Kisspeptin Depolarizes Gonadotropin-Releasing Hormone Neurons through Activation of TRPC-Like Cationic Channels

Zhang, Chunguang; Roepke, Troy A.; Kelly, Martin J.; Rønnekleiv, Oline K.

doi:10.1523/jneurosci.5352-07.2008

Cited by 211 publications

(268 citation statements)

References 80 publications

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“…This approach evidenced that the stimulatory effects of Kp-10 on GnRH secretion require the activation of phospholipase-C (PLC), mobilization of intracellular Ca 2+ stores and recruitment of ERK1/2 and p38 kinases, while kisspeptininduced GnRH release was preserved in spite of the blockade of adenylate cyclase ( Figure 1); features that are grossly similar to those initially reported for KISS1R signaling using heterologous cell systems [9]. Likewise, recent studies involving electrophysiological recordings and/or calcium imaging in GnRH neurons have supported and extended those observations, showing that long-term excitation of GnRH neurons by kisspeptin is conveyed through a PLC/calcium dependent pathway regulating multiple ion channels, including the closing of potassium channels and the activation of non-selective cation (NSC) channels, which likely include canonical transient receptor potential (TRPC) channels [13][14][15].…”

Section: Kisspeptin Signaling: Molecular Biology Of Kiss1rmentioning

confidence: 84%

Kisspeptin signaling in the brain: Recent developments and future challenges

Tena‐Sempere

2010

Molecular and Cellular Endocrinology

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Kisspeptins, a family of peptides encoded by the KISS1 gene which binds GPR54 (or KISS1 receptor), have recently emerged as essential neuropeptide regulators of key aspects of reproductive maturation and function, including puberty onset, neuroendocrine control of ovulation and metabolic regulation of fertility. Yet, while the neuroanatomy of kisspeptin system has begun to be deciphered, and the involvement of kisspeptins in the above phenomena has been experimentally documented in recent years, precise information on the signaling events underlying these functions has remained scarce. Similarly, the nature and mechanisms of action of most of the regulatory signals of KISS1 expression in the brain are largely unknown. In this review, we will comprehensively summarize some of the recent developments in these areas of kisspeptin physiology, with the ultimate aim to delineate unresolved questions and future pathways for the progression of this active field of Neuroendocrinology.

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Section: Kisspeptin Signaling: Molecular Biology Of Kiss1rmentioning

confidence: 84%

Kisspeptin signaling in the brain: Recent developments and future challenges

Tena‐Sempere

2010

Molecular and Cellular Endocrinology

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“…This inward current had a linear voltage dependence from −120 to −40 mV and was suppressed at a mean value of −41.12 ± 3.54 mV (n = 4; Fig. 2 D2), suggesting the activation of a nonselective cation conductance (27,28). This value was also close to the membrane potential measured in current-clamp mode (−45.66 ± 1.68 mV, t test; P > 0.05; n = 7; Fig.…”

Section: Pge 2 Elicits Membrane Depolarization Of Gnrh Neurons Via Amentioning

confidence: 96%

Prostaglandin E ₂ release from astrocytes triggers gonadotropin-releasing hormone (GnRH) neuron firing via EP2 receptor activation

Clasadonte

Poulain

Hanchate

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

103

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Astrocytes in the hypothalamus release prostaglandin E 2 (PGE 2 ) in response to cell-cell signaling initiated by neurons and glial cells. Upon release, PGE 2 stimulates the secretion of gonadotropin-releasing hormone (GnRH), the neuropeptide that controls reproduction, from hypothalamic neuroendocrine neurons. Whether this effect on GnRH secretion is accompanied by changes in the firing behavior of these neurons is unknown. Using patch-clamp recording we demonstrate that PGE 2 exerts a dose-dependent postsynaptic excitatory effect on GnRH neurons. These effects are mimicked by an EP2 receptor agonist and attenuated by protein kinase A (PKA) inhibitors. The acute blockade of prostaglandin synthesis by indomethacin (INDO) or the selective inhibition of astrocyte metabolism by fluoroacetate (FA) suppresses the spontaneous firing activity of GnRH neurons in brain slices. Similarly, GnRH neuronal activity is reduced in mice with impaired astrocytic PGE 2 release due to defective erbB signaling in astrocytes. These results indicate that astrocyte-to-neuron communication in the hypothalamus is essential for the activity of GnRH neurons and suggest that PGE 2 acts as a gliotransmitter within the GnRH neurosecretory system. cyclooxygenase | glia-to-neuron signaling | luteinizing hormone-releasing hormone | preoptic region | fertility I t is increasingly clear that astrocytes play an important role in maintaining central nervous system function (1-3) and controlling key bodily processes, such as breathing (4), sleep (5), and reproduction (6). Because of their perivascular and interneuronal localization, astrocytes are well positioned to sense afferent neuronal and blood-borne signals and ideally suited for the temporal and spatial propagation of these signals (7-9). The activation of astrocytes leads to the release of gliotransmitters (8, 10) that trigger rapid responses in neighboring cells and thus contribute to the region-specific homeostatic regulation of neuronal function.In the hypothalamus, astrocytes regulate the secretory activity of neuroendocrine neurons (11)(12)(13)(14). A subset of such neurons secretes the decapeptide gonadotropin-releasing hormone (GnRH), which controls both the initiation of puberty and adult reproductive function. In rodents, GnRH neurons are mostly located in the preoptic region of the ventral forebrain. They project to the median eminence of the hypothalamus, where GnRH is released into the pituitary portal blood for delivery to the anterior pituitary. In the pituitary, GnRH elicits the secretion of luteinizing hormone and follicle-stimulating hormone, which stimulate gametogenesis and gonadal hormone secretion and thus support reproductive function. It is now clear that the secretory activity of GnRH neurons is controlled by both neuronal and glial input (12,13,15,16). Whereas glutamate is a key neurotransmitter involved in the transsynaptic activation of GnRH neurons (17, 18), prostaglandin E 2 (PGE 2 ) mediates cell-cell communication between astrocytes and GnRH neurons (6,19,20). A...

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“…Kisspeptin and its receptor are critical for reproduction (10)(11)(12); both kisspeptin and kisspeptin receptor knockout mice fail to enter puberty, and humans with loss of function mutations in the kisspeptin receptor exhibit hypogonadotropic hypogonadism and are infertile (13)(14)(15). Mechanistically, kisspeptin is a potent activator of GnRH neurons (16)(17)(18)(19); it enhances pituitary gonadotropin release, triggering a cascade that is essential for entering puberty (13,20) and for maintaining ovulation and fertility (21).…”

mentioning

confidence: 99%

Melanin-concentrating hormone directly inhibits GnRH neurons and blocks kisspeptin activation, linking energy balance to reproduction

Dumalska²,

Morozova³

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

104

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A link between energy balance and reproduction is critical for the survival of all species. Energy-consuming reproductive processes need to be aborted in the face of a negative energy balance, yet knowledge of the pathways mediating this link remains limited. Fasting and food restriction that inhibit fertility also upregulate the hypothalamic melanin-concentrating hormone (MCH) system that promotes feeding and decreases energy expenditure; MCH knockout mice are lean and have a higher metabolism but remain fertile. MCH also modulates sleep, drug abuse behavior, and mood, and MCH receptor antagonists are currently being developed as antiobesity and antidepressant drugs. Despite the clinical implications of MCH, the direct postsynaptic effects of MCH have never been reported in CNS neurons. Using patch-clamp recordings in brain slices from multiple lines of transgenic GFP mice, we demonstrate a strong inhibitory effect of MCH on an exclusive population of septal vGluT2-GnRH neurons that is activated by the puberty-triggering and preovulatory luteinizing hormone surge-mediating peptide, kisspeptin. MCH has no effect on kisspeptin-insensitive GnRH, vGluT2, cholinergic, or GABAergic neurons located within the same nucleus. The inhibitory effects of MCH are reproducible and nondesensitizing and are mediated via a direct postsynaptic Ba 2؉ -sensitive K ؉ channel mechanism involving the MCHR1 receptor. MCH immunoreactive fibers are in close proximity to vGluT2-GFP and GnRH-GFP neurons. Importantly, MCH blocks the excitatory effect of kisspeptin on vGluT2-GnRH neurons. Considering the role of MCH in regulating energy balance and of GnRH and kisspeptin in triggering puberty and maintaining fertility, MCH may provide a critical link between energy balance and reproduction directly at the level of the kisspeptin-activated vGluT2-GnRH neuron.fertility ͉ gonadotropins ͉ HPG axis ͉ obesity ͉ starvation N utritional status and availability of energy stores exert a profound impact on reproductive function (1-3). Reproduction is an expensive energy-consuming process, and thus it is important that puberty, pregnancy, and lactation occur only when metabolic fuel is available (4). Availability of metabolic fuel is conveyed to the brain by peripherally generated signals, such as leptin, insulin, and ghrelin, as well as by centrally released peptides such as neuropeptide Y, melanocortins, and melanin-concentrating hormone (MCH). One or more of these signals can directly or indirectly link energy balance with reproduction at one or more levels of the hypothalamic-pituitary-gonadal (HPG) axis. Thus, insulin and leptin may indirectly influence GnRH neurons (2, 5-7); leptin could regulate the HPG axis via kisspeptin-containing hypothalamic neurons (8, 9). Kisspeptin and its receptor are critical for reproduction (10-12); both kisspeptin and kisspeptin receptor knockout mice fail to enter puberty, and humans with loss of function mutations in the kisspeptin receptor exhibit hypogonadotropic hypogonadism and are infertile (13-15). Mechanisti...

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Kisspeptin Depolarizes Gonadotropin-Releasing Hormone Neurons through Activation of TRPC-Like Cationic Channels

Cited by 211 publications

References 80 publications

Kisspeptin signaling in the brain: Recent developments and future challenges

Kisspeptin signaling in the brain: Recent developments and future challenges

Prostaglandin E ₂ release from astrocytes triggers gonadotropin-releasing hormone (GnRH) neuron firing via EP2 receptor activation

Melanin-concentrating hormone directly inhibits GnRH neurons and blocks kisspeptin activation, linking energy balance to reproduction

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Kisspeptin Depolarizes Gonadotropin-Releasing Hormone Neurons through Activation of TRPC-Like Cationic Channels

Cited by 211 publications

References 80 publications

Kisspeptin signaling in the brain: Recent developments and future challenges

Kisspeptin signaling in the brain: Recent developments and future challenges

Prostaglandin E 2 release from astrocytes triggers gonadotropin-releasing hormone (GnRH) neuron firing via EP2 receptor activation

Melanin-concentrating hormone directly inhibits GnRH neurons and blocks kisspeptin activation, linking energy balance to reproduction

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Prostaglandin E ₂ release from astrocytes triggers gonadotropin-releasing hormone (GnRH) neuron firing via EP2 receptor activation