in a particular location.
...
PMID:NPY and Y receptors: lessons from transgenic and knockout models. 1533 71
Neuropeptide Y
is the most potent physiological appetite transducer known. The NPY network is the conductor of the hypothalamic appetite regulating orchestra in the arcuate nucleus-paraventricular nucleus (ARC-PVN) of the hypothalamus. NPY and cohorts, AgrP, GABA and adrenergic transmitters, initiate appetitive drive directly through Y1, Y5, GABAA and alpha1 receptors, co-expressed in the magnocellular PVN (mPVN) and ARC neurons and by simultaneously repressing anorexigenic melanocortin signaling in the ARC-PVN axis. The circadian and ultradian rhythmicities in NPY secretion imprint the daily circadian and episodic feeding patterns. Although a number of afferent hormonal signals from the periphery can directly modulate NPYergic signaling, the reciprocal circadian and ultradian rhythmicities of anorexigenic leptin from adipocytes and orexigenic ghrelin from stomach, encode a corresponding pattern of NPY discharge for daily meal patterning. Subtle and progressive derangements produced by environmental and genetic factors in this exquisitely intricate temporal relationship between the two opposing humoral signals and the NPY network promote hyperphagia and abnormal rate of weight gain culminating in
obesity
and attendant metabolic disorders. Newer insights at cellular and molecular levels demonstrate that a breakdown of the integrated circuit due both to high and low abundance of NPY at target sites, underlies hyperphagia and increased adiposity. Consequently, interruption of NPYergic signaling at a single locus with NPY receptor antagonists may not be the most efficacious therapy to suppress hyperphagia and
obesity
. Central leptin gene therapy in rodents has been shown to subjugate, i.e. bring under homeostatic control, NPYergic signaling and suppress the age-related and dietary
obesity
for extended periods and thus shows promise as a newer treatment modality to curb the pandemic of
obesity
and metabolic syndrome.
...
PMID:NPY and cohorts in regulating appetite, obesity and metabolic syndrome: beneficial effects of gene therapy. 1533 72
Neuropeptide Y
(
NPY
) is one of the most abundant peptides in the central nervous system and currently there are four known receptor subtypes Y1, Y2, Y4 and Y5. Central
NPY
and its receptors have been implicated in a variety of physiological processes such as epilepsy, sleep,
obesity
, learning and memory, gastrointestinal regulation, alcoholism, depression and anxiety. The localization of these receptors within the brain is consistent with the roles mentioned, as they are found in varying density within the limbic structures, such as the hippocampal formation, amygdala, hypothalamus and septum. It is well understood that
NPY
produces anxiolytic responses following central administration under stressful or anxiety-provoking situations. In contrast, central administration of the neuropeptide corticotropin-releasing factor (CRF) produces anxiogenic behaviors. It has been proposed that
NPY
counteracts the effects of CRF to maintain no net change in emotional state, e.g., emotional homeostasis. In this article, we review the scientific literature describing the
NPY
-CRF relationship, specifically as it relates to the modulation of the CRF-mediated stress responses via the amygdala, a key forebrain structure involved in the regulation of emotional states.
...
PMID:Interactions between NPY and CRF in the amygdala to regulate emotionality. 1533 74
Neuropeptide Y
(
NPY
) and leptin are two peptides involved in the regulation of body weight, energy balance, and sympathetic tone. This study investigates the independent role of apneas and
obesity
on
NPY
and leptin plasma levels in patients with obstructive sleep apnea syndrome (OSAS). To this end we compared their values in 23 obese (body mass index > 30 kg/m2) and 24 nonobese (body mass index < 27 kg/m2) patients with OSAS, and in 19 obese and 18 nonobese control subjects without OSAS. Patients who used continuous positive airway pressure for more than 4 hours/night were reexamined 3 and 12 months later. We found that
NPY
levels were increased (p < 0.01) in patients with OSAS independently of
obesity
. Leptin levels were also increased in OSAS but this was mostly associated to
obesity
. Continuous positive airway pressure treatment reduced
NPY
levels in all patients and leptin levels only in nonobese patients (p < 0.01). We concluded that
NPY
and leptin plasma levels are increased in patients with OSAS. Yet, whereas the former appear independent of
obesity
, the latter are mostly associated with
obesity
.
...
PMID:Neuropeptide Y and leptin in patients with obstructive sleep apnea syndrome: role of obesity. 1551 36
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