Intracellular Calcium Concentrations Regulated by Cyclic ADP-Ribose and Heat in the Mouse Hypothalamus

Liu, Hongxiang; Lopatina, Olga; Amina, Sarwat; Higashida, Chiharu; Islam, Mohammad S.; Graeff, Richard; Lee, Hon-Cheung; Hashii, Minako; Higashida, Haruhiro

doi:10.1166/msr.2012.1015

Cited by 9 publications

(12 citation statements)

References 66 publications

(101 reference statements)

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“…Other types of voltage-dependent Ca 2+ channels are also involved in oxytocinergic neurons (Tobin et al, 2011). Recently, we showed that OXT release is also sensitive to hyperthermia and Ca 2+ influx via TRPM2 channels (Amina et al, 2010; Liu et al, 2012a). …”

Section: Oxytocin and Cyclic Adp-ribosementioning

confidence: 99%

The Roles of Oxytocin and CD38 in Social or Parental Behaviors

Lopatina¹,

Инжутова²,

Салмина³

et al. 2013

Front. Neurosci.

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The nine amino acid peptide oxytocin (OXT) has been directly associated with different types of behavioral reactions. The formation and maintenance of social relationships in youth and middle age are important components of human mental health. A deficit in healthy behavioral formation leads to social isolation and limitation of well-being. Mice are social animals and are therefore useful for investigating the neurobiological mechanisms of cognitive process control, including the development of social relationships and social skills. Studies in mice may broaden our understanding of the human condition. The multifunctional protein CD38/ADP-ribosyl cyclase is highly expressed in the brain, plays an important role in central OXT release, and regulates social memory. In this review article, we discuss the mechanisms of social behavior affected by the dysregulation of brain OXT function as a consequence of a lack of CD38. OXT bound to OXT receptors initiates autoregulatory positive feedback of OXT release in the hypothalamus and posterior pituitary. OXT bio-behavioral positive feedback is usually implicated in female reproductive systems, but can also be observed in social behavior. Exogenous stimuli (OXT treatment in vitro, OXT intravenous or intraventricular administration, and nasal OXT delivery) initiate activation of OXT neurons via PKC-CD38/ADP-ribosyl cyclase cascades and result in the modulation of social behavior in humans and mice. Based on these findings, we reviewed the functions of OXT and its properties with respect to the development of therapies for human social behavior impairments in psychological diseases. In addition, preliminary studies of continuous nasal OXT administration on subjects with autism spectrum disorders are described.

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Section: Oxytocin and Cyclic Adp-ribosementioning

confidence: 99%

The Roles of Oxytocin and CD38 in Social or Parental Behaviors

Lopatina¹,

Инжутова²,

Салмина³

et al. 2013

Front. Neurosci.

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“…We cannot exclude the possibility that CD38 may act as a binding partner of M-channels or other types of ion channels, because it has recently been shown that CD38 and TRPM2 are co-immunoprecipitated and functionally interact and that CD38 acts as an activating element for hypertonicity-induced cation channels and TRPM2 channels in cell proliferation or hypertonic volume response of cells (Numata et al, 2012). We also showed that TRPM2 channels are involved in cADPR-induced [Ca 2+ i increases in NG108-15 cells , which may explain hyperthermia-induced [Ca 2+ i increases in the hypothalamus (Liu et al, 2012). Therefore, it is of interest to examine whether TRPM2 also contributes to mAChR signaling.…”

Section: Discussionmentioning

confidence: 52%

Acetylcholine-Induced M/KCNQ Current Inhibition is Regulated by CD38 and A-Kinase Anchoring Protein in Neuroblastoma Cells

et al. 2013

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The CD38 membrane protein exhibits multifunctional activities: ADP-ribosyl cyclase, cyclic ADP-ribose hydrolase, NAD + glycohydrolase, formation of nicotinic acid adenine dinucleotide phosphate (NAADP + by base exchange and degradation of NAADP + to 2 -phospho-ADP-ribose. The intermediate product of ADP-ribosyl cyclase of CD38 is cyclic ADP-ribose (cADPR). The role of cADPR as a second messenger in neurons is not completely understood. The present study was performed to determine whether cADPR plays a role as a second messenger as a downstream component of muscarinic acetylcholine receptor (mAChR) signaling in neuronal cells. We performed electrophysiology experiments on non-inactivating voltage-dependent potassium M-like currents, which are currently defined as currents due to KCNQ 2/3 or Kv 7.2/7.3 potassium channels. We first examined NG108-15 neuroblastoma × glioma hybrid cells expressing both m1 mAChRs and human CD38. ACh-evoked inhibition of the M-like current was significantly enhanced in CD38-transformed cells compared to control cells. ACh-induced inhibition was greater in the (KCNQ) components with faster kinetics in M-like currents than another (HERG) component with a slow decay time constant. The CD38-enhanced M-like current inhibition was decreased in the presence of 8-bromo-cADPR. Although overexpression of A-kinase anchoring protein (AKAP) did not interfere with AChinduced inhibition, alternative expression of mutant AKAP lacking the protein kinase C binding domain reduced ACh-induced M-like current inhibition in transformed NG108-15 cells with CD38 and mAChRs. These results indicate that overexpression and deletion of CD38 modulate M-current inhibition by ACh, and suggest that CD38 and cADPR are located downstream of mAChRs and upstream of AKAP-involved protein kinase C-induced inhibition of Kv 7.2 channels in the mAChR signaling cascade.

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“…Subsequently, in isolated hypothalamic neurons, application of 100 pM OT results in [Ca 2+ ] i increases: a rapid initial increase and a sustained elevation lasting for 5 min [ 69 ]. OT elicits an initial elevation of the maximum [Ca 2+ ] i , and this phase is IP 3 -dependent.…”

Section: Effects Of Oxytocin On Adp-ribosyl Cyclase and Intracellularmentioning

confidence: 99%

“…Pretreatment with 8-bromo-cADPR, an antagonist of the cADPR-binding site of Ca 2+ release channels of ryanodine, inhibits OT-mediated sustained [Ca 2+ ] i increases. ADPR and β-NAD + also induce elevation of [Ca 2+ ] i and replicate the second phase of sustained [Ca 2+ ] i increases [ 49 , 69 ]. Under Ca 2+ -free conditions, the OT-mediated increase of [Ca 2+ ] i shows little change in either phase, suggesting that the two phases of [Ca 2+ ] i elevation in hypothalamic neurons are due to Ca 2+ mobilization from the intracellular Ca 2+ pools [ 49 ].…”

Section: Effects Of Oxytocin On Adp-ribosyl Cyclase and Intracellularmentioning

confidence: 99%

Somato-axodendritic release of oxytocin into the brain due to calcium amplification is essential for social memory

Higashida

2015

J Physiol Sci

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Oxytocin (OT) is released into the brain from the cell soma, axons, and dendrites of neurosecretory cells in the hypothalamus. Locally released OT can activate OT receptors, form inositol-1,4,5-trisphosphate and elevate intracellular free calcium (Ca2+) concentrations [(Ca2+)i] in self and neighboring neurons in the hypothalamus, resulting in further OT release: i.e., autocrine or paracrine systems of OT-induced OT release. CD38-dependent cyclic ADP-ribose (cADPR) is also involved in this autoregulation by elevating [Ca2+]i via Ca2+ mobilization through ryanodine receptors on intracellular Ca2+ pools that are sensitive to both Ca2+ and cADPR. In addition, it has recently been reported that heat stimulation and hyperthermia enhance [Ca2+]i increases by Ca2+ influx, probably through TRPM2 cation channels, suggesting that cADPR and TRPM2 molecules act as Ca2+ signal amplifiers. Thus, OT release is not simply due to depolarization–secretion coupling. Both of these molecules play critical roles not only during labor and milk ejection in reproductive females, but also during social behavior in daily life in both genders. This was clearly demonstrated in CD38 knockout mice in that social behavior was impaired by reduction of [Ca2+]i elevation and subsequent OT secretion. Evidence for the associations of CD38 with social behavior and psychiatric disorder is discussed, especially in subjects with autism spectrum disorder.

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Intracellular Calcium Concentrations Regulated by Cyclic ADP-Ribose and Heat in the Mouse Hypothalamus

Cited by 9 publications

References 66 publications

The Roles of Oxytocin and CD38 in Social or Parental Behaviors

The Roles of Oxytocin and CD38 in Social or Parental Behaviors

Acetylcholine-Induced M/KCNQ Current Inhibition is Regulated by CD38 and A-Kinase Anchoring Protein in Neuroblastoma Cells

Somato-axodendritic release of oxytocin into the brain due to calcium amplification is essential for social memory

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